Securities Registration (foreign Private Issuer) (f-1/a)

AMENDMENT NO. 1
TO
FORM F-1
REGISTRATION STATEMENT
UNDER
THE SECURITIES ACT OF 1933

Hejreskovvej 10A
DK-3490 Kvistgaard
Denmark
+45 33 26 83 83
(Address, including zip code, and telephone number, including area code, of Registrant's principal executive offices)

Bavarian Nordic Inc.
595 Penobscot Drive
Redwood City, CA 94063
Attention: Seth Lewis
(978) 341-5271
(Name, address, including zip code, and telephone number, including area code, of agent for service)

Approximate date of commencement of proposed sale to the public:
As soon as practicable after the effective date of this Registration Statement.

If any of the securities being registered on this Form are to be offered on a delayed or continuous basis pursuant to Rule 415 under the Securities Act of 1933, check the following box. o

If this Form is filed to register additional securities for an offering pursuant to Rule 462(b) under the Securities Act, check the following box and list the Securities Act registration statement number of the earlier effective registration statement for the same offering. o

If this Form is a post-effective amendment filed pursuant to Rule 462(c) under the Securities Act, check the following box and list the Securities Act registration statement number of the earlier effective registration statement for the same offering. o

If this Form is a post-effective amendment filed pursuant to Rule 462(d) under the Securities Act, check the following box and list the Securities Act registration statement number of the earlier effective registration statement for the same offering. o

The Registrant hereby amends this Registration Statement on such date or dates as may be necessary to delay its effective date until the Registrant shall file a further amendment which specifically states that this Registration Statement shall thereafter become effective in accordance with Section 8(a) of the Securities Act of 1933 or until the Registration Statement shall become effective on such date as the Commission, acting pursuant to said Section 8(a), may determine.

The information in this prospectus is not complete and may be changed. We may not sell these securities until the registration statement filed with the Securities and Exchange Commission is effective. This prospectus is not an offer to sell these securities and it is not soliciting an offer to buy these securities in any U.S. state or other jurisdiction where the offer or sale is not permitted.

This is an initial public offering of American Depositary Shares, or ADSs, representing shares of Bavarian Nordic A/S. Each ADS represents one-third of a share of Bavarian Nordic A/S of nominal value Danish kroner, or DKK, 10.

Currently, our shares are traded on Nasdaq Copenhagen A/S ("Nasdaq Copenhagen") under the symbol "BAVA" and our ADSs are traded on the over-the-counter market in the United States under the symbol "BVNRY." The closing price of our shares on Nasdaq Copenhagen on , 2016 was DKK per share, which equals a price of $ per ADS based on the U.S. dollar/DKK exchange rate as of , 2016 and an ADS-to-share ratio of 3:1. We have applied to list the ADSs on The NASDAQ Global Select Market under the symbol "BAVN."

We are an "emerging growth company" as defined by the Jumpstart Our Business Startups Act of 2012 and as such, will be subject to reduced public company reporting requirements for this prospectus and future filings.

Investing in the ADSs involves risks that are described in the "Risk Factors" section beginning on page 14 of this prospectus.

None of the Securities and Exchange Commission, any U.S. state securities commission, the Danish Financial Supervisory Authority, or any other foreign securities commission has approved or disapproved of these securities or determined if this prospectus is truthful or complete. Any representation to the contrary is a criminal offense.

The underwriters may also exercise their option to purchase up to an additional ADSs from us, at the same price per ADS as paid for the ADSs offered hereby, for 30 days after the date of this prospectus.

The ADSs will be ready for delivery through the facilities of The Depository Trust Company on or about , 2016.

Neither we nor the underwriters have authorized anyone to provide you with information that is different from that contained in this prospectus or in any free writing prospectus we may authorize to be delivered or made available to you. We take no responsibility for, and can provide no assurance as to the reliability of, any other information that others may give you. We and the underwriters are offering to sell ADSs and seeking offers to purchase ADSs only in jurisdictions where offers and sales are permitted. The information contained in this prospectus is accurate only as of the date on the front of this prospectus, regardless of the time of delivery of this prospectus or any sale of ADSs.

Until , 2016 (the 25th day after the date of this prospectus), all dealers that effect transactions in these securities, whether or not participating in this offering, may be required to deliver a prospectus. This is in addition to the dealers' obligation to deliver a prospectus when acting as underwriters and with respect to their unsold allotments or subscriptions.

For investors outside of the United States: Neither we nor any of the underwriters have taken any action to permit this offering or possession or distribution of this prospectus in any jurisdiction where action for that purpose is required, other than in the United States. You are required to inform yourselves about and to observe any restrictions relating to this offering and the distribution of this prospectus.

Bavarian Nordic, PROSTVAC and IMVAMUNE/IMVANEX are trademarks of ours that we use in this prospectus. This prospectus also includes trademarks, tradenames and service marks that are the property of other organizations. Solely for convenience, our trademarks and tradenames referred to in this prospectus appear without the ® and ™ symbols, but those references are not intended to indicate, in any way, that we will not assert, to the fullest extent under applicable law, our rights, or the right of the applicable licensor to our trademark and tradenames.

We maintain our books and records in Danish kroner, or DKK, and report under International Financial Reporting Standards, or IFRS, as issued by the International Accounting Standards Board, or IASB. None of the consolidated financial statements in this prospectus were prepared in accordance with accounting principles generally accepted in the United States. Except with respect to U.S. dollar amounts presented as contractual terms, all amounts that are presented in U.S. dollars herein have been translated into DKK solely for convenience at an assumed exchange rate of DKK 6.66 per 1.00 U.S. dollar, which was the exchange rate as of September 30, 2015, as reported by Danmarks Nationalbank. We use the symbol "$" to refer to the U.S. dollar herein.

All references to "shares" in this prospectus refer to shares of Bavarian Nordic A/S of nominal value DKK 10 per share.

PROSPECTUS SUMMARY

This summary highlights information contained elsewhere in this prospectus and does not contain all of the information that you should consider in making your investment decision. Before deciding to invest in the ADSs, you should read this entire prospectus carefully, including the sections of this prospectus entitled "Risk Factors" and "Management's Discussion and Analysis of Financial Condition and Results of Operations" and our consolidated financial statements contained elsewhere in this prospectus. Unless the context otherwise requires, references in this prospectus to the "company," "Bavarian Nordic," "we," "us" and "our" refer to Bavarian Nordic A/S and its subsidiaries. In this prospectus, references to "DKK" are to Danish kroner, the lawful currency of the Kingdom of Denmark.

Overview

We are a fully integrated biotechnology company developing, manufacturing and commercializing novel vaccines for the prevention of life-threatening infectious diseases and the treatment of cancer. We focus on diseases for which the unmet medical need is high and for which we can harness the power of the immune system to induce a response. Our live virus vaccine platform employs poxviruses in a modular approach to create our vaccines. This platform has generated one commercial product for smallpox, one Phase 3 immunotherapy candidate for prostate cancer, one Phase 3 candidate for Ebola and several other clinical programs in the areas of infectious disease and oncology. We recognized revenue of $182 million in 2013 and $183 million in 2014 primarily from sales of our commercial smallpox vaccine, IMVAMUNE/IMVANEX. This revenue has enabled us to invest significant capital into research and development activities, the expansion of our production infrastructure and the advancement of our clinical pipeline.

Our poxvirus vaccines are designed to enhance the immune system through the production of antibodies and the stimulation of T-cells. The poxvirus family consists of viruses with larger DNA genomes than other viruses. The large genome of poxviruses allows for insertion of genetic material encoding for multiple and relatively large antigens, which are toxins or foreign substances that induce an immune response. This enables us to create vaccines for a wide variety of diseases. It also permits us to target multiple antigens for a single disease, which we believe leads to a more robust vaccine. There are three types of poxviruses that we may employ to achieve a desired effect: Modified Vaccinia Ankara, or MVA, vaccinia and Fowlpox. We optimize these poxviruses with our proprietary technology to incorporate an antigen in order to create recombinant viral vaccines. We employ these viruses in various combinations for both the initial vaccination, or primer, and subsequent vaccination(s), or booster(s).

Our vaccine expertise has led to a 10+ year relationship with the U.S. government, pursuant to which we have been awarded approximately $1.2 billion in contracts. To date, we have recognized more than $900 million of revenue from these contracts. We believe that we are well positioned to generate additional revenue from such contracts due to our track record of success, relationships with U.S. governmental agencies and the quality of our live virus vaccines. More recently, we believe our platform has been validated by commercial relationships with two large pharmaceutical companies, Bristol-Myers Squibb, or BMS, for PROSTVAC, our Phase 3 cancer immunotherapy candidate, and the Janssen Pharmaceutical Companies of Johnson & Johnson, or Janssen, for our Ebola vaccine candidate and additional infectious disease targets. We also work closely with the National Cancer Institute, or NCI, and the National Institutes of Health, or the NIH, towards the development of key technologies underlying our product candidates.

We have built an extensive patent portfolio comprised of more than 740 granted/issued patents and more than 240 pending patent applications.

Our Infectious Disease Portfolio

IMVAMUNE/IMVANEX—Smallpox Vaccine

Smallpox is a contagious, disfiguring and often deadly disease. The Department of Homeland Security has declared smallpox to be a material threat to national security, and the U.S. Centers for Disease Control and Prevention classifies smallpox as a Category A bioterror agent. No cure or treatment for smallpox exists. The only existing vaccine approved for use in the United States to prevent smallpox is ACAM2000, a live replicating virus. ACAM2000 has several important drawbacks, including known cardiac toxicity with suspected cases of myocarditis and pericarditis observed in 5.7 per 1,000 individuals vaccinated. Additionally, the administration of the vaccine is contraindicated for certain individuals in the United States, including those with severe immunodeficiency. In the United States, this translates into a population of over 66 million people.

IMVAMUNE, which is also marketed under the trade name IMVANEX in Europe, is a non-replicating smallpox vaccine that is suitable for use in people for whom replicating smallpox vaccines are contraindicated. The vaccine is currently commercialized in a liquid frozen formulation. The vaccine is the only non-replicating smallpox vaccine approved in Europe for use in the general adult population. Although not yet approved in the United States, we have also supplied 28 million doses of IMVAMUNE/IMVANEX to the U.S. government. The U.S. government stockpiles IMVAMUNE/IMVANEX, which it would be able to distribute under an emergency use authorization, or EUA, in the event of an emergency outbreak of smallpox. IMVAMUNE is currently being evaluated in a Phase 3 program to support U.S. approval by the FDA for the entire population. We recognized revenue of DKK 839 million ($126 million) and DKK 1,024 million ($154 million) in 2013 and 2014, respectively, from sales of IMVAMUNE/IMVANEX.

We are also developing a freeze dried formulation of IMVAMUNE/IMVANEX under a contract with the U.S. government to replace the current liquid frozen version. Due to a potential shelf life of approximately 10 or more years, we believe that our freeze dried formulation is well positioned to fulfill the U.S. government's long-term requirements for a smallpox vaccine. In May 2015, we reported data from a pivotal Phase 2 randomized, double-blind trial that enrolled 650 vaccinia-naïve healthy subjects to compare the safety and immunogenicity of our freeze dried and liquid frozen formulations of IMVAMUNE/IMVANEX. The antibody response induced by the freeze dried vaccine was equivalent to the antibody response induced by the liquid frozen formulation, meeting the primary endpoint of the trial. These results provided the final clinical data required to support stockpiling of this next generation of the vaccine and the validation of the production process remains the final step towards meeting the overall requirements for the stockpiling of the vaccine by BARDA.

MVA-BN RSV—Respiratory Syncytial Virus Vaccine Candidate

Respiratory syncytial virus, or RSV, is the most common cause of lower respiratory tract infection in infants and children worldwide, resulting in a high number of hospitalizations. RSV infections are responsible each year for a similar number of deaths as the flu in children up to age 14, as well as in the elderly population. While numerous efforts have been made to develop a prophylactic vaccine, there is currently no approved vaccine against RSV.

Our product candidate, MVA-BN RSV, has been shown to be highly efficacious in preclinical models, demonstrating both an antibody and a T-cell response from the immune system. Published data have shown that both responses are required to prevent an RSV infection. In addition to antibodies in the blood, the presence of antibodies in the mucous membranes is an important barrier

to infection by RSV. Preclinical studies and clinical trials have shown that MVA-BN RSV brings about such an antibody response in the mucosa. Following a pre-investigational new drug application, or IND, meeting with the FDA, a Phase 1 trial in healthy adults was initiated in August 2015. This Phase 1 trial, which is being conducted in the United States, is evaluating the safety, tolerability and immunogenicity of our recombinant MVA-BN-based RSV vaccine in 63 healthy adults, ages 18 to 65. The trial is now fully enrolled and we anticipate results will be reported in the first half of 2016. If the Phase 1 trial is successful, we intend to rapidly progress our RSV vaccine candidate into multiple Phase 1 and Phase 2 trials in elderly and adult at-risk populations, as well as the pediatric population.

MVA-BN Filo—Ebola Vaccine Candidate and Agreement with Janssen

In 2014, in response to the crisis in West Africa, we accelerated the development and production of MVA-BN Filo, a new Ebola vaccine candidate that may eventually be deployed in a campaign to help stem a future outbreak of Ebola. This important development was possible because we recognized the public health dangers of Ebola and initiated a filovirus vaccine program in 2010. In October 2014, we entered into an agreement pursuant to which we granted Janssen an exclusive license for our MVA-BN Filo vaccine candidate. We received an upfront payment of $25 million and are entitled to receive up to $20 million in milestone payments. We are also entitled to royalties from sales outside of Africa. In consideration of the recent outbreak of Ebola in Africa, we have elected not to receive royalties from sales of MVA-BN Filo vaccine in Africa. We have also entered into a supply agreement with Janssen under which we will produce and deliver bulk material for a total value of $99 million. Furthermore, Johnson & Johnson Development Corporation made a $43 million equity investment in our company.

MVA-BN Filo is a prime-boost regimen consisting of a primer, Ad26.ZEBOV, which Janssen developed, and a boost, MVA-BN Filo, which we developed. Backed by worldwide health authorities, Janssen is fast-tracking the clinical development of this prime-boost vaccine regimen. Janssen presented preliminary results from a Phase 1 trial in May 2015, which showed that the prime-boost vaccine regimen was immunogenic. A multicenter Phase 2 clinical trial was initiated by Janssen in the United Kingdom and France in July 2015. A second Phase 2 trial with an expected enrollment of approximately 1,188 subjects and a Phase 3 trial with an expected enrollment of approximately 440 subjects have also been initiated in Africa. Data from the Phase 3 clinical trial in Africa are expected in 2016.

Following the Ebola vaccine agreement, in December 2015, we entered into a collaboration and license agreement with Janssen. Pursuant to the agreement, Janssen will acquire exclusive rights to our MVA-BN technology for use in a prime-boost vaccine regimen together with Janssen's adenovirus vector based technology. The goal is to develop a vaccine to treat chronic HPV infections as well as prevent precancerous stages of HPV-induced cancer. HPV is known to be the primary cause of cervical cancer and certain types of head and neck cancer, in addition to a number of more rare cancers. We expect that Janssen will focus initially on cervical cancer and then head and neck cancers. Janssen continues to retain an exclusive option to license MVA-BN for two additional infectious disease targets. Given the clinical efficacy seen in the reported Ebola prime-boost vaccine regimen, we believe that this prime-boost approach warrants additional investigation in several infectious diseases.

Our Cancer Immunotherapy Portfolio

Immunotherapy is part of a growing field in cancer research and treatment. Our product candidates have been designed to enhance a specific T-cell response against a tumor target. By eliciting a strong T-cell immune response, immunotherapies may slow the progress of the disease and increase overall survival, or OS, with an improved safety profile compared to many traditional

chemotherapies and hormone treatments. Another benefit of the enhanced T-cell response is that the tumor is subsequently more immunogenic and sensitive to additional targeted therapies. Based on trials conducted to date, we believe that the favorable side effect profile of our product candidates may allow them to be combined with other cancer therapies and to be used at earlier stages of disease. We are developing our immunotherapy product candidates to be used both in monotherapy and in combination regimens.

PROSTVAC for the Treatment of Prostate Cancer

According to the CDC, prostate cancer is the most common cancer in U.S. men. The American Cancer Society estimates that in 2015, approximately 220,800 new cases of prostate cancer will be diagnosed and approximately 27,540 deaths will occur. While there has been meaningful progress in the treatment of prostate cancer, including approvals of new drugs by the FDA, we believe that combination therapy holds great potential to provide a clinically meaningful advance.

PROSTVAC is a prostate-specific antigen targeted immunotherapy candidate currently in Phase 3 development for the treatment of patients with asymptomatic or minimally symptomatic metastatic castration-resistant prostate cancer, or mCRPC. PROSTVAC has been administered to more than 1,500 patients in more than 14 ongoing or completed Phase 1, Phase 2 and Phase 3 clinical trials. In several of these trials, the administration of PROSTVAC has resulted in a robust T-cell response and promising evidence of safety and efficacy, including a survival benefit, both as monotherapy and when dosed in combination with other therapies, including checkpoint inhibitors, a class of drugs that may enhance the anti-tumor T-cell response.

In March 2015, we entered into an option agreement with BMS granting BMS an option to license and commercialize PROSTVAC that included a $60 million upfront payment. If BMS exercises the option and the license goes into effect, we would be entitled to milestone payments up to an aggregate of $915 million, as well as royalty payments on the development and commercialization of PROSTVAC. See the section of this Prospectus entitled "Business—Our Partnerships—Agreement with BMS Regarding PROSTVAC." We believe that BMS's strong presence in cancer immunotherapy makes them an ideal partner to maximize the potential of PROSTVAC.

We are currently evaluating PROSTVAC in a Phase 3 clinical trial, which is known as PROSPECT. PROSPECT is a global randomized, double-blind, placebo-controlled trial in patients with asymptomatic or minimally symptomatic mCRPC. The primary objective of the trial is to determine whether the OS of patients receiving PROSTVAC, with or without the addition of GM-CSF, is superior to that of patients receiving placebo. While the placebo-controlled Phase 2 trial included the use of GM-CSF, additional clinical work has shown that the administration of GM-CSF with PROSTVAC may not be required. The PROSPECT trial was designed to potentially rule out the need for GM-CSF.

The enrollment criteria for the PROSPECT trial was designed to enroll patients who we believe would benefit most from PROSTVAC. We believe that immunotherapy takes time to demonstrate its beneficial effects, and we therefore seek to select patients who we believe have a sufficient life expectancy to benefit from PROSTVAC. Using the randomized Phase 2 trial as a guide, certain entry criteria were amended to better identify patients who we believe have a better chance of benefiting from PROSTVAC. Although the trial is powered to detect a difference in survival between active treatment and placebo at final analysis, three pre-specified interim analyses of data have been integrated into the statistical plan to evaluate whether the trial should continue as planned or potentially be stopped early for efficacy or futility. While PROSPECT is event driven, the trial met its target enrollment as of December 2014 and was fully enrolled as of January 2015, and we anticipate reporting top-line data in 2017.

We also believe that PROSTVAC has significant potential in combination therapy. Among the ongoing clinical trials of PROSTVAC that we are conducting are five Phase 2 clinical trials sponsored by the NCI, evaluating PROSTVAC in earlier prostate cancer disease settings and/or in combination with several other therapies, including checkpoint inhibitors. Following long-term survival data from a combination trial of PROSTVAC and ipilimumab, which indicated potential synergy, we have also agreed with BMS to perform a trial evaluating the combination of PROSTVAC with one of BMS's checkpoint inhibitors, which is expected to be initiated by early 2016.

CV 301 for the Treatment of Multiple Solid Tumors

CV 301 is a cancer immunotherapy candidate that targets two tumor-associated antigens, CEA and MUC-1, that are over-expressed in major cancer types, including lung, bladder and colorectal cancer. CV 301 and its precursors have been tested in 6 ongoing or completed NCI-sponsored clinical trials in various cancers, and more than 300 patients have been treated with the product candidate. One trial, which investigated the effects of CV 301 in 74 patients with resected metastatic colorectal cancer, showed a significant survival benefit over a set of matched, controlled patients who were treated at Duke University. These matched, controlled patients were not enrolled in the trial, but were colorectal cancer patients undergoing approved therapies, and each group was evaluated to compare how OS differed. While CV 301 is currently being evaluated in a Phase 2 clinical trial as monotherapy for the treatment of bladder cancer at the NCI, we are also developing an improved construct of CV 301 and expect to initiate production of new clinical trial material in the coming months in bladder and colorectal indications, among others.

Combination treatments continue to play an important role in the rapidly changing cancer treatment paradigm. Our strategy is to develop CV 301 for use in combination with checkpoint inhibitors, as there have been promising preclinical data in this area. While we have rights to multiple indications for CV 301, the initial target will be non-small cell lung cancer, or NSCLC. We expect to initiate a Phase 2 clinical trial in the second half 2016 for the treatment of NSCLC. While NSCLC represents the first clinical target in a combination regimen we plan to initiate no less than three separate randomized, placebo-controlled Phase 2 trials in NSCLC, bladder cancer and colorectal cancer, in combination with assorted checkpoint inhibitors. These trials will evaluate the efficacy of the individual components, as well as the combination of the vaccine and checkpoint inhibitor to determine what, if any, synergy can be seen in combination.

MVA-BN Brachyury for the Treatment of Metastatic Cancer and Chordoma

MVA-BN Brachyury is a cancer immunotherapy developed using our live virus platform. It is designed to induce a robust T-cell immune response against brachyury, a tumor-associated antigen that is overexpressed in major solid tumor indications. Brachyury is reported to play a key role in the metastasis and progression of tumors. Tumors that overexpress brachyury are believed to be highly resistant to current therapies and are associated with decreased survival rates.

In November 2015, we released the results of an NCI-sponsored Phase 1 trial of MVA-BN Brachyury in patients with metastatic cancer or chordoma, an ultra-orphan, or extremely rare, brachyury-expressing cancer of the skull and spine. The trial was an open-label, Phase 1 trial and enrolled 38 patients with metastatic cancer or chordoma. The objective of the trial was to determine the safety and tolerability of escalating doses of MVA-BN Brachyury and to evaluate immunologic responses as measured by an increase in brachyury-specific T-cells. Data from this trial demonstrated for the first time that an MVA-BN based vaccine targeting brachyury can induce brachyury-specific T-cell immune responses in advanced cancer patients. MVA-BN Brachyury was well-tolerated with no dose limiting toxicities. The maximum tolerated dose was not reached and no serious adverse vaccine-related events were observed. We intend to continue to work with the NCI to evaluate MVA-BN Brachyury in multiple solid tumors. We retain exclusive rights to this program and will determine if and when a corporate partnership is appropriate.

Competitive Advantages

We are a fully integrated biotechnology company, and we believe that we have several key competitive advantages in developing, producing and commercializing live virus vaccines:

§: Existing revenue generation supports current development pipeline. Our existing revenue generation from our government contracts and from our commercial partnerships can be used to invest in the advancement of our development pipeline.
§: Modular and proprietary vaccine technology. Our poxvirus-based vaccine platform takes a modular approach to live virus vaccine development, which we believe allows us to develop effective vaccines with a favorable safety profile that can be used across a variety of indications in infectious diseases and cancer.
§: Fully operational, commercial scale cGMP production facility. Our ability to effectively and efficiently produce our live virus vaccines has been demonstrated by our production of 28 million doses of IMVAMUNE/IMVANEX and more than 2 million doses of MVA-BN Filo to date.
§: Ongoing relationships with government agencies. The process for entering into government contracts is often time-consuming and complicated. We have entered into contracts with the U.S. government worth approximately $1.2 billion, of which we have recognized over $900 million in revenue to date.
§: Validating collaborations with BMS and Janssen. We have entered into an agreement granting BMS an option to commercialize PROSTVAC on a global basis and partnerships with Janssen for the development of MVA-BN Filo and a preclinical program.
§: Broad intellectual property estate. We own a broad patent portfolio of more than 740 patents and more than 240 patent applications related to our vaccine technology.
§: Experienced management team. We have a strong management team with broad expertise in the development of vaccine technologies.

Our Strategy

We have developed our live virus vaccine platform over more than 20 years with the goal of protecting the world's general and at-risk populations by providing highly immunogenic and differentiated technologies with a favorable safety profile. Our strategy includes the following elements:

§: Maintain the global leadership of our IMVAMUNE/IMVANEX franchise.
§: Maximize PROSTVAC's commercial potential as monotherapy and in combination regimens.

Implications of Being an "Emerging Growth Company" and a Foreign Private Issuer

As a company with less than $1 billion in revenue during our last fiscal year, we qualify as an "emerging growth company" as defined in the Jumpstart Our Business Startups Act of 2012, or the JOBS Act. An emerging growth company may take advantage of specified reduced reporting and other burdens that are otherwise applicable generally to public companies. These provisions include:

§: a requirement to have only two years of audited financial statements and only two years of related Management's Discussion and Analysis of Financial Condition and Results of Operations disclosure; and
§: an exemption from the auditor attestation requirement in the assessment of our internal control over financial reporting pursuant to the Sarbanes-Oxley Act of 2002, or the Sarbanes-Oxley Act.

We may take advantage of these provisions for up to five years or such earlier time that we are no longer an emerging growth company. We would cease to be an emerging growth company if we have more than $1 billion in annual revenue, have more than $700 million in market value of the equity securities held by non-affiliates, or issue more than $1 billion of non-convertible debt over a three-year period. We may choose to take advantage of some but not all of these reduced burdens, and therefore the information that we provide holders of shares and ADSs may be different than the information you might receive from other public companies in which you hold equity. In addition, Section 107 of the JOBS Act also provides that an emerging growth company can take advantage of an extended transition period for complying with new or revised accounting standards applicable to public companies. We currently prepare our consolidated financial statements in accordance with IFRS, as issued by the IASB, which do not have separate provisions for publicly traded and private companies. However, in the event that we convert to accounting principles generally accepted in the United States (which we do not currently intend to do) while we remain an emerging growth company, we have irrevocably elected to opt out of such extended transition period.

Upon consummation of this offering, we will report under the Securities Exchange Act of 1934, as amended, or the Exchange Act, as a non-U.S. company with foreign private issuer status. Even after we no longer qualify as an emerging growth company, as long as we qualify as a foreign private issuer under the Exchange Act we will be exempt from certain provisions of the Exchange Act that are applicable to U.S. domestic public companies, including:

§: the sections of the Exchange Act regulating the solicitation of proxies, consents or authorizations in respect of a security registered under the Exchange Act;
§: the sections of the Exchange Act requiring insiders to file public reports of their stock ownership and trading activities and liability for insiders who profit from trades made in a short period of time; and
§: the rules under the Exchange Act requiring the filing with the Securities and Exchange Commission, or SEC, of quarterly reports on Form 10-Q containing unaudited financial and other specified information, or current reports on Form 8-K, upon the occurrence of specified significant events.

Both foreign private issuers and emerging growth companies are also exempt from certain more stringent executive compensation disclosure rules. Thus, even if we no longer qualify as an emerging growth company, but remain a foreign private issuer, we will continue to be exempt from the more stringent compensation disclosures required of companies that are neither an emerging growth company nor a foreign private issuer.

SUMMARY CONSOLIDATED FINANCIAL DATA

The following tables present summary consolidated financial data for our business.

We derived the summary consolidated income statements data for the years ended December 31, 2014 and 2013 from our audited consolidated financial statements included elsewhere in this prospectus. We derived the summary consolidated income statements data for the nine months ended September 30, 2015 and 2014 and the summary consolidated statement of financial position data as of September 30, 2015 from our unaudited condensed consolidated interim financial statements included elsewhere in this prospectus. The pro forma data included in the summary consolidated statement of financial position data is unaudited.

We maintain our books and records in DKK, and prepare our audited consolidated financial statements in accordance with IFRS as issued by the IASB and our unaudited condensed consolidated interim financial statements in accordance with IAS 34 Interim Financial Reporting as issued by the IASB.

You should read this data together with our consolidated financial statements and related notes appearing elsewhere in this prospectus and the information under the captions "Capitalization" and "Management's Discussion and Analysis of Financial Condition and Results of Operations." Our historical results are not necessarily indicative of our future results, and our interim period results are not necessarily indicative of results to be expected for a full year or any other interim period.

Consolidated Income Statements Data:

	Year Ended December 31,							Nine Months Ended September 30,

	2014		2014		2013			2015		2015		2014
(in millions, except per share amounts)	$(1)		DKK		DKK			$(1)		DKK		DKK
Revenue	$	182.7		1,216.8		1,212.5		$	105.6		703.0		675.6
Production costs		74.4		495.1		484.7			36.9		245.7		328.1

Gross profit		108.3		721.7		727.8			68.7		457.3		347.5
Research and development costs		71.9		478.9		496.6			44.5		296.8		313.5
Distribution costs		6.8		45.1		40.8			5.0		33.0		34.4
Administrative costs		27.1		181.0		157.0			18.8		125.3		120.9

Total operating costs		105.8		705.0		694.4			68.3		455.1		468.8

Income (loss) before interest and tax (EBIT)		2.5		16.7		33.4			0.4		2.2		(121.3	)
Financial income		8.6		57.3		6.6			11.8		78.9		40.0
Financial expenses		1.5		9.7		33.8			3.1		20.6		3.2

Income (loss) before company tax		9.6		64.3		6.2			9.1		60.5		(84.5	)
Tax (benefit) on income (loss) for the year		5.7		38.4		52.9			0.5		3.4		(12.5	)

Net profit (loss) for the year	$	3.9		25.9		(46.7	)	$	8.6		57.1		(72.0	)



Earnings per share (EPS)
Basic earnings per share	$	0.15		1.0		(1.8	)	$	0.32		2.1		(2.8	)
Diluted earnings per share	$	0.15		1.0		(1.8	)	$	0.32		2.1		(2.8	)

(1): Translated solely for convenience into U.S. dollars at an assumed exchange rate of DKK 6.66 per 1.00 U.S. dollar, which was the exchange rate of such currencies as of September 30, 2015.

Investing in the ADSs involves a high degree of risk. You should carefully consider the risks described below, as well as the other information in this prospectus, including our consolidated financial statements and "Management's Discussion and Analysis of Financial Condition and Results of Operations," before deciding whether to invest in the ADSs. The occurrence of any of the events or developments described below could harm our business, financial condition, results of operations and growth prospects. In such an event, the market price of the ADSs could decline, and you may lose all or part of your investment.

We recognized limited profits in 2014 and the first nine months of 2015. Our ability to generate revenue from product sales and sustain our limited profitability depends on our ability to continue to successfully commercialize IMVAMUNE/IMVANEX and the ability of us and our collaboration partners to successfully complete the development of our product candidates and obtain the regulatory and marketing approvals necessary to commercialize one or more of our product candidates. Our ability and our collaborators' ability to generate future revenue from product sales or pursuant to milestone payments depend heavily on many factors, including, but not limited to:

A substantial portion of our revenues are attributable to government contracts and substantial delays in purchase decisions by governmental entities, governments' decisions on when and if to exercise certain options under their contracts with us, and the timing of when we achieve certain milestones that would entitle us to payment could cause our revenues and income to drop substantially or to fluctuate significantly between fiscal periods.

In cases where we, or our collaboration partners, are successful in obtaining regulatory approvals to market one or more of our product candidates, our revenue will be dependent, in part,

upon the size of the markets in the territories for which regulatory approval is granted, the price or prices at which we are able to sell such products and our ability to get paid or reimbursed for our products at such prices. If the number of individuals suitable for our product candidates is not as significant as we estimate, the indications approved by regulatory authorities are narrower than we expect or the reasonably accepted population for vaccination is narrowed by competition, physician choice or vaccination guidelines, we may not generate significant revenue from the sale of such products, even if approved. Our failure to generate revenue from sales of one or more of our product candidates or pursuant to upfront or milestone payments could have a material adverse effect on our business and financial results.

For certain clinical development programs, we depend on collaboration partners to develop and conduct clinical trials with, obtain regulatory approvals for, and market and sell our product candidates. If such collaboration partners fail to perform as expected, the potential for us to generate future revenue from such product candidates would be significantly reduced and our business would be significantly harmed.

For certain programs, we may rely on our collaboration partners to develop, conduct clinical trials of, and commercialize our product candidates. We have existing collaborations with the United States Public Health Service, or PHS, the NIH, BMS and Janssen. We may also enter into collaboration agreements with other parties in the future relating to our other product candidates. Ultimately, if such product candidates are advanced through clinical trials and receive marketing approval from the EMA, the FDA or similar regulatory authorities, certain of our collaboration partners may be responsible for commercialization of these collaboration products. The potential for us to obtain future development milestone payments and, ultimately, generate revenue from royalties on sales of such collaboration products depends on the successful development, regulatory approval, marketing and commercialization by our collaboration partners. If our collaboration partners do not perform in the manner we expect or fail to fulfill their responsibilities in a timely manner, or at all, if our agreements with them terminate or if the quality or accuracy of the clinical data they obtain is compromised, the clinical development, regulatory approval and commercialization efforts related to our product candidates could be delayed or terminated and it could become necessary for us to assume the responsibility at our own expense for the clinical development of such product candidates. In that event, we would likely be required to limit the size and scope of efforts for the development and commercialization of such product candidate; we would likely be required to seek additional financing to fund further development or identify alternative strategic collaboration partners; our potential to generate future revenue from royalties and milestone payments from such product candidates would be significantly reduced or delayed; and it could have a material adverse effect on our business and financial results.

In addition, certain collaboration agreements provide our collaboration partners with rights to terminate such agreements and licenses under various conditions, which, if exercised, would adversely affect our product development efforts, could make it difficult for us to attract new partners and adversely affect our reputation. Our collaboration partners may have the right to terminate their respective collaboration agreements with us in the event of one or more of the following reasons: our uncured material breach of the agreement for convenience or our failure, or our product candidates' failure to meet certain specified milestones. For example, under our license agreements with PHS, which provide us with the right to use certain intellectual property related to our cancer immunotherapy product candidates, PHS has the right to terminate these license agreements if we fail to execute our development plan or reach certain milestones by certain dates. Furthermore, under our agreement with BMS, BMS may choose not to exercise its option to take a license to PROSTVAC.

The timing and amount of any milestone and royalty payments we may receive under our agreements with our collaboration partners will depend on, among other things, the efforts, allocation

of resources, and successful development and commercialization of our product candidates. We cannot be certain that any of the development and regulatory milestones will be achieved or that we will receive any future milestone payments under these agreements. In addition, in certain circumstances we may believe that we have achieved a particular milestone and the applicable collaboration partner may disagree with our belief. In that case, receipt of that milestone payment may be delayed or may never be received, which may require us to adjust our operating plans.

Our product candidates will need to undergo clinical trials that are time-consuming and expensive, the outcomes of which are unpredictable, and for which there is a high risk of failure. If clinical trials of our product candidates fail to satisfactorily demonstrate safety and efficacy to the EMA, FDA and other similar regulators, we may incur additional costs or experience delays in completing, or ultimately be unable to complete, the development of these product candidates.

The European Commission (following review by the EMA) in Europe, the FDA in the United States and comparable regulatory authorities in other jurisdictions must approve new drug or biologic candidates before they can be marketed, promoted or sold in those territories. We must provide these regulatory authorities with data from nonclinical studies and clinical trials that demonstrate that our product candidates are safe and effective for a specific indication before they can be approved for commercial distribution. Our smallpox vaccine, marketed under the trade names IMVAMUNE and IMVANEX in Canada and the European Union, respectively, is our only approved product, and is not yet approved in the United States. Although not yet approved in the United States, we have also supplied 28 million doses of IMVAMUNE/IMVANEX to the U.S. government. The U.S. government stockpiles IMVAMUNE/IMVANEX in the event of an emergency outbreak of smallpox, which it would be able to distribute in such event under an EUA. We cannot assure you that our Phase 3 trials of IMVAMUNE/IMVANEX or PROSTVAC will be successful or that IMVAMUNE/IMVANEX will receive approval from the FDA or that any of our other product candidates will receive approval from the EMA or FDA or any other comparable regulatory authority.

Preclinical testing and clinical trials are long, expensive and unpredictable processes that can be subject to extensive delays. We cannot guarantee that any clinical trials will be conducted as planned or completed on schedule, if at all. For example, our ongoing Phase 3 trial of IMVAMUNE/IMVANEX is currently being conducted in collaboration with the U.S. government. The FDA has substantial control over the enrollment and other decisions regarding this trial and these decisions may cause delays or impact our ability to complete this trial to the satisfaction of the FDA or other regulatory authorities. The primary endpoint of the ongoing Phase 3 trial of PROSTVAC is event driven and it is therefore difficult to predict when OS data will be available to report. It may take several years to complete the preclinical testing and clinical development necessary to commercialize a product candidate, and delays or failure can occur at any stage. Interim results of clinical trials do not necessarily predict final results, and success in preclinical testing and early clinical trials does not ensure that later clinical trials will be successful. A number of companies in the pharmaceutical, biopharmaceutical and biotechnology industries have suffered significant setbacks in advanced clinical trials even after promising results in earlier trials, and we cannot be certain that we will not face similar setbacks. The design of a clinical trial can determine whether its results will support approval of a product, and flaws in the design of a clinical trial may not become apparent until the clinical trial is well advanced. An unfavorable outcome in one or more trials would be a major setback for our product candidates and for us. An unfavorable outcome in one or more trials may require us to delay, reduce the scope of or eliminate one or more product development programs, which could have a material adverse effect on our business and financial results.

In connection with clinical testing and trials, we face a number of risks, including risks that:

The results of preclinical studies do not necessarily predict clinical success, and larger and later-stage clinical trials may not produce the same results as earlier-stage clinical trials. Our and our collaborators' clinical trials of our product candidates conducted to date have generated favorable safety and efficacy data. However, we may have different enrollment criteria in our future clinical trials. As a result, we may not observe a similarly favorable safety or efficacy profile as in our prior clinical trials. For example, while the results of the Phase 2 trials for PROSTVAC showed potential efficacy and acceptable safety results, our Phase 3 trials may fail to produce similar results. Additionally, our Phase 3 trial of IMVAMUNE/IMVANEX may fail to show positive safety and efficacy and we may not be successful in commercializing the vaccine in the United States. It is also possible that PROSTVAC may not demonstrate any clinical benefits either as monotherapy or in combination with other therapies. In addition, we cannot assure you that in the course of potential widespread use of any of our product candidates in future, we will not suffer setbacks in maintaining production quality or stability. In addition, clinical trials of potential products often reveal that it is not possible or practical to continue development efforts for these product candidates. If we do not successfully complete preclinical and clinical development, we will be unable to market and sell our product candidates and generate additional revenue. Even if we successfully complete clinical trials, those results are not necessarily predictive of results of additional trials that may be needed before marketing applications may be submitted to the EMA or FDA, as applicable.

Furthermore, we sometimes estimate for planning purposes the timing of the accomplishment of various scientific, clinical, regulatory and other product development objectives. These milestones may include our expectations regarding the commencement or completion of scientific studies, clinical trials, the submission of regulatory filings or commercialization objectives. From time to time, we may publicly announce the expected timing of some of these milestones, such as the completion of an ongoing clinical trial, the initiation of other clinical programs, receipt of marketing approval or a commercial launch of a product. The achievement of many of these milestones may be outside of our control. All of these milestones are based on a variety of assumptions, which may cause the timing of achievement of the milestones to vary considerably from our estimates. If we fail to achieve announced milestones in the timeframes we expect, the commercialization of our product candidates may be delayed, we may not be entitled to receive certain contractual payments and it could have a material adverse effect on our business and financial results.

IMVAMUNE/IMVANEX, approved for sale in the European Union and Canada, has not yet been approved by the FDA and is supplied to the U.S. Strategic National Stockpile, or the SNS, as having fulfilled the requirements for the potential use following an EUA. There is no guarantee our Phase 3 trial of IMVAMUNE/IMVANEX will be successful or that the FDA will approve the vaccine for marketing.

IMVAMUNE/IMVANEX is currently approved for sale only in the European Union and Canada. IMVAMUNE/IMVANEX may never receive approval from the FDA. There are several factors that may impact our ability to continue to sell IMVAMUNE/IMVANEX to the U.S. government and in other jurisdictions where it is approved for sale or obtain regulatory approval from the FDA or other regulatory authorities. These factors include our ability to successfully complete the Phase 3 trial currently being conducted at a U.S. military garrison in South Korea and the successful development of the freeze dried formulation of IMVAMUNE/IMVANEX. Our failure to successfully complete the Phase 3 trial or successfully develop the freeze dried formulation may prevent us from achieving certain milestones and receiving certain milestone payments under our contracts with BARDA and may result in a decline in orders of IMVAMUNE/IMVANEX from the U.S. and other governments.

IMVAMUNE/IMVANEX or any of our product candidates for which we obtain marketing approval could be subject to post-marketing restrictions or withdrawal from the market, and we may be subject to substantial penalties if we fail to comply with regulatory requirements or experience unanticipated problems with our products following approval.

IMVAMUNE/IMVANEX or any of our product candidates for which we obtain marketing approval, as well as the manufacturing processes, post-approval studies and measures, labeling, advertising and promotional activities for such products, among other things, will be subject to continual requirements of and review by the EMA, FDA and other regulatory authorities. These requirements include submissions of safety and other post-marketing information and reports, registration and listing requirements, requirements relating to manufacturing, quality control, quality assurance and corresponding maintenance of records and documents, requirements regarding the distribution of samples to physicians and recordkeeping. Even if marketing approval of a product candidate is granted, the approval may be subject to limitations on the indicated uses for which the product may be marketed or to the conditions of approval, including the FDA requirement to implement a Risk Evaluation and Mitigation Strategy, if applicable, to ensure that the benefits of a drug or biological product outweigh its risks.

The EMA and FDA may also impose requirements for costly post-marketing studies or clinical trials and surveillance to monitor the safety or efficacy of a product, such as long term observational studies on natural exposure. The FDA and other agencies, including the Department of Justice, closely regulate and monitor the post-approval marketing and promotion of products to ensure that they are manufactured, marketed and distributed only for the approved indications and in accordance with the provisions of the approved labeling. The EMA and FDA impose stringent restrictions on manufacturers' communications regarding off-label use and if we do not market any of our product candidates for which we receive marketing approval for only their approved indications, we may be subject to warnings or enforcement action for off-label marketing. Violation of the Federal Food Drug and Cosmetic Act, and other statutes, including the False Claims Act, relating to the promotion and advertising of prescription drugs may lead to investigations or allegations of violations of federal and state health care fraud and abuse laws and state consumer protection laws.

Although we obtained a special protocol assessment from the FDA for our ongoing Phase 3 trial of PROSTVAC, a special protocol assessment does not guarantee any particular outcome from regulatory review, including any regulatory approval.

We have obtained an agreement with the FDA, following a special protocol assessment, or SPA, for the Phase 3 trial of PROSTVAC as monotherapy and in combination with GM-CSF for the

treatment of asymptomatic or minimally symptomatic mCRPC. The SPA process allows for FDA evaluation of a clinical trial protocol intended to form the primary basis of an efficacy claim in support of a Biologics License Application, or BLA. This provides a product sponsor with an agreement confirming that the design and size of a trial will be appropriate to form the primary basis of an efficacy claim for a BLA if the trial is performed according to the SPA and no substantial scientific issues essential to determining the safety or efficacy of the drug are identified after the testing has begun. Even if we believe that the data from a clinical trial are supportive, an SPA is not a guarantee of approval, and we cannot be certain that the design of, or data collected from, a trial will be adequate to demonstrate safety and efficacy, or otherwise be sufficient to support regulatory approval. There can be no assurance that the terms of an SPA will ultimately be binding on the FDA, and the FDA is not obligated to approve a BLA, even if the clinical outcome is positive. We can give no assurance that as clinical trials proceed or as part of a BLA review process, if any, the FDA will determine that a previously approved SPA is still valid.

Additionally, an SPA may be changed only with written agreement of the FDA and sponsor, and any further changes we may propose to the protocol will remain subject to the FDA's approval. The FDA may not agree to any such amendment and, even if they agree, they may request other amendments to the trial design that could require additional cost and time, as well as increase the degree of difficulty in reaching clinical endpoints. As a result, even with an SPA, we cannot be certain that the trial results will be found to be adequate to support an efficacy claim and product approval.

We selectively rely on third parties to conduct our clinical trials and perform data collection and analysis, which may result in costs and delays that prevent us from successfully commercializing our product candidates.

We currently, and expect to continue to, selectively rely on public and private research institutions, medical institutions, clinical investigators, CROs, contract laboratories and collaborators to conduct some of our early stage product development activities, perform data collection and analysis and to carry out our clinical trials. Our development activities or clinical trials conducted in reliance on third parties may be delayed, suspended or terminated if:

We generally do not have the ability to control the performance of third parties in their conduct of development activities. Third party performance failures may increase our development costs, delay our ability to obtain regulatory approval and delay or prevent the commercialization of our product candidates. While we believe that there are alternative sources to provide these services, in the event that we seek such alternative sources, we may not be able to enter into replacement arrangements without incurring delays or additional costs.

We face substantial competition from companies with considerably more resources and experience than we have, which may result in others discovering, developing, receiving approval for or commercializing products before or more successfully than us.

The pharmaceutical and biotechnology industries are highly competitive. Numerous laboratories, companies, institutions, universities and other research entities are actively involved in the discovery, research, development and marketing of vaccines to prevent infectious diseases and therapeutics to

treat cancer, making them highly competitive fields. We have competitors in each of the industry verticals in which we compete, many of which have substantially greater name recognition, commercial infrastructure and financial, technical and personnel resources than we have. Smaller or early stage companies may also prove to be significant competitors, particulary through collaborative arrangements with larger and established companies.

We compete in the areas of biodefense, commercial vaccines and treatments for infectious disease indications and immunotherapies for the treatment of cancer. Our vaccines and vaccine candidates are protected by intellectual property agreements that we own or license from third parties, and therefore are protected from competition as to the particular vaccines that we produce for the applicable indications that we target for the life of the applicable patent. However, many companies offer pharmaceutical products that may address one or more indications that our vaccines target. Other companies that compete for government contracts to develop, manufacture and commercialize vaccines for potential bioterror threats include, but are not limited to, AstraZeneca plc, Emergent BioSolutions, Inc., GlaxoSmithKline plc, Merck & Co., Inc., Pfenex Inc. and SIGA Technologies, Inc. Other companies that compete to develop, manufacture and commercialize vaccines for the prevention and treatment of infectious diseases include, but are not limited to, Johnson & Johnson, Dynavax Technologies Corporation, GenVec, Inc., Genocea Biosciences, Inc., Inovio Pharmaceuticals, Inc., Merck & Co. Inc., Novartis Pharma AG, Novavax, Inc. and Sanofi. Other companies that compete to develop, manufacture and commercialize immunotherapies for the treatment of cancer include, but are not limited to, Advaxis, Inc., Aduro Biotech, Inc., BMS, Celldex Therapeutics, Inc., Inovio Pharmaceuticals, Inc., Juno Therapeutics, Inc., Merck & Co. Inc., NEON Therapeutics, Novartis AG, Replimune Ltd and Transgene SA.

Competitors may develop novel vaccines or other technologies that could make our product candidates obsolete or uneconomical. Any of our product candidates that competes with an approved product may need to demonstrate compelling advantages in efficacy, convenience, tolerability and safety in order to be commercially successful. Any of our product candidates that are approved could also face other competitive factors in the future, including biosimilar competition, which could force us to lower prices or could result in reduced sales. Any failure to compete effectively against our current and future competitors could have a material adverse effect on our business and financial results.

Most of our immediately foreseeable future revenues are contingent upon grants and contracts from agencies of the U.S. government. We also contract with other governments and public authorities and there is a risk that political factors may have a material adverse effect on existing orders and our ability to enter into contracts and on the terms and conditions of such contracts.

Our contracts with the U.S. government are crucial to our earnings. In 2013 and 2014, revenue from agencies of the U.S. government accounted for 99.9% and 99.5%, respectively, of our total revenue, but accounted for 19.1% of our revenue for the first nine months of 2015. There is no guarantee that we will be able to enter into new agreements with the U.S. government or its agencies, or maintain existing agreements with the U.S. government or its agencies. Furthermore, our ability to maintain profitability under certain of our government contracts requires us to predict in advance the costs of development and supply of certain of our products and product candidates. For example, one of our contracts with BARDA is a cost-plus-fixed-fee contract that only reimburses certain specified activities that have been previously authorized by BARDA. There is no guarantee that additional activities will not be needed and, if so, that BARDA will reimburse us for these activities. Additionally, there are significant requirements associated with operating as a federal government contractor, which includes having appropriate accounting, project tracking and earned-

value management systems implemented and operational, and we may not be able to consistently meet these requirements. Performance under a BARDA contract requires that we comply with applicable regulations and operational mandates, which, among other things, requires us to engage internal and external expertise for compliance. Our ability to be regularly and fully reimbursed for our activities will depend on our ability to comply and demonstrate compliance with such requirements. A failure to renew or termination of our contracts with the U.S. government or its agencies would have a material adverse effect on our business and financial results.

In addition to our contracts with the U.S. government and its agencies, our contracting parties in a number of negotiations and agreements concerning IMVAMUNE/IMVANEX are other governments and public authorities. The supply of smallpox vaccines is considered by many governments to be a matter of national interest. As a result, we are subject to substantial political risks, partly in respect of the final decision as to the conclusion of agreements and partly in respect of the terms and conditions of such agreements. We seek to constantly keep in close contact, either through in-house or third-party representatives, with the governments and public authorities with which negotiations are taking place in order to gain better insight into decision-making patterns. However, changes in political dynamics in the United States or elsewhere could have a material adverse effect on our business and financial results.

All of our immediately foreseeable future revenues to support the development of IMVAMUNE/IMVANEX for the vaccination against smallpox are dependent upon our contracts with BARDA and other governmental agencies. Negotiation of such contracts and execution thereof are subject to numerous complexities and contingencies, the adverse outcome of which could harm our business and financial results.

Substantially all of our revenues that support the development of IMVAMUNE/IMVANEX for vaccination against smallpox have been derived from prior government grants and our current contracts with BARDA. Our contracts with BARDA are for the development of IMVAMUNE/IMVANEX for vaccination against smallpox in multiple forms. There can be no assurance that the FDA will ultimately accept in support of a BLA the experiments that we perform or agree that the results of these experiments support approval of IMVAMUNE/IMVANEX for vaccination against smallpox. There can be no assurances that this contract will continue, that BARDA will continue to purchase IMVAMUNE/IMVANEX under extensions of this contract, that any such extension would be on favorable terms, or that we will be able to enter into new contracts with the U.S. government to support our smallpox program. Changes in government budgets and agendas may result in a decreased and de-prioritized emphasis on supporting the development of IMVAMUNE/IMVANEX for vaccination against smallpox, which could negatively impact the revenues that may be generated from supplying our freeze dried formulation. In such event, BARDA is not required to continue funding for or to extend our existing contract. Any such reduction in our revenues from BARDA or any other government contract could materially adversely affect our financial condition and results of operations.

Additionally, U.S. government contracts typically contain provisions favorable to the government and are subject to periodic audit and modification by the government at its sole discretion, which will subject us to additional risks. For example, under our contracts with BARDA, the U.S. government has the power to unilaterally:

The U.S. government also has the right to terminate the BARDA contract if termination is in the government's interest, or if we default by failing to perform in accordance with the milestones set forth in the contract. Termination-for-convenience provisions generally enable us to recover only our costs incurred or committed (plus a portion of the agreed fee) and settlement expenses on the work completed prior to termination. Except for the amount of services received by the government, termination-for-default provisions do not permit recovery of fees. In addition, we must comply with numerous laws and regulations that affect how we conduct business with the U.S. government. Among the most significant government contracting regulations that affect our business are:

Therefore, negotiating and entering into arrangements with the U.S. government can be complex and time-consuming and may delay or alter our business development plans with respect to any specific products or product candidates.

Furthermore, we may be required to enter into agreements and subcontracts with third parties, including suppliers, consultants and other third-party contractors, in order to satisfy our contractual obligations pursuant to our agreements with the U.S. government. Negotiating and entering into such arrangements can be time-consuming and we may not be able to reach agreement with such third parties. Any such agreement must also be compliant with the terms of our government contract. Any delay or inability to enter into such arrangements or entering into such arrangements in a manner that is non-compliant with the terms of our contract, may result in violations of our contract. As a result of these provisions, we must undertake significant compliance activities. The diversion of resources from commercial programs to these compliance activities, as well as the exercise by the U.S. government of any rights under these provisions, could have a material adverse effect on our business and financial results.

Our business is subject to periodic audit by the U.S. government, including under our contracts with BARDA, and a negative audit could adversely affect our business.

U.S. government agencies, such as the Department of Health and Human Services, or HHS, routinely audit and investigate government contractors and recipients of federal grants, including our contracts with BARDA. These agencies review a contractor's performance under its contracts, cost structure and compliance with applicable laws, regulations and standards.

The HHS can also review the adequacy of, and a contractor's compliance with, its internal control systems and policies, including the contractor's purchasing, property, estimating, compensation and management information systems. Any costs found to be improperly allocated to a specific contract will not be reimbursed, while such costs already reimbursed must be refunded. If an audit uncovers improper or illegal activities, we may be subject to civil and criminal penalties and administrative sanctions, including:

In addition, we could suffer serious reputational harm if allegations of impropriety were made against us by the U.S. government, which could have a material adverse effect on our business and financial results.

Our research and development plans regarding PROSTVAC and our other cancer immunotherapy product candidates are to a large extent dependent upon our Cooperative Research and Development Agreements.

We conduct a large portion of our research and development for PROSTVAC and our other cancer immunotherapy product candidates under two Cooperative Research and Development Agreements, or CRADAs, we entered into with the NCI. We are obligated to make annual payments under each CRADA. In addition, although the CRADAs have five year terms, and our CRADA relating to the development of PROSTVAC has been extended for an additional five year term through August 2018, either party to the CRADAs has the right to terminate the CRADAs upon 60 days' notice to the other party. As a result, no assurance can be given that the NCI will not terminate either CRADA in the future and that the CRADAs will, therefore, remain in effect until we complete our desired research thereunder.

We manufacture clinical and commercial supplies or our product candidates at a single location. Any disruption at this facility could adversely affect our business and results of operations.

We own and operate a vaccine manufacturing facility in Kvistgaard, Denmark. We rely on this facility for the manufacture of clinical and commercial supply of all of our product candidates. If our facility were damaged or destroyed, or otherwise subject to disruption, it would require substantial lead-time to replace our manufacturing capabilities. In such event, we would be forced to identify and rely entirely on third-party contract manufacturers for an indefinite period of time. Any disruptions or delays at our facility or its failure to meet regulatory compliance would impair our ability to develop and commercialize our product candidates, which would adversely affect our business and results of operations.

Our product candidates are complex to manufacture, and we may encounter difficulties in production that could have a material adverse effect on our business and financial results.

Our products must be made consistently and in compliance with a clearly defined manufacturing process. Accordingly, it is essential to be able to validate and control the manufacturing process to assure that it is reproducible. Slight deviations anywhere in the manufacturing process, including obtaining materials, filling, labelling, packaging, storage and shipping and quality control and testing, some of which all pharmaceutical companies, including us, experience from time to time, may result in batch failures, delay in the release of batches, product recalls or spoilage. If microbial, viral or other contaminations are discovered in our product candidates or in the manufacturing facilities in which our product candidates are made, such manufacturing facilities may need to be closed for an extended period of time to investigate and remedy the contamination. Further, as product candidates are developed through preclinical to late stage clinical trials towards approval and commercialization, it is common that various aspects of the development program, such as manufacturing methods, are altered along the way in an effort to optimize processes and results. Such changes carry the risk that they will not achieve these intended objectives, and any of these changes could cause our product candidates to perform differently and affect the results of ongoing clinical trials or other future clinical trials. Any failure to manufacture products up to regulatory standards could lead to increased costs due to duplicative or replacement manufacturing, product recalls or a loss of reputation.

Our product candidates approved for commercial sale or used in late-stage clinical trials must be manufactured in accordance with cGMP regulations. These regulations govern manufacturing processes and procedures, including record keeping and the implementation and operation of quality systems to control and assure the quality of investigational products and products approved for sale. We and our collaborators must supply all necessary documentation in support of a new drug application or foreign equivalent on a timely basis and must adhere to cGMP requirements enforced by the EMA, the FDA and other regulatory agencies. If we or our collaborators fail to comply with cGMP, we could experience a disruption in the supply of our product candidates, which could delay or prevent regulatory approval or commercial launch of such candidates, which could have a material adverse effect on our business and financial results.

In addition, we may not be able to successfully increase the manufacturing capacity for any of our product candidates in a timely or cost-effective manner, or at all. In addition, quality issues may arise during scale-up activities. If we are unable to successfully scale up the manufacture of our product candidates in sufficient quality and quantity, the development and testing of that product candidate and regulatory approval or commercial launch of any resulting product may be delayed, which could have a material adverse effect on our business and financial results.

We rely on IDT Biologika to fill, finish and package IMVAMUNE/IMVANEX, and if IDT Biologika should fail to perform, our commercialization and development efforts for IMVAMUNE/IMVANEX could be delayed or stopped.

We rely on IDT Biologika to fill, finish and package IMVAMUNE/IMVANEX in the liquid frozen formulation prior to its distribution. Additionally, the freeze dried formulation of IMVAMUNE/IMVANEX is currently being developed and it is uncertain whether IDT Biologika will be willing to provide this service of producing this formulation in the quantities required or that IDT Biologika will be willing to provide this service on terms that are acceptable to us. If IDT Biologika is not capable or is unwilling to provide these services and we are unable to locate third parties to perform these functions on terms that are acceptable to us on a timely basis or at all, or if the third parties we identify fail to perform their obligations up to expected standards or at all, the progress of our clinical trials could be delayed or even suspended and the commercialization of IMVAMUNE/IMVANEX could be delayed or prevented, either of which would have a material adverse effect on our business and financial results.

Any changes in our suppliers' positions and their ability to supply the raw materials required by us may have an impact on our ability to fulfill customer contracts. There is a risk that our raw material suppliers may not always be able to deliver the raw materials used in our planned production.

A number of raw materials and sterile single-use devices are used to manufacture our product candidates. Some of the raw materials are general purpose materials used by other pharmaceutical manufacturers, while others are manufactured specifically for use by us, either because of special quality requirements, including in particular the specific pathogen-free eggs, or SPF eggs, used in production, or the packaging in which they are supplied, and certain products manufactured by Invitrogen Corporation. The sterile single-use devices are predominantly custom-made for the production of our product candidates.

To the extent possible, we aim to have at least two suppliers of critical raw materials. When this has not been possible, the aim is for the raw materials to be manufactured by an alternative supplier, at some delay, if the primary supplier should fail to deliver. If a primary supplier fails to deliver or delivers less of a critical raw material than agreed, it may take three to six months, or more, before an alternative supplier will be able to supply raw materials of the same quality. There is a risk that the required number of SPF eggs of the required quality may not always be available to meet our needs. Our supply of SPF eggs is more susceptible to disruption than the other consumables required for the production of our product candidates in that they cannot be stored to any significant extent. Additionally, certain of the supplies manufactured by Invitrogen Corporation are not currently available from other suppliers.

Consequently, supplier failure may cause production delays of three to six months, or more. Where possible, we seek to safeguard against this risk by maintaining large raw material inventories. However, there is still the risk that we will not be able to source important raw materials required for the production of our product candidates, which could have a material adverse effect on our business and financial results.

There is a risk that our products may have major side effects that may give rise to substantial liability claims.

As a biopharmaceutical company producing vaccines, we operate in a market that is subject to risk of liability. We may be subject to future liability claims alleging adverse effects from clinical trials

of our products. This risk of liability claims is significantly increased by concluding agreements for the supply of smallpox vaccines that remain to be completed or approved for use in humans. Any liability claims could have a material adverse effect on our business, financial position, results of operations and future growth prospects.

There is a risk that we may not be able to maintain insurance coverage, and that existing or any future insurance policies or our own resources will not sufficiently cover claims for damages that may be received in the future.

Our business exposes us to potential product liability and other liability risks that are inherent in clinical development, manufacturing, marketing and use of human therapeutic products. It is generally necessary for us to secure certain levels of insurance as a condition for the conduct of clinical trials and any sale or use of our products. We have taken out product liability insurance with respect to all clinical trials and ongoing trials performed to date for which we were responsible.

We may seek to expand our insurance coverage if the sales of IMVAMUNE/IMVANEX increase significantly, if we obtain marketing approval for any of the product candidates or if other risks related to our business increase. We may not be able to obtain or maintain adequate protection against potential liabilities at acceptable cost. If we are unable to obtain insurance or other protection against potential product liability claims, we could be exposed to significant liabilities, which may materially and adversely affect our business and financial position. These liabilities could prevent or interfere with our product development and commercialization efforts. If we are sued for any injury caused by our products or processes, our liability could exceed our product liability insurance coverage and our own financial resources, and consequently could have a material adverse effect on our business, financial position, results of operations and future growth prospects.

Our future success depends on our ability to retain our management team and key employees.

We are highly dependent on the management, development, clinical, financial and business development expertise of our management team and key employees. Recruiting and retaining qualified scientific and clinical personnel will also be critical to our success. The loss of the services of any of the members of our management team or key employees could impede the achievement of our development and commercialization objectives and seriously harm our ability to successfully implement our business strategy. Furthermore, replacing any of the members of our management team or key employees may be difficult and may take an extended period of time because of the limited number of individuals in our industry with the breadth of skills and experience required to successfully develop, gain regulatory approval for and commercialize drugs. Competition to hire from this limited pool is intense, and we may be unable to hire, train, retain or motivate the members of our management team or key employees on acceptable terms given the competition among numerous pharmaceutical and biotechnology companies for similar personnel. We also experience competition for the hiring of scientific and clinical personnel from universities and research institutions. If we are unable to continue to attract and retain high quality management and employees, our ability to pursue our growth strategy will be limited.

Government restrictions on pricing and reimbursement, as well as other healthcare payor cost-containment initiatives, may negatively impact our ability to generate revenues.

Sales of certain of our product candidates, if and when approved for marketing, will depend, in part, on the extent to which our products will be covered by third-party payors, such as government health care programs, commercial insurance and managed healthcare organizations. These third-

party payors are increasingly reducing reimbursements for medical products, drugs and services. Because coverage and reimbursement determinations are made on a payer-by-payer basis, obtaining coverage and adequate reimbursement from one payor does not guarantee that we will obtain similar coverage or reimbursement from another payor. In addition, government and other authorities have continued implementing cost containment programs, including price controls, restrictions on coverage and reimbursement, and requirements for substitution of generic products and/or biosimilars. Adoption of price controls and cost containment measures, and adoption of more restrictive policies in jurisdictions with existing controls and measures, could further limit our net revenue and results. Decreases in third-party reimbursement for our product candidates or a decision by a third-party payor not to cover our product candidates or provide only limited reimbursement for our product candidates could reduce physician usage of our products once approved and have a material adverse effect on our sales, results of operations and financial condition. Further, the adoption and implementation of any future governmental cost containment or other health reform initiative may result in additional downward pressure on the price that we may receive for any approved product.

We are subject to healthcare laws and regulations, which may require substantial compliance efforts and could expose us to criminal sanctions, civil penalties, contractual damages, reputational harm and diminished profits and future earnings, among other penalties.

Healthcare providers, such as physicians and others, will play a primary role in the recommendation and prescription of our products, if approved. Our arrangements with such persons and third-party payors and our general business operations will expose us to broadly applicable fraud and abuse and other healthcare laws and regulations that may constrain the business or financial arrangements and relationships through which we research, market, sell and distribute our products, if we obtain marketing approval. Restrictions under applicable U.S. federal, state and non-U.S. healthcare laws and regulations include, but are not limited to, the following:

Ensuring that our business arrangements with third parties comply with applicable healthcare laws and regulations will likely be costly. It is possible that governmental authorities will conclude that our business practices do not comply with current or future statutes, regulations or case law involving applicable fraud and abuse or other healthcare laws and regulations. If our operations were found to be in violation of any of these laws or any other governmental regulations that may apply to us, we may be subject to significant civil, criminal and administrative penalties, damages, fines, disgorgement, individual imprisonment, possible exclusion from government funded healthcare programs, such as Medicare and Medicaid, contractual damages, reputational harm, diminished profits and future earnings, and curtailment of our operations, any of which could substantially disrupt our operations. If the physicians or other providers or entities with whom we expect to do business are found not to be in compliance with applicable laws, they may be subject to criminal, civil or administrative sanctions, including exclusions from government funded healthcare programs.

Our employees and collaborators may engage in misconduct or other improper activities, including violating applicable regulatory standards and requirements or engaging in insider trading, which could significantly harm our business.

We are exposed to the risk of employee fraud or other misconduct and the fraud and misconduct of our collaborators. Misconduct by our employees or our collaborators could include intentional failures to comply with legal requirements or the requirements of CMMS, the EMA, the FDA and other government regulators, provide accurate information to applicable government authorities, comply with fraud and abuse and other healthcare laws and regulations in the United States, or similar laws in Denmark and elsewhere, report financial information or data accurately or disclose unauthorized activities to us. In particular, sales, marketing and business arrangements in the healthcare industry are subject to extensive laws and regulations intended to prevent fraud, misconduct, kickbacks, self-dealing and other abusive practices. These laws and regulations restrict or prohibit a wide range of pricing, discounting, marketing and promotion, sales commission, customer incentive programs and other business arrangements. Employee or collaborator misconduct could also involve the improper use of, including trading on, information obtained in the

course of clinical trials, which could result in regulatory sanctions and serious harm to our reputation. We have adopted a Code of Business Conduct and Ethics, but it is not always possible to identify and deter employee misconduct, and the precautions we take to detect and prevent this activity may be ineffective in controlling unknown or unmanaged risks or losses or in protecting us from governmental investigations or other actions or lawsuits stemming from a failure to comply with these laws or regulations. If any such actions are instituted against us, and we are not successful in defending ourselves or asserting our rights, those actions could have a significant impact on our business, including the imposition of significant fines or other sanctions.

Changes in Danish, U.S. or other foreign tax laws or compliance requirements, or the practical interpretation and administration thereof, could have a material adverse effect on our business, financial condition and results of operations.

We are affected by various Danish, U.S. and foreign taxes, including direct and indirect taxes imposed on our global activities, such as corporate income, withholding, customs, excise/energy, value added, environmental and other taxes. Significant judgment is required in determining our provisions for taxes and there are many transactions and calculations where the ultimate tax determination is uncertain.

In particular, we are contemplating seeking an advance pricing agreement procedure between Danish and U.S. tax authorities concerning the tax treatment of potential future revenue from PROSTVAC in order to establish a pre-agreed split of income thereon to be taxed in Denmark and the United States, respectively. Depending on whether we obtain an advance pricing agreement and depending on the split of income between Denmark and the United States determined therein, we could potentially face double taxation of our profits or a higher effective tax rate than expected.

Further, we also engage in a number of intra-group transactions between legal entities in different jurisdictions and, although we believe that we follow generally accepted transfer pricing practices, our interpretation may be challenged.

Should any of the risks described above materialize as a result of changes in Danish or foreign direct or indirect tax laws or compliance requirements, the practical interpretation and administration thereof, including in respect to market practices, or otherwise, it could have a material adverse effect on our business, financial condition and results of operations.

If we are unable to obtain or protect intellectual property rights related to our products and product candidates, we may not be able to compete effectively in our market.

We rely upon a combination of patents, trade secret protection and confidentiality agreements to protect the intellectual property related to our products and product candidates. The strength of patents in the biotechnology and pharmaceutical field involves complex legal and scientific questions and can be uncertain. The patent applications that we own or in-license may fail to result in issued patents with claims that cover the products in the United States or in other countries. If this were to occur, early biosimilar competition could be expected against IMVAMUNE/IMVANEX, PROSTVAC and other product candidates in development. There is no assurance that all of the potentially relevant prior art relating to our patents and patent applications has been found and cited in every patent office, which can invalidate a patent, prevent a patent from issuing based on a pending patent application, or limit our ability to assert a patent in the event of potential infringement by a third party. Even if patents do successfully issue, third parties may challenge their validity, enforceability, scope or ownership, which may result in such patents, or our rights to such patents, being narrowed or invalidated. Furthermore, even if they are unchallenged, our patents and patent applications may

not adequately protect our intellectual property or prevent others from designing around our claims. If the patent applications we hold or license with respect to IMVAMUNE/IMVANEX and PROSTVAC fail to issue or if their breadth or strength of protection is threatened, it could dissuade companies from collaborating with us to develop, and threaten our ability to commercialize, our products. We cannot offer any assurances about which, if any, patents will issue or whether any issued patents will be found not invalid and not unenforceable, will go unthreatened by third parties or will adequately protect our products and product candidates. Further, if we encounter delays in regulatory approvals, the period of time during which we could market IMVAMUNE/IMVANEX and PROSTVAC under patent protection could be reduced. Since patent applications in the United States and most other countries are confidential for a period of time after filing, and some remain so until issued, we cannot be certain that we or our licensors were the first to file any patent application related to IMVAMUNE/IMVANEX, PROSTVAC or our other product candidates. Furthermore, if third parties have filed such patent applications, an interference proceeding in the United States can be provoked by a third party or instituted by us to determine who was the first to invent any of the subject matter covered by the patent claims of our applications. An unfavorable outcome could require us to cease using the related technology or to attempt to license it from the prevailing party, which may not be possible.

In addition to the protection afforded by patents, we rely on trade secret protection and confidentiality agreements to protect proprietary know-how that is not patentable, processes for which patents are difficult to enforce and other elements of our drug discovery and development processes that involve proprietary know-how, information or technology that is not covered by patents. Although we expect all of our employees to assign their inventions to us, and all of our employees, consultants, advisors and any third parties who have access to our proprietary know-how, information or technology to enter into confidentiality agreements, we cannot provide any assurances that all such agreements have been duly executed, that such agreements provide adequate protection and will not be breached, that our trade secrets and other confidential proprietary information will not otherwise be disclosed or that competitors will not otherwise gain access to our trade secrets or independently develop substantially equivalent information and techniques. If we are unable to prevent material disclosure of the non-patented intellectual property related to our technologies to third parties, and there is no guarantee that we will have any such enforceable trade secret protection, we may not be able to establish or maintain a competitive advantage in our market, which could materially adversely affect our business, results of operations and financial condition.

Further, the laws of some countries do not protect patents and other proprietary rights to the same extent or in the same manner as the laws of the United States. As a result, we may encounter significant problems in protecting and defending our intellectual property abroad. We may also fail to pursue or obtain patents and other intellectual property protection relating to our products and product candidates in all countries.

Finally, certain of our activities and our licensors' activities have been funded, and may in the future be funded, by the U.S. federal government. When new technologies are developed with U.S. federal government funding, the government obtains certain rights in any resulting patents, including a nonexclusive license authorizing the government to use the invention for non-commercial purposes. These rights may permit the government to disclose our confidential information to third parties and to exercise "march-in" rights to use or allow third parties to use our patented technology. The government can exercise its march-in rights if it determines that action is necessary because we fail to achieve practical application of the U.S. government-funded technology, because action is necessary to alleviate health or safety needs, to meet requirements of federal regulations or to give preference to U.S. industry. In addition, U.S. government-funded inventions must be reported to the

government, U.S. government funding must be disclosed in any resulting patent applications, and our rights in such inventions may be subject to certain requirements to manufacture products in the United States.

Our ability to compete may decline if we do not adequately protect our proprietary rights.

Our commercial success depends on obtaining and maintaining proprietary rights to our product candidates and defending these rights against third-party challenges. We will only be able to protect our product candidates and their uses from unauthorized use by third parties to the extent that valid and enforceable patents, or effectively protected trade secrets, cover them. Our ability to obtain patent protection for our product candidates is uncertain due to a number of factors, including, but not limited to:

Even if we have or obtain patents covering our product candidates or compositions, we may still be barred from making, using and selling our product candidates or technologies because of the patent rights of others. Others may have filed, and in the future may file, patent applications covering compositions or products that are similar or identical to ours. There are many issued U.S., European and other national patents relating to vaccine and cancer immunotherapy products, and some of these relate to product candidates we intend to commercialize. Numerous U.S., European and other national issued patents and pending patent applications owned by others exist in the cancer treatment field in which we are developing products. These could materially affect our ability to develop our product candidates or sell our products if approved. Because patent applications can take many years to issue, there may be currently pending applications unknown to us that may later result in issued patents that our product candidates or compositions may infringe. These patent applications may have priority over patent applications filed by us.

Obtaining and maintaining a patent portfolio entails significant expense and resources. Part of the expense includes periodic maintenance fees, renewal fees, annuity fees, various other governmental fees on patents and/or applications due in several stages over the lifetime of patents and/or applications, as well as the cost associated with complying with numerous procedural provisions during the patent application process. We may not choose to pursue or maintain protection for particular inventions. In addition, there are situations in which failure to make certain payments or noncompliance with certain requirements in the patent process can result in abandonment or lapse of a patent or patent application, resulting in partial or complete loss of patent rights in the relevant jurisdiction. If we choose to forego patent protection or allow a patent application or patent to lapse purposefully or inadvertently, our competitive position could suffer.

Legal actions to enforce our patent rights can be expensive and may involve the diversion of significant management time. In addition, these legal actions could be unsuccessful and could also result in the invalidation of our patents or a finding that they are unenforceable. We may or may not choose to pursue litigation or other actions against those that have infringed on our patents, or used them without authorization, due to the associated expense and time commitment of monitoring these activities. If we fail to protect or to enforce our intellectual property rights successfully, our competitive position could suffer, which could harm our results of operations.

Issued patents covering our product candidates could be found invalid or unenforceable if challenged in court.

If we initiate legal proceedings against a third party to enforce a patent covering our product candidate or technology, the defendant could counterclaim that the patent covering our product candidate or technology is invalid or unenforceable. In patent litigation in the United States, and in many other countries, defendant counterclaims alleging invalidity and unenforceability are commonplace. Grounds for a validity challenge include alleged failures to meet any of several statutory requirements, including lack of novelty, obviousness (lack of inventive step) or non-enablement. Grounds for unenforceability assertions include allegations that someone connected with prosecution of the patent withheld relevant information from the U.S. Patent and Trademark Office, or USPTO, as well as with the European Patent Office, or made a misleading statement, during prosecution. Third parties may also raise similar claims before administrative bodies in the United States or abroad, even outside the context of litigation. Such mechanisms include re-examination, post-grant review and/or inter partes review and equivalent proceedings in non-U.S. jurisdictions, and opposition proceedings. Such proceedings could result in revocation or amendment of our patents in such a way that they no longer cover our product candidates or competitive products. The outcome following legal assertions of invalidity and unenforceability is unpredictable. With respect to validity, for example, we cannot be certain that there is no invalidating prior art, of which we or the patent examiner were unaware during prosecution. Further, we cannot be certain that all of the potentially relevant art relating to our patents and patent applications has been cited in every patent office. If a defendant were to prevail on a legal assertion of invalidity or unenforceability, we would lose at least part, and perhaps all, of the patent protection on our product candidates.

Biopharmaceutical patents and patent applications involve highly complex legal and factual questions, which, if determined adversely to us, could negatively impact our patent position.

The patent positions of biopharmaceutical companies can be highly uncertain and involve complex legal and factual questions. The interpretation and breadth of claims allowed in some patents covering biopharmaceutical compositions may be uncertain and difficult to determine, and are often affected materially by the facts and circumstances that pertain to the patented compositions and the related patent claims. The standards of the USPTO are evolving and could

change in the future. Consequently, we cannot predict the issuance and scope of patents with certainty. Patents, if issued, may be challenged, invalidated or circumvented. U.S. patents and patent applications may also be subject to interference proceedings, and U.S. patents may be subject to reexamination proceedings, post-grant review and/or inter partes review in the USPTO. Non-U.S. patents may also be subject to opposition or comparable proceedings in the corresponding patent office, which could result in either loss of the patent or denial of the patent application, or loss or reduction in the scope of one or more of the claims of the patent or patent application. In addition, such interference, reexamination, post-grant review, inter partes review and opposition proceedings may be costly. Accordingly, rights under any issued patents may not provide us with sufficient protection against competitive products or processes.

In addition, changes in or different interpretations of patent laws in the United States and other countries may permit others to use our or our licensors' discoveries or to develop and commercialize our technology and products without providing any compensation to us, or may limit the number of patents or claims we can obtain. The laws of some countries do not protect intellectual property rights to the same extent as U.S. laws and those countries may lack adequate rules and procedures for defending our intellectual property rights.

If we fail to obtain and maintain patent protection and trade secret protection for our product candidates, we could lose our competitive advantage and competition we face would increase, reducing any potential revenues and adversely affecting our ability to attain or maintain profitability.

From time to time, the U.S. Supreme Court, other federal courts, the U.S. Congress, the USPTO or similar authorities in other countries may change the standards of patentability and any such changes could have a negative impact on our business. In addition, the Leahy-Smith America Invents Act, or the America Invents Act, which was signed into law in 2011, includes a number of significant changes to U.S. patent law. These changes include a transition from a "first-to-invent" system to a "first inventor to file" system, changes to the way in which issued patents are challenged, and changes to the way in which patent applications are disputed during the examination process. These changes may favor larger and more established companies that have greater resources to devote to patent application filing and prosecution. The USPTO has developed new regulations and procedures to govern the full implementation of the America Invents Act, and many of the substantive changes to patent law associated with the America Invents Act, and, in particular, the first inventor to file provisions, became effective on March 16, 2013. Substantive changes to patent law associated with the America Invents Act, or any subsequent U.S. legislation regarding patents, may affect our ability to obtain patents, and if obtained, to enforce or defend them. Accordingly, it is not clear what, if any, impact the America Invents Act will have on the cost of prosecuting our U.S. patent applications, our ability to obtain U.S. patents based on our discoveries and our ability to enforce or defend any patents that may issue from our patent applications, all of which could have a material adverse effect on our business.

If we do not obtain protection under the Hatch-Waxman Amendments and similar non-U.S. legislation for extending the term of patents covering each of our product candidates, our business may be materially harmed.

Depending upon the timing, duration and conditions of FDA marketing approval of our product candidates, one or more of our U.S. patents may be eligible for limited patent term extension under the Drug Price Competition and Patent Term Restoration Act of 1984, referred to as the Hatch-Waxman Amendments, and similar legislation in the European Union. The Hatch-Waxman Amendments permit a patent term extension of up to five years for a patent covering an approved

product as compensation for effective patent term lost during product development and the FDA regulatory review process. However, we may not receive an extension if we fail to apply within applicable deadlines, fail to apply prior to expiration of relevant patents or otherwise fail to satisfy applicable requirements. Moreover, the length of the extension could be less than we request. If we are unable to obtain patent term extension or the term of any such extension is less than we request, the period during which we can enforce our patent rights for that product will be shortened and our competitors may obtain approval to market competing products sooner. As a result, our revenue from applicable products could be reduced, possibly materially.

If we are unable to protect the confidentiality of our trade secrets, our business and competitive position would be harmed.

In addition to patent protection, because we operate in the highly technical field of development of therapies, we rely in part on trade secret protection in order to protect our proprietary technology and processes. However, trade secrets are difficult to protect. We have entered into confidentiality and intellectual property assignment agreements with our employees, consultants, outside scientific collaborators, sponsored researchers and other advisors. These agreements generally require that the other party keep confidential and not disclose to third parties all confidential information developed by the party or made known to the party by us during the course of the party's relationship with us. These agreements also generally provide that inventions conceived by the party in the course of rendering services to us will be our exclusive property. However, these agreements may not be honored and may not effectively assign intellectual property rights to us.

In addition to contractual measures, we try to protect the confidential nature of our proprietary information using physical and technological security measures. Such measures may not, for example, in the case of misappropriation of a trade secret by an employee or third party with authorized access, provide adequate protection for our proprietary information. Our security measures may not prevent an employee or consultant from misappropriating our trade secrets and providing them to a competitor, and recourse we take against such misconduct may not provide an adequate remedy to protect our interests fully. Enforcing a claim that a party illegally disclosed or misappropriated a trade secret can be difficult, expensive and time-consuming, and the outcome is unpredictable. In addition, courts outside the United States may be less willing to protect trade secrets. Trade secrets may be independently developed by others in a manner that could prevent legal recourse by us. If any of our confidential or proprietary information, such as our trade secrets, were to be disclosed or misappropriated, or if any such information was independently developed by a competitor, our competitive position could be harmed.

We will not seek to protect our intellectual property rights in all jurisdictions throughout the world and we may not be able to adequately enforce our intellectual property rights even in the jurisdictions where we seek protection.

Filing, prosecuting and defending patents on our product candidates in all countries and jurisdictions throughout the world would be prohibitively expensive, and our intellectual property rights in some countries outside the United States could be less extensive than those in the United States, assuming that rights are obtained in the United States. Competitors may use our technologies in jurisdictions where we do not pursue and obtain patent protection to develop their own products and, further, may export otherwise infringing products to territories where we have patent protection, but enforcement is not as strong as that in the United States. These products may compete with our products and our patents or other intellectual property rights may not be effective or sufficient to prevent them from competing. Even if we pursue and obtain issued patents in particular jurisdictions, our patent claims or other intellectual property rights may not be effective or sufficient to prevent third parties from so competing.

In addition, the laws of some non-U.S. countries do not protect intellectual property rights to the same extent as the federal and state laws in the United States. Many companies have encountered significant problems in protecting and defending intellectual property rights in certain non-U.S. jurisdictions. The legal systems of some countries, particularly developing countries, do not favor the enforcement of patents and other intellectual property protection, especially those relating to biopharmaceuticals or biotechnologies. This could make it difficult for us to stop the infringement of our patents, if obtained, or the misappropriation of our other intellectual property rights. For example, many countries have compulsory licensing laws under which a patent owner must grant licenses to third parties. In addition, many countries limit the enforceability of patents against third parties, including government agencies or government contractors. In these countries, patents may provide limited or no benefit. Patent protection must ultimately be sought on a country-by-country basis, which is an expensive and time-consuming process with uncertain outcomes. Accordingly, we may choose not to seek patent protection in certain countries, and we will not have the benefit of patent protection in such countries.

Proceedings to enforce our patent rights in non-U.S. jurisdictions could result in substantial costs and divert our efforts and attention from other aspects of our business, could put our patents at risk of being invalidated or interpreted narrowly, could put our patent applications at risk of not issuing, and could provoke third parties to assert claims against us. We may not prevail in any lawsuits that we initiate and the damages or other remedies awarded, if any, may not be commercially meaningful. In addition, changes in the law and legal decisions by courts in the United States and other countries may affect our ability to obtain adequate protection for our technology and the enforcement of intellectual property. Accordingly, our efforts to enforce our intellectual property rights around the world may be inadequate to obtain a significant commercial advantage from the intellectual property that we develop or license.

Third parties may assert ownership or commercial rights to inventions we develop.

Third parties may in the future make claims challenging the inventorship or ownership of our intellectual property. We have written agreements with collaborators that provide for the ownership of intellectual property arising from our collaborations. These agreements provide that we must negotiate certain commercial rights with collaborators with respect to joint inventions or inventions made by our collaborators that arise from the results of the collaboration. In some instances, there may not be adequate written provisions to address clearly the resolution of intellectual property rights that may arise from collaboration. If we cannot successfully negotiate sufficient ownership and commercial rights to the inventions that result from our use of a third-party collaborator's materials where required, or if disputes otherwise arise with respect to the intellectual property developed with the use of a collaborator's samples, we may be limited in our ability to capitalize on the market potential of these inventions. In addition, we may face claims by third parties that our agreements with employees, contractors or consultants obligating them to assign intellectual property to us are ineffective, or in conflict with prior or competing contractual obligations of assignment, which could result in ownership disputes regarding intellectual property we have developed or will develop and interfere with our ability to capture the commercial value of such inventions. Litigation may be necessary to resolve an ownership dispute, and if we are not successful, we may be precluded from using certain intellectual property, or may lose our exclusive rights in that intellectual property. Either outcome could have an adverse impact on our business.

If we fail to comply with our obligations under license or technology agreements with third parties, or if our rights to develop and commercialize our product candidates are limited under license or technology agreements with third parties, we could lose license rights that are critical to our business.

We license intellectual property that is critical to our business, including licenses underlying the technology in our vaccine and cancer immunotherapy product candidates, and in the future we may enter into additional agreements that provide us with licenses to valuable intellectual property or technology. These licenses impose various royalty payments, milestones and other obligations on us. If we fail to comply with any of these obligations, the licensor may have the right to terminate the license. Termination by the licensor would cause us to lose valuable rights, and could prevent us from distributing our current tests, or inhibit our ability to commercialize future test candidates. Our business would suffer if any current or future licenses terminate, if the licensors fail to abide by the terms of the license, if the licensors fail to prevent infringement by third parties, if the licensed patents or other rights are found to be invalid or unenforceable, or if we are unable to enter into necessary licenses on acceptable terms.

Third parties may assert that our employees or consultants have wrongfully used or disclosed confidential information or misappropriated trade secrets.

We employ individuals who were previously employed at universities or other biotechnology or pharmaceutical companies, including our competitors or potential competitors. Although we try to ensure that our employees and consultants do not use the proprietary information or know-how of others in their work for us, and no such claims against us are currently pending, we may be subject to claims that we or our employees, consultants or independent contractors have used or disclosed intellectual property, including trade secrets or other proprietary information, of a former employer or other third parties. Litigation may be necessary to defend against these claims. If we fail in defending any such claims, in addition to paying monetary damages, we may lose valuable intellectual property rights or personnel. Even if we are successful in defending against such claims, litigation could result in substantial costs and be a distraction to management and other employees.

In addition, the research resulting in certain of our licensed patent rights and technology has been, and may in the future be, funded by the U.S. government. When new technologies are developed with U.S. government funding, the U.S. government generally obtains certain rights in any resulting patents and inventions, including a non-exclusive license to practice or have practiced on behalf of the U.S. government such patents and inventions. These rights may further permit the U.S. government to disclose our confidential information to third parties and to exercise march-in rights to allow third parties to use our licensed technology. The U.S. government can exercise its march-in rights if it determines that action is necessary because we or our licensors fail to achieve practical application of the U.S. government-funded technology, or because action is necessary to alleviate health or safety needs, to meet requirements of federal regulations or to give preference to U.S. industry. In addition, our rights in such inventions may be subject to certain requirements to manufacture products embodying such inventions in the United States. Any exercise by the U.S. government of such rights could harm our business, financial condition, results of operations and future growth prospects.

A dispute concerning the infringement or misappropriation of our proprietary rights or the proprietary rights of others could be time-consuming and costly, and an unfavorable outcome could harm our business.

There is significant litigation in the biopharmaceutical industry regarding patent and other intellectual property rights. While we are not currently subject to any pending intellectual property

litigation, and are not aware of any such threatened litigation, we may be exposed to future litigation by third parties based on claims that our product candidates, technologies or activities infringe the intellectual property rights of others. If our development activities are found to infringe any such patents, we may have to pay significant damages or seek licenses to such patents. A patentee could prevent us from using the patented drugs or compositions. We may need to resort to litigation to enforce a patent issued to us, to protect our trade secrets, or to determine the scope and validity of third-party proprietary rights. From time to time, we may hire scientific personnel or consultants formerly employed by other companies involved in one or more areas similar to the activities conducted by us. Either we or these individuals may be subject to allegations of trade secret misappropriation or other similar claims as a result of prior affiliations. If we become involved in litigation, it could consume a substantial portion of our managerial and financial resources, regardless of whether we win or lose. We may not be able to afford the costs of litigation. Any adverse ruling or perception of an adverse ruling in defending ourselves against these claims could have a negative impact on our cash position. Any legal action against us or our collaborators could lead to:

Any of these outcomes could hurt our cash position and financial condition and our ability to develop and commercialize our product candidates.

If our trademarks and trade names are not adequately protected, we may not be able to build name recognition in our markets of interest.

Our registered trademarks, including IMVAMUNE/IMVANEX, PROSTVAC and MVA-BN or unregistered trademarks or trade names may be challenged, infringed, circumvented or declared generic or determined to be infringing on other marks. We may not be able to protect our rights to these trademarks and trade names, which we will need to build name recognition by potential partners or customers in our markets of interest. Over the long term, if we are unable to establish name recognition based on our trademarks and trade names, we may not be able to compete effectively.

As a holder of our ADSs, you will not be treated as one of our shareholders and you will not have shareholder rights. Our depositary, Deutsche Bank Trust Company Americas, will be the holder of the shares underlying your ADSs. As a holder of ADSs, you will have contractual ADS holder rights. The deposit agreement among us, the depositary and you, as an ADS holder, and all other persons directly and indirectly holding ADSs sets out ADS holder rights as well as the rights and obligations of the depositary. ADS holders may only exercise voting rights with respect to the shares underlying their respective ADSs in accordance with the provisions of the deposit agreement, which provides that you may vote the shares underlying the ADSs for any particular matter to be voted on by our shareholders either by withdrawing the shares underlying the ADSs or, to the extent permitted by applicable law and as permitted by the depositary, by requesting a temporary registration as shareholder in our shares and authorizing the depositary to act as proxy. Voting instructions may be

given only in respect of a number of ADSs representing an integral number of shares or other deposited securities. At our 2016 annual general meeting, we intend to propose that our articles of association be amended to permit pass-through voting by ADS holders, who, assuming the success of such proposal, would thereafter be permitted to indicate their voting preference to the depositary in accordance with and subject to the depositary's procedures. Even if you are able to instruct the depositary to vote the shares underlying your ADSs, we cannot guarantee you that the depositary will vote in accordance with your instructions. Please see the risk factor entitled "You may not be able to exercise your right to vote the shares underlying the ADSs."

There has been no prior market for the ADSs on a U.S. national securities exchange and an active and liquid market for our securities may fail to develop, which could harm the market price of the ADSs.

Prior to this offering, while our shares have been traded on Nasdaq Copenhagen since November 1998 and we have ADSs that trade on the U.S. over-the-counter market, there has been no public market on a U.S. national securities exchange for our ADSs or our shares. Although we have applied to list our ADSs on The NASDAQ Global Select Market, an active trading market for our ADSs may never develop or be sustained following this offering. The offering price of our ADSs will be based on the market price for our shares on Nasdaq Copenhagen at the time of this offering. This offering price may not be indicative of the market price of our ADSs or shares after this offering. In the absence of an active trading market for our ADSs or shares, investors may not be able to sell their ADSs at or above the offering price or at the time that they would like to sell.

The trading price of our equity securities may be volatile, and purchasers of our ADSs could incur substantial losses.

The market prices of our ADSs and shares may be volatile. The stock market in general and the market for biopharmaceutical companies in particular have experienced extreme volatility that has often been unrelated to the operating performance of particular companies. As a result of this volatility, investors may not be able to sell their ADSs or shares at or above the price originally paid for the security. The market price for our ADSs and shares may be influenced by many factors, including, but not limited to:

These and other market and industry factors may cause the market price and demand for our ADSs to fluctuate substantially, regardless of our actual operating performance, which may limit or prevent investors from readily selling their shares or ADSs and may otherwise negatively affect the liquidity of the trading market for ADSs.

We have broad discretion over the use of the net proceeds from this offering and may use them in ways with which you do not agree and in ways that may not increase the value of your investment.

Our board of directors and management will have broad discretion over the application of the net proceeds that we receive from this offering. We may spend or invest these proceeds in a way with which our shareholders and holders of ADSs disagree. Failure by our management to apply these funds effectively could harm our business and financial condition. Pending their use, we may invest the net proceeds from this offering in a manner that does not produce income or that loses value. These investments may not yield a favorable return to our investors.

If securities or industry analysts do not publish research or publish inaccurate or unfavorable research about our business, the price of the ADSs and their trading volume could decline.

The trading market for the ADSs and shares depends in part on the research and reports that securities or industry analysts publish about us or our business. If no or few securities or industry analysts cover our company, the trading price for the ADSs would be negatively impacted. If one or more of the analysts who covers us downgrades our equity securities or publishes inaccurate or unfavorable research about our business, the price of ADSs would likely decline. If one or more of these analysts ceases coverage of our company or fails to publish reports on us regularly, or downgrades our securities, demand for ADSs could decrease, which could cause the price of the ADSs or their trading volume to decline.

We intend to retain all available funds and any future earnings and, consequently, your ability to achieve a return on your investment will depend on appreciation in the price of the ADSs.

We have never declared or paid any cash dividends on our shares, and we intend to retain all available funds and any future earnings to fund the development and expansion of our business. Therefore, you are not likely to receive any dividends on your ADSs for the foreseeable future and the success of an investment in ADSs will depend upon any future appreciation in its value. Consequently, investors may need to sell all or part of their holdings of ADSs after price appreciation, which may never occur, as the only way to realize any future gains on their investment. There is no guarantee that the ADSs will appreciate in value or even maintain the price at which our shareholders have purchased them. Investors seeking cash dividends should not purchase the ADSs or shares.

In addition, exchange rate fluctuations may affect the amount of DKK that we are able to distribute, and the amount in U.S. dollars that our shareholders receive upon the payment of cash

dividends or other distributions we declare and pay in DKK, if any. Additionally, dividends will generally be subject to Danish withholding tax. See the section of this prospectus titled "Certain Material Danish Income Tax Consequences" for a more detailed description of Danish taxes on dividends. These factors could harm the value of the ADSs.

ADS investors may also not realize all of the benefits of being a shareholder in our company. For instance, the votes of ADS holders will not be represented directly on the books of the company, but only through a vote by the depositary of the underlying shares, which vote will reflect the ADS majority's election on the vote of all such shares. Please see the risk factor entitled "You may not be able to exercise your right to vote the shares underlying the ADSs." Separately, the Company may elect to offer subscription rights to its shareholders without offering such rights to ADS holders. Please see the risk factor entitled "Holders of our ADSs may not be able to exercise the pre-emptive subscription rights related to the shares that they represent, and may suffer dilution of their equity holding in the event of future issuances of our shares."

Investors in this offering will experience immediate and substantial dilution in the book value of their investment.

The initial public offering price of the ADSs is substantially higher than the pro forma net tangible book value per ADS before giving effect to this offering. Accordingly, if you invest in the ADSs in this offering, you will incur immediate substantial dilution of approximately DKK per ADS ($ ) (based on the net tangible book value per share underlying the ADSs), based on an assumed initial public offering price of $ per ADS (DKK ), and our pro forma net tangible book value as of September 30, 2015. In addition, following this offering, investors in this offering will have contributed approximately % of the total gross consideration paid by shareholders to purchase our outstanding shares and ADSs, but will only own ADSs representing approximately % of our shares and ADSs outstanding after this offering. Furthermore, if the underwriters exercise their option to purchase additional ADSs, if board authorizations to issue additional shares, or ADSs or outstanding warrants or convertible securities are issued and subsequently exercised, you could experience further dilution. For a further description of the dilution that you will experience immediately after this offering, see the section of this prospectus titled "Dilution."

Investors should be aware that the rights provided to our shareholders and holders of ADSs under Danish corporate law and our articles of association differ in certain respects from the rights that you would typically enjoy as a shareholder of a U.S. company under applicable U.S. federal and state laws.

Under Danish corporate law, except in certain limited circumstances, which require at a minimum that a proposal for inspection has been supported by a minimum of 25% of the shareholders voting and being present at a general meeting, our shareholders may not ask for an inspection of our corporate records, while under Delaware corporate law any shareholder, irrespective of the size of such shareholder's shareholdings, may do so. Shareholders of a Danish limited liability company are also unable to initiate a derivative action, a remedy typically available to shareholders of U.S. companies, in order to enforce a right of our company, in case we fail to enforce such right ourselves, other than in certain cases of board member/management liability under limited circumstances. In addition, a majority of our shareholders may release a member of our board of directors or our executive management from any claim of liability we may have, including if such board member or manager has acted in bad faith or has breached his or her duty of loyalty. However, a shareholder may bring a derivative action on behalf of our Company against, among other persons, a member of our board of directors or our executive management, provided that the circumstances of the act or omission giving rise to the claim of liability were not known to

the shareholders at the time of such shareholder resolution, or if shareholders representing at least 10% of the share capital represented at the relevant general meeting has opposed such shareholder resolution. In contrast, most U.S. federal and state laws prohibit a company or its shareholders from releasing a board member from liability altogether if such board member has acted in bad faith or has breached such board member's duty of loyalty to our company. Additionally, distribution of dividends from Danish companies to foreign companies and individuals can be subject to non-refundable withholding tax, and not all receiving countries allow for deduction. See the section of this prospectus titled "Certain Material Danish Income Tax Consequences" for a more detailed description of the withholding tax. Also, the rights as a creditor may not be as strong under Danish insolvency law as under U.S. law or other insolvency law, and consequently creditors may recover less in the event our company is subject to insolvency compared to a similar case including a U.S. debtor. In addition, the use of the tax asset consisting of the accumulated tax losses requires that we are able to generate positive taxable income and the use of tax losses carried forward to offset against future income is subject to certain restrictions and can be restricted further by future amendments to Danish tax law. Finally, Danish corporate law may not provide appraisal rights in the case of a business combination equivalent to those generally afforded a shareholder of a U.S. company under applicable U.S. laws. For additional information on these and other aspects of Danish corporate law and our articles of association, see the section herein entitled "Description of Share Capital." As a result of these differences between Danish corporate law and our articles of association, on the one hand, and U.S. federal and state laws, on the other hand, in certain instances, you could receive less protection as an equity holder of our company than you would as a shareholder of a U.S. company.

You may not be able to exercise your right to vote the shares underlying your ADSs.

Absent said withdrawal or, to the extent permitted by applicable law and as permitted by the depositary, temporary registration and proxy, Danish law prevents the depositary from differentiated voting at our general meetings unless our articles of association specifically allow for this, which is currently not the case, meaning that all votes on the shares held by the depositary, including those underlying the ADSs issued in this offering, would need to be cast either in favor or against any proposal at our general meetings, if such shares were voted at all. Our board of directors is committed to using reasonable efforts to work towards removing this restriction at our 2016 annual general meeting. If this restriction is removed, the depositary would be able to vote the shares registered in its name that underlie the ADSs to more closely reflect the preferences of the ADS holders, thereby effectively permitting pass-through voting by ADS holders who indicate their preference to the depositary in accordance with and subject to the depositary's procedures.

In such an instance, if we ask for your instructions, the depositary, upon timely notice from us, will notify you of the upcoming vote and arrange to deliver our voting materials to you. We cannot guarantee that you will receive the voting materials in time to ensure that you can instruct the depositary to vote your shares or to withdraw your shares so that you can vote them yourself. If the

depositary does not receive timely voting instructions from you, it may give a proxy to a person designated by us to vote the shares underlying your ADSs. Voting instructions may be given only in respect of a number of ADSs representing an integral number of shares or other deposited securities. In addition, the depositary and its agents are not responsible for failing to carry out voting instructions or for the manner of carrying out voting instructions. This means that you may not be able to exercise any right to vote that you may have with respect to the underlying shares, and there may be nothing you can do if the shares underlying your ADSs are not voted as you requested. In addition, the depositary is only required to notify you of any particular vote if it receives notice from us at least 30 days in advance of the scheduled meeting. Our articles of association permits, in the case of general meetings, and requires, in the case of extraordinary meetings, notice to be delivered within a shorter time span, in which case the depositary would not be required to provide you with notice of and access to such vote.

You may be subject to limitations on the transfer of your ADSs and the withdrawal of the underlying shares.

Your ADSs, which may be evidenced by ADRs, are transferable on the books of the depositary. However, the depositary may close its books at any time or from time to time when it deems expedient in connection with the performance of its duties. The depositary may refuse to deliver, transfer or register transfers of your ADSs generally when our books or the books of the depositary are closed, or at any time if we or the depositary think it is advisable to do so because of any requirement of law, government or governmental body, or under any provision of the deposit agreement, or for any other reason subject to your right to cancel your ADSs and withdraw the underlying shares. Temporary delays in the cancellation of your ADSs and withdrawal of the underlying shares may arise because the depositary has closed its transfer books or we have closed our transfer books, the transfer of shares is blocked to permit voting at a shareholders' meeting or we are paying a dividend on our shares. In addition, you may not be able to cancel your ADSs and withdraw the underlying shares when you owe money for fees, taxes and similar charges and when it is necessary to prohibit withdrawals in order to comply with any laws or governmental regulations that apply to ADSs or to the withdrawal of shares or other deposited securities. See the section of this prospectus titled "Description of American Depositary Shares."

We are incorporated under the laws of Denmark. Substantially all of our assets are located outside of the United States. The majority of our board members and employees reside outside of the United States. As a result, it may not be possible for investors to effect service of process within the United States upon such persons or to enforce against them or us in U.S. courts, including judgments predicated upon the civil liability provisions of the U.S. securities laws.

The United States and Denmark currently do not have a treaty providing for the reciprocal recognition and enforcement of judgments (other than arbitration awards) in civil and commercial matters. Consequently, a final judgment for payment given by a U.S. court, whether or not predicated solely upon U.S. securities laws, would not be enforceable in Denmark.

In order to obtain a judgment that is enforceable in Denmark, the party in whose favor a final and conclusive judgment of the U.S. court has been rendered will be required to file its claim again with a court of competent jurisdiction in Denmark. The Danish court will not be bound by the judgment by the U.S. court, but the judgement may be submitted as evidence. It is up to the Danish court to assess the judgment by the U.S. court and decide if and to what extent the judgment should be followed.

Danish courts are likely to deny claims for punitive damages and may grant a reduced amount of damages compared to U.S. courts.

Based on the lack of a treaty as described above, U.S. investors may not be able to enforce against us or members of our board of directors or our executive management, or certain experts named herein who are residents of Denmark or countries other than the United States any judgments obtained in U.S. courts in civil and commercial matters, including judgments under the U.S. federal securities laws.

As a foreign private issuer, we are exempt from a number of rules under the U.S. securities laws and are permitted to file less information with the SEC than a U.S. company. This may limit the information available to holders of ADSs.

We are a foreign private issuer, as defined in the SEC's rules and regulations, and, consequently, we are not subject to all of the disclosure requirements applicable to public companies organized within the United States. For example, we are exempt from certain rules under the Exchange Act that regulate disclosure obligations and procedural requirements related to the solicitation of proxies, consents or authorizations applicable to a security registered under the Exchange Act, including the U.S. proxy rules under Section 14 of the Exchange Act. In addition, our officers and directors are exempt from the reporting and "short-swing" profit recovery provisions of Section 16 of the Exchange Act and related rules with respect to their purchases and sales of our securities. Moreover, while we currently publish annual and quarterly reports on our website pursuant to the rules of Nasdaq Copenhagen and expect to file such financial reports on an annual and quarterly basis with the SEC, we will not be required to file such reports with the SEC as frequently or as promptly as U.S. public companies and will not be required to file quarterly reports on Form 10-Q or current reports on Form 8-K that a domestic company would be required to file under the Exchange Act. Accordingly, there may be less publicly available information concerning our company than there would be if we were not a foreign private issuer.

As a foreign private issuer and as permitted by the listing requirements of The NASDAQ Global Select Market, we will rely on certain home country corporate governance practices rather than the corporate governance requirements of The NASDAQ Global Select Market.

We qualify as a foreign private issuer. As a result, in accordance with the listing requirements of The NASDAQ Global Select Market, we will rely on home country governance requirements and certain exemptions thereunder rather than relying on the corporate governance requirements of The NASDAQ Global Select Market. For instance, the Listing Rules for the NASDAQ Stock Market, or the NASDAQ Listing Rules, for domestic U.S. issuers require listed companies to have, among other things, a majority of their board members be independent, and to have independent director oversight of executive compensation, nomination of board members and corporate governance matters. However, as a foreign private issuer, while we intend to comply with these requirements, we are permitted to follow home country practice in lieu of the above requirements. Danish law does not require that a majority of our board consist of independent directors or the implementation of a nominating and corporate governance committee, and our board may thus in the future not include, or include fewer, independent directors than would be required if we were subject to the NASDAQ Listing Rules, or they may decide that it is in our interest not to have a compensation committee or nominating and corporate governance committee, or have such committees governed by practices that would not comply with the NASDAQ Listing Rules. We intend to follow home country practice with regard to, among other things, quorum requirements generally applicable to general meetings of shareholders. Danish law does not have a regulatory regime for the solicitation of proxies and the solicitation of proxies is not a generally accepted business practice in Denmark, thus our practice will vary from the requirement of NASDAQ Listing Rule 5620(b). In addition, our shareholders have

authorized our board of directors to issue securities, including in connection with certain events such as the acquisition of shares or assets of another company, the establishment of or amendments to equity-based compensation plans for employees, rights issues at or below market price, certain private placements, directed issues at or above market price, and issuance of convertible notes. To this extent, our practice varies from the requirements of NASDAQ Rule 5635, which generally requires an issuer to obtain shareholder approval for the issuance of securities in connection with such events. For an overview of our corporate governance principles, see "Description of Share Capital." Accordingly, you may not have the same protections afforded to shareholders of companies that are subject to these NASDAQ requirements.

U.S. holders of ADSs may suffer adverse tax consequences if we are characterized as a passive foreign investment company.

Generally, if, for any taxable year, at least 75% of our gross income is passive income, or at least 50% of the value of our assets is attributable to assets that produce passive income or are held for the production of passive income, including cash, we would be characterized as a passive foreign investment company, or PFIC, for U.S. federal income tax purposes. For purposes of these tests, passive income includes dividends, interest, and gains from the sale or exchange of investment property and rents and royalties other than rents and royalties which are received from unrelated parties in connection with the active conduct of a trade or business. If we are characterized as a PFIC, U.S. holders of the ADSs may suffer adverse tax consequences, including having gains realized on the sale of the ADSs treated as ordinary income, rather than capital gain, the loss of the preferential rate applicable to dividends received on the ADSs by individuals who are U.S. holders, and having interest charges apply to distributions by us and the proceeds of sales of the ADSs. See "Certain Material U.S. Federal Income Tax Considerations—Passive Foreign Investment Company Considerations."

Our status as a PFIC will depend on the composition of our income and the composition and value of our assets, which may be determined in large part by reference to the market value of the ADSs and our shares, which may be volatile, from time to time. Our status may also depend, in part, on how quickly we utilize the cash proceeds from this offering in our business. Based on certain estimates of our gross income and assets, and on the nature of our business, we do not expect to be characterized as a PFIC for our taxable year ending December 31, 2015. However, there can be no assurance that we will not be considered a PFIC for any taxable year.

We must maintain effective internal control over financial reporting, and if we are unable to do so, the accuracy and timeliness of our financial reporting may be adversely affected, which could hurt our business, lessen investor confidence and depress the market price of our securities.

We must maintain effective internal control over financial reporting in order to accurately and timely report our results of operations and financial condition. In addition, as a public company listed in the United States, the Sarbanes-Oxley Act will require, among other things, that we assess the effectiveness of our internal control over financial reporting at the end of each fiscal year. We anticipate being first required to issue management's annual report on internal control over financial reporting, pursuant to Section 404 of the Sarbanes-Oxley Act, in connection with issuing our consolidated financial statements as of and for the year ending December 31, 2016.

The rules governing the standards that must be met for our management to assess our internal control over financial reporting pursuant to Section 404 of the Sarbanes-Oxley Act are complex and require significant documentation, testing and possible remediation. These stringent standards require that our audit committee be advised and regularly updated regarding management's review

of internal control over financial reporting. We have started the process of designing, implementing and testing the internal control over financial reporting required to comply with this obligation. This process is time-consuming, costly and complicated. In addition, our independent registered public accounting firm will be required to attest to the effectiveness of our internal controls over financial reporting beginning with our annual report following the date on which we are no longer an "emerging growth company," which may be up to five fiscal years following the date of this offering. Our management may not be able to effectively and timely implement controls and procedures that adequately respond to the increased regulatory compliance and reporting requirements that will be applicable to us as a public company listed in the United States. If we fail to staff our accounting and finance function adequately or maintain internal control over financial reporting adequate to meet the demands that will be placed upon us as a public company listed in the United States, our business and reputation may be harmed and the price of our ADSs may decline. Furthermore, investor perceptions of us may be adversely affected, which could cause a decline in the market price of our securities.

Holders of our ADSs will not be able to exercise the pre-emptive subscription rights related to the shares that they represent, and may suffer dilution of their equity holding in the event of future issuances of our shares.

Under the Danish Companies Act, our shareholders benefit from a pre-emptive subscription right on the issuance of shares for cash consideration only and not in the event of issuance of shares against non-cash contribution or debt conversion. Shareholders' pre-emptive subscription rights, in the event of issuances of shares against cash payment, may be disapplied by a resolution of the shareholders at a general meeting of our shareholders and/or the shares may be issued on the basis of an authorization granted to the board of directors pursuant to which the board may disapply the shareholders' pre-emptive subscription rights. Such shares may be issued at or above market value or below market value in the case of rights issues or pursuant to a resolution of the shareholders. The absence of pre-emptive rights for existing equity holders may cause dilution to such holders.

Furthermore, our ADS holders would not be entitled, even if such rights accrued to our shareholders in any given instance, to receive such pre-emptive subscription rights related to the shares that they represent. Rather, the depositary is required to endeavor to sell any such subscription rights that may accrue to the shares underlying the ADSs and to remit the net proceeds therefrom to the ADS holders pro rata. In addition, if the depositary is unable to sell rights, the depositary will allow the rights to lapse, in which case you will receive no value for these rights. Further, if we offer holders of our shares the option to receive dividends in either cash or shares, under the deposit agreement, ADS holders will not be permitted to elect to receive dividends in shares or cash, but will receive whichever option we provide as a default to shareholders who fail to make such an election.

This prospectus contains forward-looking statements concerning our business, operations and financial performance and condition, as well as our plans, objectives and expectations for our business operations and financial performance and condition. Any statements contained herein that are not statements of historical facts may be deemed to be forward-looking statements. In some cases, you can identify forward-looking statements by terminology such as "aim," "anticipate," "assume," "believe," "contemplate," "continue," "could," "due," "estimate," "expect," "goal," "intend," "may," "objective," "plan," "predict," "potential," "positioned," "seek," "should," "target," "will," "would," and other similar expressions that are predictions of or indicate future events and future trends, or the negative of these terms or other comparable terminology. These forward-looking statements include, but are not limited to, statements about:

These forward-looking statements are based on management's current expectations, estimates, forecasts and projections about our business and the industry in which we operate and management's beliefs and assumptions, and are not guarantees of future performance or development and involve known and unknown risks, uncertainties and other factors that are in some cases beyond our control. As a result, any or all of our forward-looking statements in this prospectus may turn out to be inaccurate. Factors that may cause actual results to differ materially from current expectations include, among other things, those listed under "Risk Factors" and elsewhere in this prospectus. Potential investors are urged to consider these factors carefully in evaluating the forward-looking statements. These forward-looking statements speak only as of the date of this prospectus. Except as required by law, we assume no obligation to update or revise these forward-looking statements for any reason, even if new information becomes available in the future. You should, however, review the factors and risks we describe in the reports we will file from time to time with the SEC after the date of this prospectus. See "Where You Can Find More Information."

This prospectus contains estimates, projections and other information concerning our industry, our business, and the markets for our product and product candidates. Information that is based on estimates, forecasts, projections, market research or similar methodologies is inherently subject to uncertainties, and actual events or circumstances may differ materially from events and circumstances that are assumed in this information. Unless otherwise expressly stated, we obtained this industry, business, market and other data from our own internal estimates and research as well as from reports, research surveys, studies and similar data prepared by market research firms and other third parties, industry, medical and general publications, government data and similar sources.

In addition, assumptions and estimates of our and our industry's future performance are necessarily subject to a high degree of uncertainty and risk due to a variety of factors, including those described in "Risk Factors." These and other factors could cause our future performance to differ materially from our assumptions and estimates. See "Special Note Regarding Forward-Looking Statements."

We estimate that the net proceeds from the sale of ADSs in this offering will be approximately $ (DKK ), after deducting the underwriting commission and estimated offering expenses payable by us, based on an assumed initial public offering price of $ per ADS (DKK ), the U.S. dollar equivalent of the closing price of our shares on Nasdaq Copenhagen on , 2016 of DKK , at the U.S. dollar/DKK exchange rate of as of , 2016 and an ADS-to-share ratio of 3:1. If the underwriters exercise their option to purchase additional ADSs in full, we estimate that the net proceeds to us from this offering will be approximately $ (DKK ), after deducting the underwriting commission and estimated offering expenses payable by us. Each $ (DKK ) increase (decrease) in the assumed initial public offering price of $ per ADS (DKK ), would increase (decrease) the net proceeds to us from this offering, after deducting the underwriting commission and estimated offering expenses payable by us, by $ (DKK ), assuming that the number of ADSs offered by us, as set forth on the cover page of this prospectus, remains the same. We may also increase or decrease the number of ADSs we are offering. An increase (decrease) of in the number of ADSs we are offering would increase (decrease) the net proceeds to us from this offering, after deducting the underwriting commission and estimated offering expenses payable by us, by $ (DKK ), assuming the assumed initial public offering price stays the same.

We intend to use the net proceeds from this offering, together with our existing cash resources, to accelerate our commercial vaccine pipeline as it relates to infectious disease and cancer immunotherapy, including specifically:

By applying the net proceeds of this offering in the manner set forth above, we believe that we will be able to advance our clinical testing of MVA-BN RSV through ; advance our clinical testing of CV 301 through and of MVA-BN Brachyury through ; and advance certain other preclinical programs in our infectious disease and cancer immunotherapy portfolio through Phase 1 clinical trials. Due to the uncertainties inherent in the clinical development and regulatory approval process, it is difficult to estimate with certainty the exact amounts of the net proceeds from this offering that may be used for any of the above purposes on a stand-alone basis. See "Risk Factors—We have broad discretion in the use of the net proceeds from this offering and may use them in ways with which you do not agree and in ways that may not increase the value of your investment."

Pending our application of the net proceeds from this offering, we plan to invest such proceeds in bank accounts and/or securities of limited duration.

We have never declared or paid cash dividends on our share capital. We intend to retain all available funds and any future earnings to fund the development and expansion of our business. Any future determination related to dividend policy will be made at the discretion of our board of directors. To understand how any future determination by our company as to our dividend policy would affect you as a holder of ADSs, please see the section of this Prospectus entitled "Description of American Depositary Shares—Dividends and Other Distributions."

The following table sets forth our capitalization and cash and cash equivalents as of September 30, 2015:

Actual data as of September 30, 2015 in the table below is derived from our unaudited condensed consolidated interim financial statements. The pro forma data included in the table below is also unaudited. You should read this information together with our unaudited condensed consolidated interim financial statements appearing elsewhere in this prospectus and the information set forth under the headings "Selected Consolidated Financial Data," "Use of Proceeds" and "Management's Discussion and Analysis of Financial Condition and Results of Operations."

If you invest in the ADSs in this offering, your interest will be immediately diluted to the extent of the difference between the initial public offering price per ADS in this offering and the net tangible book value per ADS after this offering. Dilution results from the fact that the initial public offering price per ADS is substantially in excess of the net tangible book value per ADS. As of September 30, 2015, we had a historical net tangible book value per ADS of $ (DKK ), or DKK per share ($ ). Our net tangible book value per share represents total consolidated tangible assets less total consolidated liabilities, all divided by the number of shares outstanding on September 30, 2015.

After giving effect to the sale of ADSs in this offering at an assumed initial public offering price of $ per ADS (DKK ), the U.S. dollar equivalent of the closing price of our shares on Nasdaq Copenhagen on , 2016 of DKK , at the U.S. dollar/DKK exchange rate of as of , 2016 and an ADS-to-share ratio of 3:1, and after deducting the underwriting commission and estimated offering expenses, our pro forma net tangible book value at September 30, 2015 would have been $ (DKK ) per share, or $ per ADS (DKK ). This represents an immediate increase in pro forma net tangible book value of $ (DKK ) per share to existing shareholders and an immediate dilution of $ per ADS (DKK ) to new investors. The following table illustrates this dilution per ADS:

A $ increase (DKK ) (decrease) in the assumed initial public offering price of $ per ADS (DKK ), the U.S. dollar equivalent of the closing price of our shares on Nasdaq Copenhagen on , 2016 of DKK , at the U.S. dollar/DKK exchange rate of as of , 2016 and an ADS-to-share ratio of 3:1, would increase (decrease) our pro forma net tangible book value as of September 30, 2015 after this offering by approximately DKK per share ($ ), or $ per ADS (DKK ), and would increase (decrease) dilution to investors in this offering by $ per ADS (DKK ), assuming that the number of ADSs offered by us, as set forth on the cover page of this prospectus, remains the same, after deducting the underwriting commission and estimated offering expenses payable by us. We may also increase or decrease the number of ADSs we are offering. An increase (decrease) of in the number of ADSs we are offering would increase (decrease) our pro forma net tangible book value as of September 30, 2015 after this offering by approximately DKK per share ($ ), or approximately $ per ADS (DKK ), and would decrease (increase) dilution to investors in this offering by approximately $ per ADS (DKK ), assuming the assumed initial public offering price per ADS remains the same, after deducting the underwriting commission and estimated offering expenses payable by us. The pro forma information is illustrative only, and we will adjust this information based on the actual initial public offering price and other terms of this offering

determined at pricing. If the underwriters fully exercise their option to purchase additional ADSs, pro forma net tangible book value after this offering would increase to approximately $ per ADS (DKK ), and there would be an immediate dilution of approximately $ per ADS (DKK ) to new investors.

We may choose to raise additional capital due to market conditions or strategic considerations even if we believe we have sufficient funds for our current or future operating plans. To the extent that we raise additional capital through the sale of equity or convertible debt securities, the issuance of these securities could result in further dilution to our equity holders.

The following table shows, as of December 31, 2015, on a pro forma basis, the number of ADSs purchased from us, the total consideration paid to us and the average price paid per share by existing shareholders and by new investors purchasing ADSs in this offering at an assumed initial public offering price of $ per ADS (DKK ), the U.S. dollar equivalent of the closing price of our shares on Nasdaq Copenhagen on , 2016 of DKK , at the U.S. dollar/DKK exchange rate of as of , 2016 and an ADS-to-share ratio of 3:1, before deducting the underwriting commission and estimated offering expenses payable by us (in thousands, except share and per share amounts and percentages):

The number of shares and ADSs to be outstanding after this offering is based on the number of shares outstanding as of December 31, 2015, and excludes up to 1,624,605 shares that may be issued upon the exercise of outstanding warrants, and assumes no exercise of the underwriters' option to purchase up to additional ADSs.

Our business is primarily conducted in Denmark, and we maintain our books and records in Danish kroner. We have presented results of operations in Danish kroner. We have also presented select financial information in U.S. dollars for your convenience in the sections entitled "Summary Consolidated Financial Data," "Selected Consolidated Financial Data," "Management's Discussion and Analysis of Results of Operations" and in certain other sections of this prospectus. On September 30, 2015, the exchange rate was DKK 6.66 per 1.00 U.S. dollar. On December 31, 2015, the exchange rate was DKK 6.8300 per 1.00 U.S. dollar. For the convenience of the reader, this prospectus also includes other translations from DKK to U.S. dollars and U.S. dollars to DKK. Unless specified as of a specific date, or otherwise indicated, translations from DKK to U.S. dollars and from U.S. dollars to DKK were made at the rate of DKK 6.66 per 1.00 U.S. dollar, the official exchange rate quoted as of September 30, 2015 by Danmarks Nationalbank. Such U.S. dollar amounts are not necessarily indicative of the amounts of U.S. dollars that could actually have been purchased upon exchange of DKK at the dates indicated. The rates set forth below are provided solely for your convenience and may differ from the actual rates used in the preparation of our consolidated financial statements and other financial data included in this prospectus.

The following table presents information on the exchange rates between the DKK and the U.S. dollar for the periods indicated, as published by Danmarks Nationalbank:

The following tables present selected consolidated financial data for our business.

We derived the selected consolidated income statements data for the years ended December 31, 2014 and 2013 and the selected consolidated statement of financial position data as of December 31, 2014 from our audited consolidated financial statements included elsewhere in this prospectus. We derived the selected consolidated income statements data for the nine months ended September 30, 2015 and 2014 and the selected consolidated statement of financial position data as of September 30, 2015 from our unaudited condensed consolidated interim financial statements included elsewhere in this prospectus.

MANAGEMENT'S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND
RESULTS OF OPERATIONS

You should read the following discussion and analysis of our financial condition and results of operations together with our financial statements and the related notes and other financial information included elsewhere in this prospectus. The following discussion is based on our financial information prepared in accordance with IFRS as issued by the IASB, which might differ in material respects from accounting principles generally accepted in other jurisdictions, including accounting principles generally accepted in the United States. Some of the information contained in this discussion and analysis or set forth elsewhere in this prospectus, including information with respect to our plans and strategy for our business, includes forward-looking statements that involve risks and uncertainties. You should review the "Risk Factors" section of this prospectus for a discussion of important factors that could cause actual results to differ materially from the results described in or implied by the forward-looking statements contained in the following discussion and analysis. All currency translations are provided solely for convenience into U.S. dollars at an assumed exchange rate of DKK 6.66 per 1.00 U.S. dollar, which was the exchange rate of such currencies as of September 30, 2015.

We are a fully integrated biotechnology company developing, manufacturing and commercializing novel vaccines for the prevention of life-threatening infectious diseases and the treatment of cancer. We focus on diseases for which the unmet medical need is high and for which we can harness the power of the immune system to induce a response. Our live virus vaccine platform has generated one commercial product for smallpox, one Phase 3 immunotherapy candidate for prostate cancer, one Phase 3 candidate for Ebola and several other clinical programs in the areas of infectious disease and oncology. We recognized revenue of $182 million in 2013 (DKK 1,213 million) and $183 million in 2014 (DKK 1,217 million) primarily from sales of our commercial smallpox vaccine, IMVAMUNE/IMVANEX. This revenue has enabled us to invest significant capital into research and development activities, the expansion of our production infrastructure and the advancement of our clinical pipeline.

Our expertise in vaccine design and production has led to a 10+ year relationship with the U.S. government pursuant to which we have been awarded approximately $1.2 billion in contracts. To date, we have recognized more than $900 million of revenue from these contracts. We have also established commercial relationships with Bristol-Myers Squibb, BMS, for the commercialization of PROSTVAC our Phase 3 cancer immunotherapy candidate, and with the Janssen Pharmaceutical Companies of Johnson & Johnson, or Janssen, for our Ebola vaccine candidate and additional infectious disease targets, including human papillomavirus. Our numerous contracts with governmental entities and pharmaceutical companies may generally be classified as either:

In 2014, we generated revenues of DKK 1,217 million ($183 million) and earnings before interest and taxes, or EBIT, of DKK 17 million ($3 million). 2014 represented the third year in a row with revenues in excess of DKK 1,000 million ($150 million) and the second year in a row with positive EBIT. In the first nine months of 2015, we generated DKK 703 million ($106 million) in

revenues and EBIT of DKK 2 million ($0.3 million). As of September 30, 2015, we had cash and cash equivalents of DKK 462 million ($69 million). In addition, we held investments in securities of DKK 772 million ($116 million). We also maintained credit lines of DKK 393 million ($59 million) as of such date, of which DKK 384 million ($58 million) was undrawn.

Revenue comprises the fair value of the consideration received or receivable for sales of goods and income derived from development services, including sale of delivered development services under the IMVAMUNE/IMVANEX development project with BARDA. Revenue is measured net of value added tax, duties, etc. collected on behalf of a third party and discounts. The revenue is recognized when it is probable that future economic benefits will flow to us and these benefits can be measured reliably, and when any significant risks and rewards of ownership of the goods or right to the services are transferred and we no longer retain managerial responsibility for, or control of, the goods or services sold.

Agreements with commercial partners generally include non-refundable upfront license and collaboration fees, milestone payments, the receipt of which is dependent upon the achievement of certain clinical, regulatory or commercial milestones, as well as royalties on product sales of licensed products, if and when such product sales occur, and revenue from the supply of products. For these agreements that include multiple elements, total contract consideration is attributed to separately identifiable components on a reliable basis that reasonably reflects the selling prices that might be expected to be achieved in stand-alone transactions, provided that each component has value to the partner on a stand-alone basis. The allocated consideration is recognized as revenue in accordance with the principles described above.

Sales of goods and licenses that transfer the rights associated with ownership of an intangible asset are recognized at a point in time when control is transferred. Revenue from development services and licenses that do not transfer the right of ownership to an intangible asset are recognized over time in line with the execution and delivery of the work.

If multiple components are not separable, they are combined into a single component and recognized over the period during which we are actively involved in development and deliver significant services to the collaboration partner.

Since 2007, we have been awarded four significant supply contracts with a total value of more than $950 million. Two contracts in 2007 and 2013 were awarded by BARDA for the delivery of 28 million doses of liquid frozen IMVAMUNE/IMVANEX to the U.S. Strategic National Stockpile, or SNS. A third contract from BARDA was awarded in July 2015 under which we intend to produce and deliver IMVAMUNE/IMVANEX bulk product. The fourth significant supply contract is with Janssen for the delivery of MVA-BN Filo bulk product equivalent of approximately 2 million doses of our Ebola vaccine.

Prior to 2015, we have generated substantially all of our revenue from sales of IMVAMUNE/IMVANEX and the remainder from development contracts with the U.S. government. Revenue associated with the delivery of 28 million doses of liquid frozen IMVAMUNE/IMVANEX was recognized as revenue from 2010 through January 2015.

In 2014, our revenue from sales of IMVAMUNE/IMVANEX was DKK 1,024 million ($154 million). In January 2015, we completed the delivery of the 8 million doses of IMVAMUNE/IMVANEX to the U.S. government, pursuant to which we recognized the final tranche of revenue under the contract for liquid frozen IMVAMUNE/IMVANEX.

For the nine months ended September 30, 2015, we generated revenue of DKK 78 million ($12 million) from sales of IMVAMUNE/IMVANEX. Decreased sales of IMVAMUNE/IMVANEX in the nine months ended September 30, 2015 versus the same period in 2014 reflects the transition of IMVAMUNE/IMVANEX from a liquid frozen formulation to a freeze dried formulation. Currently, we are finalizing the validation of the freeze drying production of IMVAMUNE/IMVANEX. In 2016, we expect IMVAMUNE/IMVANEX revenue to increase over 2015 as we expect to initiate bulk production of IMVAMUNE/IMVANEX that could transition into the freeze dried formulation. The IMVAMUNE/IMVANEX bulk product contract is expected to be recognized as revenue in 2016 and the beginning of 2017 as the bulk product is delivered.

In October 2014, we entered into an arrangement with Janssen with respect to the MVA-BN Filo vaccine. The Janssen arrangement consisted of a license contract valued at $45 million, a supply contract valued at $99 million and a $43 million equity investment by Johnson & Johnson Development Corporation. The increase of our share capital and proceeds from the equity investment with Johnson & Johnson Development Corporation were reflected in our consolidated statement of financial position as of December 31, 2014.

Under the license arrangement, we received $25 million as an upfront payment, which was recognized as a prepayment from customers in our statement of financial position as of December 31, 2014 and, of which $23 million will be recognized as revenue on a pro rata basis as we deliver the MVA-BN Filo bulk product and $2 million will be recognized as project income. The remaining $20 million will be paid based on the achievement of certain milestones. These milestone payments will be recognized as revenue when milestones are achieved.

Under the supply agreement, we received a prepayment of $35 million, which was recognized as a prepayment from customers in the statement of financial position as of December 31, 2014. In January 2015, we received another prepayment of $36 million from customers. The two prepayments will be recognized as revenue on a pro rata basis as we deliver MVA-BN Filo bulk product. The remaining $28 million under the supply contract will be invoiced and revenue recognized pro rata as we deliver MVA-BN Filo bulk product.

All deliveries of MVA-BN Filo to Janssen under the current supply contract are expected to be completed in 2015, pursuant to which we expect to recognize all of the related revenue under the contract for MVA-BN Filo. Therefore, our revenue in 2015 has been and will be driven by the reduced delivery of IMVAMUNE/IMVANEX to the U.S. government and increased delivery of MVA-BN Filo to Janssen.

For the nine months ended September 30, 2015, we generated revenue of DKK 519 million ($78 million) from sales of MVA-BN Filo bulk product.

In September 2015, we announced the award of a subcontract from Janssen, valued at $9 million. This is part of a contract awarded to Janssen by BARDA to support the advanced development and production of the Ebola prime-boost vaccine regimen. The five-year base subcontract covers studies to improve the production process and establish long-term storage of the MVA-BN Filo bulk vaccine. The contract also includes options for an additional $24 million to

implement process development activities for the formulation of a final drug product with a longer shelf life.

In December 2015, we entered into an additional licensing and collaboration agreement with Janssen. Pursuant to the agreement, we will receive an initial upfront payment of $9 million as well as potential future payments upon reaching development and commercial milestones, together with the upfront payment, totaling up to $171 million. We are also eligible to receive single-digit tiered royalties on future product sales. The initial upfront payment under this agreement is expected to be received and revenue recognized in 2016.

In March 2015, we entered into an Option and License Agreement with BMS under which we can receive up to $975 million in upfront and milestone payments. The agreement includes the following payments:

We received the upfront option grant payment of $60 million, which was recognized as a prepayment from customers in our statement of financial position as of September 30, 2015 and will be recognized as revenue if and when BMS exercises the option (or if the option expires unexercised). Upon any such exercise of the option by BMS, the PROSTVAC license and any associated trial information to date will effectively transfer to BMS without any restrictions. Accordingly, we will recognize as revenue the option exercise and license payments. As BMS and we have agreed that we will complete the PROSPECT trial, a portion of the payment will be allocated to the completion of the PROSPECT trial if BMS exercises its option before the PROSPECT trial is completed. Upon completion of the PROSPECT trial, we will recognize as revenue the Phase 3 completion milestone payments. Regulatory and sales milestone payments will be recognized as revenue when relevant milestones are achieved.

The National Cancer Institute (NCI) has rights to 10% of the upfront option payment of $60 million, which has been paid as of September 30, 2015, as well as 10% of the option exercise and license payment of $80 million, if and when BMS exercises the option.

If our ongoing development efforts are successful, we would expect to generate revenue from sales of additional products and milestone payments, development payments and royalties on sales of products that we license to third parties.

We maintain a production facility in Kvistgaard, Denmark. During the nine months ended September 30, 2015, we produced at such facility IMVAMUNE/IMVANEX, Ebola vaccines, clinical batches to support future trials and collaborations, while also preparing the PROSTVAC production

process for commercial launch. Production costs consist of costs incurred in generating the revenue for the year. Costs for raw materials, consumables, production staff and a proportion of production overhead, including maintenance, depreciation and impairment of tangible assets used in production as well as operation, administration and management of the production facility are recognized as production costs. In addition, the costs related to excess capacity and write-down to net realizable value of goods on stock are recognized.

The primary production costs that we incur are cost of goods sold for IMVAMUNE/IMVANEX and MVA-BN Filo and costs related to sale of contract work.

Research and development costs include salaries and costs directly attributable to our research and development projects, less government grants. Furthermore, salaries and costs supporting direct research and development, including costs of patents, rent, leasing and depreciation attributable to laboratories, and external scientific consultancy services, are recognized under research and development costs. Contract research costs incurred to achieve revenue are recognized under production costs. Research costs are expensed in the year they occur.

Development costs are generally expensed in the year they occur. Capitalization of development costs does not begin until it is deemed realistic that the product can be completed and marketed, and it is highly likely that a marketing authorization will be received. In addition, there must be sufficient certainty that the future earnings to us will cover not only production costs, direct distribution and administrative costs, but also the development costs.

However, we have met the criteria to capitalize the development costs attributable to the development of IMVAMUNE/IMVANEX, as the IMVAMUNE/IMVANEX contract with the U.S. government initially comprised the delivery of 20 million doses and an option to buy additional doses. For this reason, capitalization of the development costs attributable to this development project began at the date of regulatory approval of the clinical trial.

Capitalized development costs regarding the registration of IMVAMUNE/IMVANEX contract with the U.S. government are expensed (amortized) and recognized in the income statement under research and development costs when the related income on delivery of the development results have been earned and recognized as revenue. When the development has been completed and IMVAMUNE/IMVANEX has been approved by the U.S. Food and Drug Administration, or the FDA, the remaining carrying amount will be amortized in concurrence with the delivery of doses over the expected economic life of the asset.

Grants that compensate us for research and development expenses incurred, which are recognized directly in the income statement, are set off against the costs of research and development at the time when a final and binding right to the grant has been obtained.

The above stated accounting policies require that we split our research and development spending into three categories:

The successful development of our product candidates is highly uncertain. We believe that significant investment in product development is a competitive necessity and plan to continue these investments in order to be in a position to realize the potential of our product candidates. We cannot reasonably estimate or know the nature, timing and projected costs of the efforts that will be necessary to complete the remainder of the development of, or the period, if any, in which material net cash flows may commence from any of our product candidates in development. This is due to the numerous risks and uncertainties associated with developing drugs, including the uncertainty of:

A change in the outcome of any of these variables with respect to the development of a product candidate could mean a significant change in the costs and timing associated with the development of that product candidate.

We expect that the magnitude of any increase in our research and development spending will be dependent upon such factors as the results from our ongoing preclinical studies and clinical trials, the size, structure and duration of any follow on clinical program that we may initiate, and the cost associated with producing our product candidates on a large scale basis for later stage clinical trials. Furthermore, if the FDA, the European Medicine Agency or other regulatory authority were to require us to conduct clinical trials beyond those which we currently anticipate will be required for the completion of the clinical development of a product candidate, or if we experience significant delays in enrollment in any of our clinical trials, we could be required to expend significant additional financial resources and time on the completion of clinical development.

Our total annual research and development spending, including amounts that have been capitalized, was DKK 556 million in 2013 and DKK 572 million ($86 million) in 2014. During 2013 and 2014, we were conducting three Phase 3 trials: two regarding IMVAMUNE/IMVANEX for U.S. approval and one regarding PROSTVAC for U.S. and EU approval. We are currently experiencing declining costs for these three Phase 3 trials. However, we expect to continue to invest in developing our pipeline. In the coming years, we expect that the majority of our research and

development spending will be related to our other earlier stage candidates, CV 301 and MVA-BN RSV.

Distribution costs include costs incurred for distribution of goods sold and sales campaigns, including costs for sales and distribution personnel, advertising costs and depreciation and amortization of property, plant and equipment and intangible assets used in the distribution process. We expect that our distribution costs will increase as we add personnel to support the increased scale of our operations.

Administrative costs include costs of company management, staff functions, administrative personnel, office costs, rent, lease payments and depreciation not relating specifically to production, research and development activities or distribution costs. We expect that our administrative costs will increase as we add personnel to support the increased scale of our operations and become subject to certain reporting obligations under the U.S. securities laws.

Financial income includes interest income from bank and deposit contracts, interest income and positive fair value adjustments of financial instruments and securities, and net foreign exchange gains (including foreign exchange differences arising from intercompany balances). Financial expenses includes interest expenses on debt, net negative value adjustments of financial instruments and securities, net foreign exchange losses (including foreign exchange differences arising from intercompany balances), and adjustments of the net present value of provisions.

Financial Results for the Nine Months Ended September 30, 2015 Compared to the Nine Months Ended September 30, 2014

Revenue generated for the nine months ended September 30, 2015 was DKK 703 million ($106 million) compared to DKK 676 million for the nine months ended September 30, 2014. This increase was due to increased revenue from product sales, which totalled DKK 597 million ($90 million) for the nine months ended September 30, 2015 compared to DKK 576 million for the nine months ended September 30, 2014, and higher revenue from contract work in the amount of DKK 107 million ($16 million) for the nine months ended September 30, 2015 compared to DKK 99 million for the nine months ended September 30, 2014.

Revenue from product sales of DKK 597 million ($90 million) for the nine months ended September 30, 2015 was generated from the sale of MVA-BN Filo Bulk Drug Substance to Janssen in the amount of DKK 519 million ($78 million), the sale of the last 276,000 doses of IMVAMUNE/IMVANEX under the 8 million dose order from the U.S. government in the amount of DKK 49 million ($7 million), and the sale of IMVAMUNE/IMVANEX to other customers in the amount of DKK 29 million ($4 million). Revenue from product sale of DKK 576 million for the nine months ended September 30, 2014 was generated from the sale of 3.7 million doses of IMVAMUNE/IMVANEX under the 8 million dose order from U.S. government.

Production costs for the nine months ended September 30, 2015 were DKK 246 million ($37 million) compared to DKK 328 million for the nine months ended September 30, 2014. Costs related directly to revenue for the nine months ended September 30, 2015 were DKK 199 million ($30 million) compared to DKK 322 million for the nine months ended September 30, 2014. In 2014 we produced and sold final drug product (in vials), whereas in 2015, we produced and sold bulk drug substance, which generated fewer costs. Other production costs for the nine months ended September 30, 2015 were DKK 47 million ($7 million) compared to DKK 6 million for the nine months ended September 30, 2014. This increase was primarily due to a higher scrap, or unusable materials, related to the production of bulk material.

The research and development spending is separated into three different categories. Research and development costs related to the development of IMVAMUNE/IMVANEX for regulatory approval in the United States is capitalized. Research and development costs performed as part of revenue generating contracts with the U.S. government is shown under production costs as contract costs. All other research and development costs are shown as research and development costs.

The research and development spending for the nine months ended September 30, 2015 and 2014 are shown in the table below:

The total research and development spending for the nine months ended September 30, 2015 was DKK 297 million ($45 million) compared to DKK 314 million for the nine months ended

September 30, 2014. As part of our growth strategy, research and development functions were centralized during the first half of 2015 and, as a result, headcount has been reduced by approximately 40 employees.

Research and development costs shown under production costs were DKK 56 million ($8 million) for the nine months ended September 30, 2015, which were broadly in line with the DKK 51 million for the nine months ended September 30, 2014. The capitalized development costs related to IMVAMUNE/IMVANEX for regulatory approval in the United States were relatively high during the nine months ended September 30, 2014 since the Company enrolled for the Phase 3 trial during 2014. The expensing (amortization) of costs attributable to the IMVAMUNE/IMVANEX development project was relatively low during the nine months ended September 30, 2015 as only 276,000 doses were delivered to the U.S. Government compared to 3.7 million doses during the nine months ended September 30, 2014.

Distribution costs amounted to DKK 33 million ($5 million) for the nine months ended September 30, 2015, which were in line with the DKK 34 million for the nine months ended September 30, 2014.

Administrative costs totalled DKK 125 million ($19 million) for the nine months ended September 30, 2015, which were in line with the DKK 121 million for the nine months ended September 30, 2014.

Financial income for the nine months ended September 30, 2015 was DKK 79 million ($12 million) compared to DKK 40 million for the nine months ended September 30, 2014. The increase was due to gains on foreign exchange primarily related to an intercompany loan in U.S. dollars from our parent company to our U.S. subsidiary in California. An increase in the U.S. dollars/DKK rate will result in an unrealized foreign exchange gain as our parent company will have a larger outstanding receivable from the loan when converted to DKK while our U.S. subsidiary will have an unchanged debt in U.S. dollars.

Financial expenses totalled DKK 21 million ($3 million) for the nine months ended September 30, 2015 compared to DKK 3 million for the nine months ended September 30, 2014. The increase was due to unrealized revaluation losses on our securities of DKK 19 million ($3 million).

Tax for the nine months ended September 30, 2015 was DKK 3 million ($1 million) corresponding to an effective tax rate of 5.6%. The low effective tax rate was primarily due to an intercompany transaction that results in a tax deductible expenditure for Bavarian Nordic A/S and is taxable income in Bavarian Nordic, Inc. But since the taxable income in Bavarian Nordic, Inc. can be offset with previously non-recognized tax losses carry forward, the net impact at the group level is a tax income leading to a low effective tax rate for the nine month period ended September 30, 2015.

Tax for the nine months ended September 30, 2014 was a benefit of DKK 13 million corresponding to an effective tax rate of 15%. The low rate was due to non-recognized deferred tax asset on the period's loss in Bavarian Nordic, Inc. Inclusion of Bavarian Nordic, Inc.'s loss would have increased the negative tax amount and raised the effective tax rate.

Financial Results for the Year Ended December 31, 2014 Compared to the Year Ended December 31, 2013

Revenue for the year ended December 31, 2014 was DKK 1,217 million ($183 million) compared to revenue of DKK 1,213 million for the year ended December 31, 2013. The revenue in 2014 was comprised of deliveries of IMVAMUNE/IMVANEX to the SNS in the amount of DKK 1,018 million, revenue from our ongoing development contract with the U.S. government in the amount of DKK 193 million and sales of IMVAMUNE/IMVANEX to other customers in the amount of DKK 6 million. The revenue in 2013 was comprised of revenue from IMVAMUNE/IMVANEX delivered to the SNS of DKK 839 million and revenue related to contract work, including sale of development results, of DKK 373 million.

Production costs amounted to DKK 495 million ($74 million) for the year ended December 31, 2014 compared to DKK 485 million for the year ended December 31, 2013. Costs related directly to revenue for the year ended December 31, 2014 amounted to DKK 503 million ($76 million) compared to DKK 433 million for the year ended December 31, 2013. This increase is related to the higher product sale. Other production costs totaled DKK (8) million ($ (1) million) for the year ended December 31, 2014 compared to DKK 51 million for the year ended December 31, 2013. This decrease in other production costs was due to a very successful production performance with reversal of write-downs of DKK 12 million ($2 million) in 2014, and a provision made for scrap of products in 2013, which did not materialize in 2014.

Our principal research and development costs for the years ended December 31, 2014 and 2013 are shown in the following table:

The total research and development spending for the year ended December 31, 2014 was DKK 572 million ($86 million), including contract costs recognized as production costs as well as capitalized development costs, compared to research and development costs of DKK 556 million for the year ended December 31, 2013. The increase was primarily related to the development of PROSTVAC. Costs related to the development of PROSTVAC for the year ended December 31, 2014 were DKK 279 million ($42 million) compared to costs of DKK 181 million for the year ended December 31, 2013. We amortized DKK 46 million ($7 million) related to the ongoing IMVAMUNE/IMVANEX development project for the year ended December 31, 2014 compared to DKK 148 million for the year ended December 31, 2013. The decrease is explained below.

Research and development costs shown under production costs were DKK 92 million ($14 million) for the year ended December 31, 2014 compared to DKK 105 million for the year ended December 31, 2013.

Our capitalized research and development costs related to IMVAMUNE/IMVANEX for regulatory approval in the United States were DKK 47 million ($7 million) for the year ended December 31, 2014 compared to DKK 102 million for the year ended December 31, 2013. This decrease was due to the 4,000 subject Phase 3 trial for IMVAMUNE/IMVANEX, which was enrolled in 2013 and as to which we incurred most of the cost in 2013 as compared to 2014. The amortized research and development costs related to IMVAMUNE/IMVANEX for regulatory approval in the United States decreased by DKK 103 million ($15 million). This decrease was due to the amortization in 2013, during which all doses delivered to the U.S. government to that date were amortized. The amortization was linked to the number of doses delivered annually. However, when the amortization started—upon award of the 8 million dose order—all doses delivered under the 20 million dose order were amortized.

The distribution costs were DKK 45 million ($7 million) for the year ended December 31, 2014 compared to DKK 41 million for the year ended December 31, 2013. The increase was due to increased commercial activities after the approval of IMVAMUNE/IMVANEX in the European Union and Canada.

Administrative costs were DKK 181 million ($27 million) for the year ended December 31, 2014 compared to DKK 157 million for the year ended December 31, 2013. This increase was due to increased costs for consultants and lawyers.

Financial income for the year ended December 31, 2014 was DKK 57 million ($9 million), compared to DKK 7 million for the year ended December 31, 2013. This increase was primarily attributable to an increased U.S. dollar/DKK exchange rate for the year ended December 31, 2014, resulting in an unrealized net foreign exchange gain related to the intercompany loan between our parent company and our U.S. subsidiary, of DKK 38 million ($6 million). Financial expenses for the year ended December 31, 2014 was DKK 10 million ($1 million) compared to DKK 34 million for the year ended December 31, 2013. This decrease was primarily attributable to unrealized net foreign exchange losses of DKK 22 million in 2013.

Tax on the income for the year ended December 31, 2014 was DKK 38 million ($6 million) corresponding to an effective tax rate of 60%. The effective tax rate was above the Danish Company

tax rate of 24.5% due to non-recognized deferred tax asset on the period's loss in Bavarian Nordic, Inc. and adjustments of deferred tax due to change in tax rates.

Tax on the income for the year ended December 31, 2013 was DKK 53 million corresponding to an effective tax rate of 853%, primarily due to a DKK 38 million tax expense related to adjustment of the deferred tax asset due to changed tax rates (from 25% to 22% in 2016).

As of September 30, 2015, we had cash and cash equivalents of DKK 462 million ($69 million). In addition, we held investments in securities of DKK 772 million ($116 million). We also maintained credit lines of DKK 393 million ($59 million) as of such date, of which DKK 384 million ($58 million) was undrawn.

We require cash to meet our operating expenses and capital expenditures. We have funded our cash requirements from inception through September 30, 2015 principally with a combination of revenue from product sales, including contract work for the U.S. government, debt financings, revenue under our collaboration agreement with Janssen, development funding from government entities and, to a lesser extent, from the sale of our common stock.

The following table provides information regarding our cash flows for the years ended December 31, 2014 and 2013 and the nine months ended September 30, 2015 and 2014.

Net cash provided by operating activities totalled DKK 339 million ($51 million) for the year ended December 31, 2014 compared to DKK 147 million for the year ended December 31, 2013. The increase was primarily due to the prepayments received from the agreement with Janssen in October 2014 in the amount of $60 million.

Net cash provided by operating activities for the nine months ended September 30, 2015 was DKK 270 million ($41 million) compared to net cash used in operating activities of DKK 210 million for the nine months ended September 30, 2014. This increase was primarily due to the second upfront payment under the development supply agreement with Janssen in the amount of $36 million and the upfront payment from the license agreement with BMS for PROSTVAC in the amount of $60 million.

Net cash used in investing activities was DKK 504 million ($76 million) for the year ended December 31, 2014 compared to DKK 147 million for the year ended December 31, 2013. This increase was primarily due to investment in securities in the amount of DKK 398 million ($60 million), which was partly offset by a decrease in investment in intangible assets in the amount of DKK 57 million ($9 million).

Net cash used in investing activities for the nine months ended September 30, 2015 was DKK 239 million ($36 million) compared to net cash provided by investing activities of DKK 13 million for the nine months ended September 30, 2014. The cash used in the nine months ended September 30, 2015 was primarily related to net investment in securities in the amount of DKK 209 million ($31 million). Investment in property, plant and equipment and intangible assets amounted to DKK 30 million ($5 million) compared to DKK 83 million in the nine months ended September 30, 2014. During the nine months ended September 30, 2014, we spent DKK 43 million in intangible investments of which DKK 39 million was related to the IMVAMUNE/IMVANEX development project and DKK 40 million in tangible investments of which DKK 23 million was related to the expansion of the Kvistgaard facility. In the same period, we had a net disposal of securities in the amount of DKK 96 million.

Net cash provided by financing activities totalled DKK 216 million ($32 million) for the year ended December 31, 2014 compared to net cash used in financing activities of DKK 7 million for the year ended December 31, 2013. The increase was primarily due to proceeds from Johnson & Johnson Development Corporation's equity investment of $43 million and proceeds from our warrant program in the amount of DKK 14 million ($2 million), which was partly offset by a higher repayment on our mortgage and construction loan in the amount of DKK 42 million ($6 million).

Net cash provided by financing activities for the nine months ended September 30, 2015 was DKK 16 million ($2 million) compared to net cash used in financing activities of DKK 4 million for the nine months ended September 30, 2014. The increase was primarily due to higher proceeds from exercise of our warrant programs in the amount of DKK 16 million ($2 million).

The net increase in cash and cash equivalents for the nine months ended September 30, 2015 was DKK 48 million ($7 million).

The following tables summarize our contractual obligations at December 31, 2014.

As of September 30, 2015, our principal amount of debt outstanding to credit institutions, undrawn credit facilities and guarantees received was comprised primarily of the following:

As of December 31, 2014 our operating lease obligations were comprised primarily of the following:

As of December 31, 2014 our contractual obligations under collaborative agreements were comprised primarily of a commitment for a filling campaign in March 2015, future NCI CRADA payments for PROSTVAC and CV 301 and potential NIH milestone payments for PROSTVAC.

We believe that the net proceeds from this offering, together with our existing securities, cash and cash equivalents, revenue from IMVAMUNE/IMVANEX and MVA-BN Filo product sales, milestones from collaborations and other committed sources of funds, will be sufficient to enable us to fund our anticipated operating expenses, capital expenditure and debt service requirements for at least the next 12 months. We have based this estimate on assumptions that may prove to be wrong. We expect to continue to fund a significant portion of our development and commercialization costs for our product candidates with internally generated funds from sales of IMVAMUNE/IMVANEX and MVA-BN Filo. There are numerous risks and uncertainties associated with IMVAMUNE/IMVANEX and MVA-BN Filo product sales, and with the development and commercialization of our product candidates. In addition, our ability to borrow additional amounts under our loan agreements is subject to our satisfaction of specified conditions.

We may require additional sources of funds for future acquisitions that we may make or, depending on the size of the obligation, to meet balloon payments upon maturity of our current borrowings. To the extent our capital resources are insufficient to meet our future capital requirements, we will need to finance our cash needs through public or private equity offerings, debt financings, or corporate collaboration and licensing arrangements.

Additional equity or debt financing, grants, or corporate collaboration and licensing arrangements, may not be available on acceptable terms, if at all. If adequate funds are not available, we may be required to delay, reduce the scope of or eliminate our research and development programs or reduce our planned commercialization efforts. If we raise additional funds by issuing equity securities, our stockholders may experience dilution. Debt financing, if available, may involve agreements that include covenants limiting or restricting our ability to take specific actions, such as incurring additional debt, making capital expenditures or declaring dividends. Any debt financing or additional equity that we raise may contain terms, such as liquidation and other preferences, that are not favorable to us or our shareholders. If we raise additional funds through collaboration and licensing arrangements with third parties, it may be necessary to relinquish valuable rights to our technologies or product candidates, or grant licenses on terms that may not be favorable to us.

Our activities primarily expose us to the financial risks of changes in foreign currency exchange rates. We have from time to time purchased or sold foreign exchange options to manage our currency exposure to such risks.

Our parent company's functional currency is DKK, although our U.S. subsidiaries use the U.S. dollar for their functional currency. Our production site is in Denmark and the related cost base is mainly determined in DKK. Our consolidated presentation currency for our consolidated financial statements is DKK. Currencies other than DKK are considered a foreign currency.

We have the highest exposure for exchange rate risks in U.S. dollar. A substantial part of our revenue and cost base arises from U.S. dollar contracts. However, the annual net exposure in U.S. dollar (positive cash flow) has still been more than $100 million the last couple of years, meaning that we have a material exposure towards the development in the U.S. dollar exchange rates.

Our foreign exchange policy is as follows: Generally, we seek to minimize exchange rate risk on cash flows in foreign currencies by natural hedging through matching of income and expenses in U.S. dollars. At a minimum, twice per year, when preparing our annual forecast and budget, we calculate our net exposure in U.S. dollars for the coming 12 months. Based on such calculations, it is decided whether to hedge our net exposure by entering foreign exchange contracts or options. The net exposure only includes committed sales contracts, meaning that non-committed sales contracts are excluded although included as revenue in the budget.

We have an intercompany loan in U.S. dollars from our parent company in Denmark (Bavarian Nordic A/S) to our U.S. subsidiary in California. This loan cannot be hedged. This means that an increase in the U.S. dollar/DKK exchange rate will result in a non-cash foreign exchange gain as our parent company will have a larger outstanding receivable from the loan when converted to DKK, while our U.S. subsidiary will have an unchanged debt in U.S. dollars. A decrease in the U.S. dollar/DKK rate will result in a non-cash foreign exchange loss as the parent company will have a smaller outstanding receivable from the loan when converted to DKK, while our U.S. subsidiary will have an unchanged debt in U.S. dollar. As of September 30, 2015 the loan amounted to $51 million.

We perform an analysis and report on our foreign currency exposure on an annual basis. At September 30, 2015, the carrying amount of our foreign currency denominated monetary assets (including our intercompany loan) was $114 million, of which we held $51 million denominated in U.S. dollars and our foreign currency denominated monetary liabilities was $1 million. The net proceeds from this offering in U.S. dollars may be partially held in U.S. dollars and partially converted to our functional currency.

A sensitivity analysis of our exposure to the U.S. dollar based on outstanding foreign currency denominated monetary items as of September 30, 2015 shows that a strengthening of U.S. dollar against DKK by 10% would increase net profit or loss and equity by DKK 76 million ($11 million). A 10% weakening of the U.S. dollar against DKK would decrease profit or loss and equity by a similar amount.

We consider all of our material counterparties, including the U.S. government, the European Union, BMS and Janssen to be creditworthy. Our trade receivables consist of a small number of large transactions with our collaboration partners and other biopharmaceutical companies. This may lead to a significant concentration of credit risk, but we consider the credit risk for each of our collaboration partners, and other customers with whom we conduct business, to be low. We limit our credit risk on securities, cash and cash equivalents by depositing our cash reserves with banks that maintain high credit ratings assigned by international credit rating agencies.

We manage our liquidity risk by maintaining adequate cash reserves at banks, and by continuously monitoring our cash forecasts, our actual cash flows and by matching the maturity profiles of financial assets and liabilities. We believe that our existing securities, cash and cash equivalents as of September 30, 2015, along with the proceeds from this offering, will be sufficient to meet our projected cash requirements for at least the 12 months from the date of this prospectus.

Our most liquid assets are securities, cash and cash equivalents. Because of their liquidity, these assets are not directly affected by inflation. We have intangible and tangible assets in the value of our intellectual property. Because we intend to retain and continue to use our intangible assets and property, plant and equipment, we believe that the incremental inflation related to replacement costs of such items will not materially affect our operations. However, the rate of inflation affects our expenses, such as those for employee compensation and contract services, which could increase our level of expenses and the rate at which we use our resources.

Our consolidated financial statements have been prepared in accordance with IFRS as issued by the IASB. A description of our significant accounting policies is provided in our audited consolidated financial statements as of and for the years ended December 31, 2014 and 2013 included elsewhere in this prospectus.

The IASB has issued new standards and revisions to existing standards and new interpretations, which are mandatory for accounting periods commencing on or after January 1, 2014. The implementation of new or revised standards and interpretations that are in force have not changed the accounting policies and thus have not affected net profit for the year or the financial position.

At the date of publication of the consolidated financial statements, a number of new and amended standards and interpretations have not yet entered into force. Therefore, they are not incorporated in the consolidated financial statements.

IASB has issued IFRS 9 "Financial Instruments," with an effective date of January 1, 2018. However, it has not yet been implemented. IFRS 9 "Financial Instruments" is part of IASB's project to replace IAS 39 "Financial Instruments: Recognition and Measurement," and the new standard will change the classification, presentation and measurement of financial instruments and hedging requirements. We are assessing the impact of the standard, but it is not expected to have any material impact on future consolidated financial statements.

IFRS 15 "Revenue from Contracts with Customers" is effective for annual periods beginning on or after January 1, 2018. However, it has not yet been implemented. Entities will apply a five-step model to determine when, how and at what amount revenue is to be recognized depending on whether certain criteria are met. Before implementation of the standard, we will assess whether IFRS 15 "Revenue from Contracts with Customers" has an impact on current and new significant agreements. The new standard is not expected to have any material impact on future consolidated financial statements.

In the preparation of the consolidated financial statements, management makes a number of accounting estimates that form the basis for the presentation, recognition and measurement of our assets and liabilities.

The recognition and measurement of assets and liabilities often depends on future events that are somewhat uncertain. In that respect, it is necessary to assume a course of events that reflects management's assessment of the most probable course of events.

In connection with the preparation of the consolidated financial statements, management has made a number of estimates and assumptions concerning carrying amounts. Management has made the following accounting judgments, which significantly affect the amounts recognized in the consolidated financial statements:

Please refer to the notes to our audited consolidated financial statements included elsewhere in this prospectus for further description of the significant accounting estimates and assumptions used.

Implications of Being an "Emerging Growth Company" and a Foreign Private Issuer

We are a fully integrated biotechnology company developing, manufacturing and commercializing novel vaccines for the prevention of life-threatening infectious diseases and the treatment of cancer. We focus on diseases for which the unmet medical need is high and for which we can harness the power of the immune system to induce a response. Our live virus vaccine platform employs poxviruses in a modular approach to create our vaccines. This platform has generated one commercial product for smallpox, one Phase 3 immunotherapy candidate for prostate cancer, one Phase 3 candidate for Ebola and several other clinical programs in the areas of infectious disease and oncology. We recognized revenue of $182 million in each of 2013 and 2014, primarily from sales of our commercial smallpox vaccine, IMVAMUNE/IMVANEX. This revenue has enabled us to invest significant capital into research and development activities, the expansion of our production infrastructure and the advancement of our clinical pipeline.

Our poxviruses are designed to enhance the immune system through the production of antibodies and the stimulation of T-cells. The poxvirus family consists of viruses with larger DNA genomes than other viruses. The large genome of poxviruses allows for insertion of genetic material encoding for multiple and relatively large antigens, which are toxins or foreign substances that induce an immune response. This enables us to create vaccines for a wide variety of diseases. It also permits us to target multiple antigens for a single disease which we believe leads to a more robust vaccine. Our modular approach has three core components, which can be combined in a prime-boost regimen in various formulations. There are three types of poxviruses that we may employ to achieve a desired effect: Modified Vaccinia Ankara, or MVA, vaccinia and Fowlpox. We optimize these poxviruses with our proprietary technology to incorporate an antigen in order to create recombinant viral vaccines. We employ these viruses in various combinations for both the initial vaccination, or primer, and subsequent vaccination(s), or booster(s).

Our expertise in this field has led to a 10+ year long relationship with the U.S. government, pursuant to which we have been awarded approximately $1.2 billion in contracts. To date, we have recognized more than $900 million of revenue from these contracts. We believe that we are well positioned to generate additional revenue from such contracts due to our track record of success, relationships with U.S. governmental agencies and the quality of our live virus vaccines. More recently, we believe our platform has been validated by commercial relationships with two large pharmaceutical companies, Bristol-Myers Squibb, or BMS, for PROSTVAC, our Phase 3 cancer immunotherapy candidate, and the Janssen Pharmaceutical Companies of Johnson & Johnson, or Janssen, for our Ebola vaccine candidate and additional infectious disease targets, including human papillomavirus, or HPV.

Our vaccine portfolio consists of two product categories: infectious disease vaccines and cancer immunotherapies. Our infectious disease portfolio includes the following:

We are also developing a pipeline of cancer immunotherapy product candidates to harness the power of the immune system to fight cancer. Our product candidates have been designed to enhance a specific T-cell response against a tumor target. In addition, this targeted T-cell response also inflames the tumor, thereby making it more sensitive to additional targeted therapies.

In order to advance our pipeline, we have established and will continue to assess collaborations with third parties. We work closely with the NCI, and other institutes and centers of the National Institutes of Health, or NIH, towards the development of key technologies underlying our product candidates. We have established relationships with the U.S. Public Health Emergency Medical Countermeasures Enterprise, or PHEMCE, as well as its member organizations, including the Biomedical Advanced Research and Development Authority, or BARDA, the Department of Defense, or DOD, and the Department of Homeland Security, or DHS. To advance PROSTVAC and MVA-BN Filo, we have established collaborations with BMS and Janssen, respectively. We currently retain worldwide commercial rights to MVA-BN RSV, MVA-BN Brachyury and CV 301 for multiple solid tumor indications.

We own and operate a fully integrated, highly scalable current Good Manufacturing Practices, or cGMP, commercial scale vaccine production facility in Kvistgaard, Denmark. This facility has been inspected by the European Medicine Agency, or EMA, and the FDA without notice of any material deficiency. As part of the contract to supply 28 million doses of IMVAMUNE/IMVANEX to the U.S. government, we have had numerous successful inspections by the NIH and BARDA. We have built an extensive patent portfolio comprised of more than 740 granted/issued patents and more than 240 pending patent applications. Our ability to manufacture our live virus vaccines has been demonstrated by our production of 28 million doses of IMVAMUNE/IMVANEX to date and more than 2 million doses of our MVA-BN Filo product candidate for Ebola.

We have leveraged our live virus vaccine platform to generate one commercial vaccine that is part of seven clinical programs in our focus areas of infectious diseases and cancer immunotherapy. The chart below summarizes the stage of each of our active clinical development programs. Please

also see a description of certain supply and research and development agreements, pursuant to which we are developing certain of these products under the caption "—Our Partnerships."

In addition to our clinical pipeline, we have multiple ongoing preclinical programs. These include multiple contracts with U.S. government agencies, including the NCI and BARDA. Through the Janssen collaboration, we are also exploring additional diseases and targets; specifically, MVA-BN is being actively evaluated in preclinical stages for the early treatment and prevention of HPV-induced cancers. MVA-BN is also being evaluated for the treatment and prevention of two undisclosed infectious disease targets for the potential further expansion of the Janssen collaboration. We and Janssen are also developing the MVA-BN vaccine to target Marburg virus. We also continue to collaborate with the NCI and to develop our own proprietary immunotherapy programs.

A vaccine is a biological preparation that provides active immunity for the prevention of an infectious disease, or the treatment of infectious disease or cancer. All of our vaccines contain live viruses, some of which have been attenuated, or altered so as not to replicate in human cells. These vaccines are designed to harness the power of the immune system to induce a response.

Our live virus vaccine platform uses three poxviruses to stimulate the immune system: MVA, vaccinia, and Fowlpox. Poxviruses are a family of viruses that have been extensively studied as vaccine vectors, or delivery vehicles. Each of these poxviruses has certain desirable attributes that

contribute to the versatility of our platform and the potentially favorable safety profile and effectiveness of our vaccines. MVA can be designed to be replication incompetent in humans, which enables a favorable safety profile. Vaccinia has been used effectively in millions of people to eradicate smallpox. This virus accommodates large DNA fragments and has been shown to induce robust immune responses. Fowlpox virus, or FPV, is replication incompetent and does not result in neutralizing antibodies in humans, which enables multiple boosts.

We use live viruses as vectors, or delivery vehicles, to transmit a combination of one or more antigens, promoters and/or costimulatory molecules for a particular indication, which we encode within the virus' DNA. A promoter is a region of DNA that initiates transcription of a particular gene and costimulatory molecules play a key role in the initiation of an immune response. The incorporated antigen causes the body's immune system to produce antibodies against it. The graphic below illustrates how we create our live virus vaccines.

In order to increase the effectiveness of live virus vaccines, many vaccines are delivered through repeated vaccination to "boost" immune responses. The basic prime-boost strategy involves priming the immune system to a target antigen delivered by one vector and then selectively boosting this immunity by re-administration of the antigen with one or more subsequent vectors. The key strength of this strategy is that greater levels of immunity are established than can be attained by a single vaccine administration. Prime-boosting permits the potential synergistic enhancement of immunity to the target antigen. Hence we are able to use MVA or vaccinia followed by multiple Fowlpox boosts in order to create a greater synergistic immune response, which is typically reflected in an increased number of T-cells directed at the specific antigen.

A core component of our live virus vaccine platform is Modified Vaccinia Ankara-Bavarian Nordic, or MVA-BN, our proprietary and patented vaccine technology. Our intellectual property estate, technical know-how and expertise help to secure our leading position in poxvirus vaccine

development. To develop the MVA-BN vector, we created a further attenuated version of the MVA virus that was used to pre-vaccinate more than 100,000 individuals against smallpox in Germany in the 1970s. While we have shown that MVA-BN fails to replicate in numerous human cell lines and is safe in highly immune compromised mice, all other public sources of MVA replicate in one or more human cell lines and have lead to the death of severely immune compromised mice.

MVA-BN is capable of acting as a delivery vehicle for DNA-expressing diseases other than smallpox. MVA-BN is a particularly good vector as it is based on the vaccinia virus, which induces strong immune-stimulation, is non-replicating and therefore unable to cause disease induction in patients, leading to its favorable safety profile. It also has large double-stranded DNA genomes, which are capable of incorporating long and complex antigens. The inability to replicate in human cells and the favorable safety profile of MVA-BN in severely immune compromised animals makes MVA-BN a highly attractive vaccine candidate, particularly for high risk populations, such as young children, immune compromised and elderly, who all have weakened and/or immature immune systems. MVA-BN has been shown to have a favorable safety profile in more than 7,600 people, which includes more than 1,000 immune compromised individuals such as HIV infected subjects. As a result, we believe MVA-BN is an adaptable vaccine technology suitable for addressing a wide variety of infectious disease and cancer.

Our cancer immunotherapy candidates, PROSTVAC, CV 301 and MVA-BN Brachyury employ our VF-TRICOM technology, which we license from the NCI and the United States Public Health Service, or PHS. This technology includes a vaccinia-based priming dose (V) followed by multiple Fowlpox-based boosting doses (F), and incorporates three human immune costimulatory molecules, or TRICOM: TRIad of COstimulatory Molecules, engineered to enhance immune system response to the tumor target. Both the priming and boosting doses encode one or more tumor-associated antigens intended to activate the body's immune system against these antigens. This heightens a key role of the immune system, which is the detection of these antigens, which many tumor cells produce, to permit subsequent targeting for eradication.

Beyond the benefits of the prime-boost regimen of vaccinia and Fowlpox, the inclusion of TRICOM serves as a genetic adjuvant within our product candidates. These three natural, human, immune-enhancing, costimulatory molecules serve multiple purposes. Two of the molecules, ICAM-1 and LFA-3, assist in binding T-cells to an affected cell, while the third molecule, B7.1, serves as a potent stimulator of tumor-associated antigen-specific T-cells. Each of these molecules has been shown to enhance antigen specific T-cell responses, but the combined use of the three costimulatory molecules acts synergistically to further enhance antigen-specific T-cell responses. Because cancer immunotherapy works by generating an immune response from a patient, larger immune responses may correlate with improved patient outcomes and may therefore be more effective in using the body's own defense mechanisms to fight cancer.

We own and operate a fully integrated, highly scalable vaccine production facility, which we believe plays a key role in our capabilities. Our approximately 100,000 square foot multiproduct production facility in Kvistgaard, Denmark operates in accordance with cGMP and houses production, quality assurance, quality control, or QC, and administration. Our production facility has been inspected by the EMA and the FDA without notice of any material deficiency. This facility is used for the production of all of our current clinical candidates. To date, we have produced at our facility and delivered 28 million doses of IMVAMUNE/IMVANEX, as well as more than 2 million doses of our MVA-BN Filo candidate for Ebola. We believe that our production facility would also be able to support all of our future commercial activities at currently anticipated levels of production,

including the production of all clinical trial materials and the potential commercialization of our late-stage product candidates.

We are a fully integrated biotechnology company, and we believe that we have several key competitive advantages in developing, producing and commercializing live virus vaccines:

We have leveraged our live virus vaccine platform to create a commercial smallpox vaccine and a pipeline of infectious disease vaccine candidates. Our portfolio of our infectious disease products is shown below:

Smallpox is a contagious, disfiguring and often deadly disease. Naturally occurring smallpox was eradicated worldwide by 1980 as a result of an unprecedented global immunization campaign. Samples of the smallpox virus have been kept for research purposes, which has led to concerns that smallpox could someday be used as a biological warfare agent. The DHS has declared smallpox to be a material threat to national security and the U.S. Centers for Disease Control and Prevention, or CDC, classifies smallpox as a Category A bioterror agent. Additionally, smallpox has been identified as a high-priority threat by PHEMCE. No cure or treatment for smallpox exists.

The only existing vaccine approved for use in the United States to prevent smallpox is ACAM2000, a live replicating virus. ACAM2000 has several important drawbacks, including known cardiac toxicity with suspected cases of myocarditis and pericarditis observed in 5.7 per 1,000 individuals vaccinated. Additionally, the administration of the vaccine is contraindicated for certain individuals in the United States including those with severe immunodeficiency and who are not expected to benefit from the vaccine. These individuals include severely immuno-compromised individuals and the following individuals who are otherwise at increased safety risk: pregnant women; individuals with HIV infection; individuals with a history of eczema or atopic dermatitis; individuals who are undergoing bone marrow transplantation or individuals with primary or acquired immunodeficiency who require isolation; or infants less than one year of age. In the United States, this translates into a population of over 66 million people.

IMVAMUNE, which is also marketed under the trade name IMVANEX in Europe, is a non-replicating smallpox vaccine distributed in liquid frozen formulation that is suitable for use in people for whom replicating smallpox vaccines are contraindicated. The vaccine is the only non-replicating smallpox vaccine approved in Europe for use in the general adult population.

Although not yet approved in the United States, IMVAMUNE/IMVANEX is currently stockpiled by the U.S. government for emergency use in people for whom replicating smallpox vaccines are contraindicated. BARDA is currently sponsoring a Phase 3 trial with IMVAMUNE/IMVANEX comparing the safety and immunogenicity to ACAM2000. This trial is designed to support the FDA approval for use of the vaccine in the entire population. In 2013 and 2014, we had revenue of $125 million and $153 million, respectively, from sales of IMVAMUNE/IMVANEX.

Since 2010, we have delivered 28 million doses of IMVAMUNE/IMVANEX to the U.S. Strategic National Stockpile, or SNS. The deliveries of the initial 20 million doses were completed in 2013, followed by replenishment orders for 8 million doses, with final deliveries having occurred in early 2015. The doses of our existing liquid frozen formulation of IMVAMUNE/IMVANEX delivered to the SNS have a shelf life of approximately three years. The following chart shows our deliveries of IMVAMUNE/IMVANEX to SNS since 2010, not including a $133 million bulk order placed by BARDA in July 2015. The annual and accumulated doses of IMVAMUNE/IMVANEX delivered to the SNS are illustrated in the chart below:

The U.S. government has a long-term strategy to provide sufficient non-replicating smallpox vaccine to protect 66 million people, representing 132 million doses of IMVAMUNE/IMVANEX, to address those for whom a replicating smallpox vaccine is contraindicated or who have severe immunodeficiency and who are not expected to benefit from the vaccine. These individuals include severely immuno-compromised individuals and the following individuals who are otherwise at increased safety risk: pregnant women; individuals with HIV infection; individuals with a history of eczema or atopic dermatitis; individuals who are undergoing bone marrow transplantation or individuals with primary or acquired immunodeficiency who require isolation; or infants less than one year of age.

As part of this strategy, we were awarded a contract in 2009 to develop a freeze dried formulation of IMVAMUNE/IMVANEX, which we believe indicates the U.S. government's desire to develop an improved formulation of IMVAMUNE/IMVANEX to replace the liquid frozen formulation of IMVAMUNE/IMVANEX currently stockpiled in the SNS. To date, we have been awarded $94 million to transition the current liquid frozen formulation of IMVAMUNE/IMVANEX, which possesses a shelf life of approximately three years, into a freeze dried formulation with a potential shelf life of approximately 10 or more years and potentially no storage limitations. In April 2014, the U.S. government exercised an option at a value of $22 million under the ongoing development contract to fund the validation of the production process with a larger commercial capacity in preparation for future production of this formulation of the vaccine.

In July 2015, we received a new order from BARDA for a bulk supply of IMVAMUNE/IMVANEX valued at $133 million. Under this new order, which is an extension of an existing contract, we will produce and store a bulk supply of IMVAMUNE/IMVANEX. This bulk material could be converted into freeze dried IMVAMUNE/IMVANEX at a later date, once the freeze drying production process is transferred to a commercial line and is approved by the U.S. regulatory authorities.

In May 2015, we reported data from a pivotal Phase 2 randomized, double-blind trial that enrolled 650 vaccinia-naïve healthy subjects to compare the safety and immunogenicity of our freeze dried and liquid frozen formulations of IMVAMUNE/IMVANEX. The antibody response induced by the freeze dried vaccine was equivalent to the antibody response induced by the liquid frozen formulation, meeting the primary endpoint of the trial. Both formulations also recorded a similar safety profile. Similar data have also been generated in the various animal efficacy models. The following chart shows the comparative immune response generated by liquid frozen compared to freeze dried formulations of IMVAMUNE/IMVANEX, which supports the apparent equivalent effectiveness of both formulations. The graph below shows the results of the enzyme-linked immunosorbent assay, or ELISA, that measures antibody response.

These results provided the final clinical data required to support stockpiling of this next generation of the vaccine in the SNS in the event of an emergency use authorization, or an EUA, and the validation of the production process remains the final step towards meeting the overall U.S. regulatory requirements for the stockpiling of the vaccine.

In August 2014, we signed two contracts with the Canadian authorities for the delivery of a total of 65,700 doses of IMVAMUNE/IMVANEX. During the first quarter of 2015, we delivered 45,700 doses of IMVAMUNE/IMVANEX to the PHAC, thus fulfilling the base contract awarded in 2014. The PHAC has an option to acquire more than 300,000 additional doses. In addition, we had a contract with the Canadian Department of National Defence for 20,000 doses, which were delivered during the second quarter of 2015.

A small recurrent order under a five-year contract with an Asian country was also delivered in the second quarter of 2015.

Before being approved in the European Union and Canada, commercial quantities of the vaccine were produced and sold to other governments globally under their respective national

emergency rules. We continue to explore additional market opportunities for IMVAMUNE/IMVANEX and expect to enter into contracts for further sales outside the United States in the coming years.

While the U.S. government may administer IMVAMUNE/IMVANEX in the event of an emergency under an EUA, our contracts with BARDA obligate us to submit an investigational new drug application, or IND, and seek formal approval of IMVAMUNE/IMVANEX from the FDA. We submitted INDs for our liquid frozen formulation of IMVAMUNE/IMVANEX on March 5, 2004 and for our freeze dried formulation of IMVAMUNE/IMVANEX on November 30, 2012. We have discussed with the FDA and received its comments to the proposed parameters for two Phase 3 trials to support the registration of liquid frozen formulation of IMVAMUNE/IMVANEX in the United States. These two Phase 3 trials include a lot consistency trial in 4,000 healthy individuals and a trial in 440 military personnel. The latter trial is designed to demonstrate non-inferiority between IMVAMUNE/IMVANEX and ACAM2000.

In May 2015, we reported initial results from the first Phase 3 lot-to-lot trial, which was designed as a randomized, double-blind, placebo-controlled trial in 4,000 vaccinia-naïve subjects. Three thousand subjects were vaccinated with three different production lots of the liquid frozen formulation of IMVAMUNE/IMVANEX, with 1,000 subjects per lot, and compared to 1,000 subjects who received placebo. The three lots of IMVAMUNE/IMVANEX induced equivalent antibody responses, meeting the primary endpoint of the trial, while the favorable safety profile of IMVAMUNE/IMVANEX was confirmed. The graph below shows the results of the enzyme-linked immunosorbent assay, or ELISA, that measures antibody response.

Subjects in our trial were monitored closely for cardiac events as these were observed in trials with ACAM2000. No serious adverse reactions were reported among the 3,000 subjects vaccinated with IMVAMUNE/IMVANEX, confirming the results of a smaller Phase 2 placebo-controlled trial that was recently published. We believe that the safety profile of IMVAMUNE/IMVANEX differentiates it from ACAM2000, the only approved smallpox vaccine in the United States, which has a high rate of cardiac complications in healthy vaccinees, 5.73 events per 1,000 immunizations.

The second Phase 3 trial comparing the safety and immunogenicity of IMVAMUNE/IMVANEX to ACAM2000 was initiated at a U.S. military garrison in South Korea in the first quarter of 2015. The trial is a randomized controlled trial comparing IMVAMUNE/IMVANEX to ACAM2000. This is a two-arm trial conducted by the U.S. Army Medical Research Institute of Infectious Diseases, and designed to enroll 440 patients. We expect enrollment to be complete in 2017.

RSV is the most common cause of lower respiratory tract infection in infants and children worldwide, resulting in a high number of hospitalizations. Most infants are infected before age one, and virtually everyone contracts an RSV infection by age two. RSV infections are responsible each year for a similar number of deaths as the flu in children up to age 14, as well as in the elderly population. It is estimated that more than 64 million people are infected globally each year, yet unlike the flu, there is no vaccine to prevent RSV, presenting a large unmet medical need and market opportunity.

While numerous efforts have been made to develop a prophylactic vaccine, there is no approved vaccine against RSV. There are two major subtypes of RSV: subtype A and subtype B. The two subtypes are typically present either simultaneously or alternately during yearly epidemics. The more severe illnesses, which usually predominate during outbreaks, are associated with the subtype A strain.

MVA-BN RSV is our product candidate for the vaccination of RSV. Published data from preclinical studies have shown that both an antibody and a T-cell response are required to prevent an RSV infection. Accordingly, we have designed our product candidate to elicit responses against both RSV subtypes A and B. Our product candidate has been shown to be highly efficacious in nonclinical studies, demonstrating both an antibody and a T-cell response from the immune system. Importantly, multiple clinical trials have shown that the prevention of RSV is dependent upon an antibody response within the mucosa. In addition to antibodies in the blood, the presence of antibodies in the mucous membrane is an important barrier to infection by RSV. Preclinical studies and clinical trials have shown that our product candidate brings about such an antibody response in the mucosa. The chart below shows the results of a study in cotton rats, which evidenced an increase in immunogloblin G antibody, or IgG, production in blood, and in immunoglobulin A antibody, or IgA, production in mucous, which provides evidence of an antibody response to RSV. These data show that when MVA-BN RSV is administered, there is evidence of an increase in antibodies of >7-fold and >75-fold in the blood and the mucosa, respectively, following a single vaccination.

Following a pre-IND meeting with the FDA, we filed our IND for MVA-BN RSV on May 29, 2015 and a Phase 1 trial in healthy adults was initiated in August 2015. This Phase 1 trial, which is being conducted in the United States, is evaluating the safety, tolerability and immunogenicity of our recombinant MVA-BN-based RSV vaccine in 63 healthy adults, ages 18 to 65. The trial is now fully enrolled and subjects were enrolled into three groups with each group receiving a different dose of MVA-BN RSV. One group enrolled subjects of 50 to 65 years of age who received a higher dose of MVA-BN RSV in order to evaluate the immune responses in an elderly population, which is a key target for the vaccine candidate. Volunteers in each group were randomized to receive two vaccinations of MVA-BN RSV vaccine or placebo. The primary objective of this trial is to demonstrate safety and reactogenicity of MVA-mBN294B (MVA-BN RSV vaccine), and the secondary objective is RSV-specific (ELISA, PRNT, ELISPOT/ICS) and vaccinia-specific immune response to MVA-BN-RSV vaccine.

We anticipate results from this current Phase 1 trial will be reported in the first half of 2016. If the Phase 1 trial is successful, we intend to rapidly progress our RSV vaccine candidate into multiple Phase 1 and Phase 2 trials, looking not only at elderly and at risk populations, but also at the pediatric population.

MVA-BN Filo is a prime-boost regimen consisting of a primer, Ad26.ZEBOV, which Janssen developed, and a boost, MVA-BN Filo, which we developed. Our vaccine candidate, MVA-BN Filo, contains the gene of the glycoprotein of Ebola Zair, or ZEBOV, the species responsible for the recent outbreak of Ebola in Western Africa, as well the genes of the glycoproteins of Ebola Sudan and of Marburg virus. Therefore, the vaccine candidate that we constructed is designed to provide protection not only against the Ebola virus that is the cause of the current outbreak, but also against the two other most common causes of viral hemorrhagic fevers.

In October 2014, we entered into a collaboration and license agreement for the development and commercialization of an Ebola vaccine with Janssen. The deal was part of a commitment made by Johnson & Johnson of more than $200 million to accelerate and significantly expand the production of an Ebola vaccine. Under the terms of the agreement, we granted Janssen an exclusive license for our MVA-BN Filo vaccine candidate. We received an upfront payment of $25 million and are entitled to receive up to $20 million milestone payments, in addition to potential royalties on commercial sales at certain price levels outside Africa. Due to the recent outbreak of Ebola in Africa, we have elected not to receive royalties for sales in Africa. We have also entered into a supply agreement with Janssen under which we will produce and deliver to Janssen bulk material equivalent to approximately 2 million doses of MVA-BN Filo. The supply agreement has a value of $99 million. Furthermore, Johnson & Johnson Development Corporation made a $43 million equity investment in our company. Janssen will be fully responsible for all costs associated with the development and commercialization of the vaccine candidate. In emergency outbreak situations, the agreement does not exclude us from collaborating with other parties in the development and supply of Ebola vaccines for preclinical studies and clinical trials.

Backed by worldwide health authorities, Janssen is fast-tracking the clinical development of the prime-boost vaccine regimen. Janssen presented preliminary results from a Phase 1 first in human trial in May 2015 at a meeting of the FDA's Vaccines and Related Biological Products Advisory Committee as part of discussions regarding the development and licensure of Ebola vaccines. In the trial, conducted by the Oxford Vaccines Group, 72 healthy volunteers were randomized into four groups receiving the vaccine regimen or placebo. The preliminary results from the ongoing trial confirmed the preclinical results, and show that the prime-boost vaccine regimen was immunogenic, regardless of the order of vaccine administration, and that both vaccine candidates only provoked temporary reactions normally expected from vaccination, thus requiring a booster. The below data shows the effectiveness of a boost by showing increased antibody production in healthy individuals when treated with a prime-boost vaccine regimen of MVA-BN Filo and Ad26.ZEBOV significantly exceeds that of placebo, regardless of which vaccine is administered as a prime dose and which is administered as a boost:

A multicenter Phase 2 clinical trial was initiated by Janssen in the United Kingdom and France in July 2015. The trial is intended to evaluate the safety, tolerability and immunogenicity of the vaccine regimen. Also led by the Oxford Vaccines Group, the trial will enroll 612 healthy adult volunteers, who will be randomized into three cohorts, all receiving the Ad26.ZEBOV prime or placebo on day 1 and then the MVA-BN Filo boost or placebo on days 29, 57 or 85. A second Phase 2 trial with an expected enrollment of approximately 1,188 subjects and a Phase 3 trial with an expected enrollment of approximately 440 subjects have been initiated in Africa. Data from the Phase 3 clinical trial in Africa are expected in 2016.

Following the Ebola vaccine agreement, we and Janssen agreed to collaborate on the evaluation of MVA-BN for three additional infectious disease targets. Janssen has been granted the exclusive option to collaborate on one or more of the targets following the preclinical evaluation of MVA-BN-based vaccine candidates, which we will develop. The terms of any such collaboration would be separately negotiated at that time. Given the clinical efficacy seen in the recently reported Ebola prime-boost vaccine regimen, we believe that the combination approach of an adenovirus-prime along with an MVA-boost in additional infectious disease targets has the potential to improve the induction of strong immune responses in the short term due to the highly immunogenic

adenovirus, and provide long-term protection against a given target, and will warrant additional investigation.

In December 2015, we entered into a collaboration and license agreement with Janssen for one of the three additional infectious disease targets. Pursuant to the agreement, Janssen will acquire exclusive rights to our MVA-BN technology for use in a prime-boost vaccine regimen together with Janssen's adenovirus vector based technology. The goal is to develop a vaccine to treat chronic HPV infections as well as prevent precancerous stages of HPV-induced cancer. HPV is known to be the primary cause of cervical cancer and certain types of head and neck cancer, in addition to a number of more rare cancers. We expect that Janssen will focus initially on cervical cancer and then head and neck cancers. Janssen continues to retain an exclusive option to license MVA-BN for the two additional undisclosed infectious disease targets.

We have built a pipeline of immunotherapy candidates for major cancers with large unmet medical needs. We are leveraging our live virus vaccine platform to create novel, off-the-shelf immunotherapy candidates to selectively target and kill cancer cells with limited side- or off-target effects.

Immunotherapy is part of a growing field in cancer research and treatment. Our product candidates have been designed to enhance a specific T-cell response against a tumor target. These targeted immunotherapies are therefore able to harness the power of the immune system to fight cancer. By eliciting a strong T-cell immune response, immunotherapies may slow the progress of the disease and increase overall survival, or OS, with an improved safety profile compared to many traditional chemotherapies and hormone treatments. Another benefit of the enhanced T-cell response is that the tumor is subsequently more immunogenic and sensitive to additional targeted therapies.

We are advancing multiple targeted immunotherapy candidates, the most advanced of which is PROSTVAC, a targeted immunotherapy candidate that is now being evaluated as first-line, single-agent therapy for prostate cancer as well as in combination with other novel agents where the potential exists for therapeutic synergy. PROSTVAC is currently in a Phase 3 pivotal trial for the treatment of mCRPC. In March 2015, we entered into an option agreement with BMS that included a $60 million upfront payment and subsequent milestone payments up to an aggregate of $915 million, as well as royalty payments, granting BMS commercialization rights to PROSTVAC. See the section of this Prospectus entitled "Business—Our Partnerships—Agreement with BMS Regarding PROSTVAC."

We are also developing CV 301 and MVA-BN Brachyury. CV 301 is a novel immunotherapy candidate that targets two tumor-associated antigens, CEA and MUC-1, which are over-expressed in major cancer types. CV 301 is currently being evaluated in an NCI-sponsored Phase 2 clinical trial for bladder cancer, and we expect to initiate a Phase 2 clinical trial in NSCLC in 2016. MVA-BN Brachyury is a novel immunotherapy candidate designed to induce a robust T-cell immune response against brachyury. Tumors that overexpress brachyury are believed to be highly resistant to current therapies and are associated with decreased survival rates.

A key part of our strategy to advance our targeted immunotherapy candidates is to establish collaborations and relationships with third parties. To this end, we have partnered with BMS, the NIH and the PHS to research and develop our immunotherapy candidates.

Vaccines within our cancer immunotherapy portfolio have been observed to induce an antigen cascade, a process by which the body employs T-cells against antigens that were not present in the

initial vaccination in addition to T-cells against antigens that were present in the initial vaccination. This results in supplemental immune responses that were not the specific target of the vaccine. For example, although PROSTVAC encodes PSA and CV 301 encodes CEA and MUC-1, blood samples taken from patients treated with PROSTVAC and CV 301 evidenced T-cells targeted against a number of additional tumor antigens not seen prior to treatment. We see the induction of the antigen cascade as promising evidence of efficacy of our immunotherapies because it is a result of the tumor cells dying, and releasing new tumor antigens that the immune system can identify and target. This process is believed to be an essential component of the benefit seen in the clinic.

The following is a summary of our cancer immunotherapy product candidate portfolio:

According to the CDC, prostate cancer is the most common cancer in U.S. men. The American Cancer Society estimates that in 2015, approximately 220,800 new cases of prostate cancer will be diagnosed and approximately 27,540 deaths will result from prostate cancer. It is estimated that one U.S. man out of seven will be diagnosed with prostate cancer during his lifetime. Prostate cancer is the second leading cause of cancer death in U.S. men, behind only lung cancer. It is estimated that one U.S. man out of 38 will die of prostate cancer. However, a diagnosis of prostate cancer is not necessarily deadly, as more than 2.9 million U.S. men who have been diagnosed with prostate cancer at some point are still alive today.

Prostate cancer may be treated with a combination of surgery, radiation, hormone therapy, chemotherapy, biologic therapy and bisphosphonate therapy. While there has been meaningful progress in the treatment of prostate cancer, including approvals of new drugs by the FDA, we believe that combination therapy holds great potential to provide a clinically meaningful advance.

PROSTVAC is a PSA targeted immunotherapy candidate that we believe can be used as monotherapy or in combination with other immunotherapies. PROSTVAC is currently in Phase 3 development as monotherapy for the treatment of patients with asymptomatic or minimally symptomatic mCRPC. mCRPC is prostate cancer that no longer responds to most hormone

treatments and has spread to other parts of the body. We have observed in clinical trials consistent evidence of the effectiveness of PROSTVAC as monotherapy by increasing the length of OS. Currently, PROSTVAC is also undergoing clinical trials to determine its effectiveness in combination therapy.

A robust data package has been collected that includes data from 11 completed or ongoing Phase 1 and Phase 2 trials, and an ongoing Phase 3 clinical trial, in which more than 1,500 patients have been treated with PROSTVAC. Data from these trials indicate that PROSTVAC has generally been well-tolerated. The main findings from the Phase 1 and Phase 2 trials of patients with advanced prostate cancer show the following:

We have clinical data supporting the synergistic effect of combining PROSTVAC with the checkpoint inhibitor antibody Yervoy, or ipilimumab. This led to an agreement between BMS and ourselves to perform a Phase 2 trial to further investigate the combination of PROSTVAC with one of BMS's checkpoint inhibitor cancer immunotherapy candidates in a neoadjuvant setting of prostate cancer. Neoadjuvant therapy is a treatment such as chemotherapy, radiation therapy or hormone therapy given as a first step to shrink a tumor before the main treatment, such as surgery. While checkpoint inhibitors as monotherapy have yet to show a clinically significant impact on OS in prostate cancer, clinical data suggest that using checkpoint inhibitors in combination with PROSTVAC may create an effective treatment option in terms of OS. We believe this is due to PROSTVAC's ability to stimulate an anti-prostate cancer immune response in the majority of treated men combined with the ability of checkpoint inhibitors to make the anti-cancer immune response more effective.

In August 2008, we entered into a Cooperative Research and Development Agreement, or CRADA, with the NCI, pursuant to which we and the NCI will jointly develop new immunotherapies for the treatment of prostate cancer. Under the CRADA, we have rights to exclusively license intellectual property that results from this collaboration. In addition to the CRADA, in August 2008, we also entered into a license agreement with the PHS under which we were granted a license to intellectual property rights covering PROSTVAC.

On March 4, 2015, we entered into an option and license agreement with BMS, or the BMS agreement, granting BMS an option to commercialize PROSTVAC that included a $60 million upfront payment. If BMS exercises its option and the license goes into effect, we would be entitled to milestone payments of up to an aggregate of $915 million, as well as royalty payments on the development and commercialization of PROSTVAC. See the section of this Prospectus entitled "Business—Our Partnerships—Agreement with BMS Regarding PROSTVAC." The BMS agreement provides BMS an exclusive option to license and commercialize PROSTVAC globally. We have also agreed to enter into a supply contract with BMS. This agreement will be effective upon BMS's exercise of its option pursuant to which we will undertake the future commercial production of PROSTVAC. See "—Our Partnerships—Agreement with BMS regarding PROSTVAC."

We believe that BMS's strong presence in cancer immunotherapy makes them an ideal partner to maximize the potential of PROSTVAC as a stand-alone treatment as well as in combination with immune checkpoint inhibitors from BMS's portfolio. BMS's portfolio of immune checkpoint inhibitors

includes the anti-cytotoxic T-lymphocyte-associated protein 4, or anti-CTLA-4, or ipilimumab, which is the first approved immune checkpoint inhibitor for melanoma. The BMS portfolio also includes the fully human PD-1, or programmed cell death protein 1 immune checkpoint inhibitor Opdivo, or nivolumab, which received FDA approval in March 2015 for lung cancer. Most recently, these two drugs were approved as a combination therapy for the treatment of melanoma. Following long-term survival data from a combination trial of PROSTVAC and ipilimumab, which indicated potential synergy, we have also agreed with BMS to perform a trial evaluating the combination of PROSTVAC with one of BMS's checkpoint inhibitors.

PROSTVAC has been the subject of multiple Phase 2 clinical trials. In these trials, PROSTVAC used as monotherapy or in combination therapy, has consistently shown an OS benefit compared to either median predicted survival, based on historical data, or placebo-controls. The largest and most robust of these Phase 2 trials was a multicenter, double-blind, placebo-controlled trial enrolling 125 mCRPC patients randomized 2:1 in favor of PROSTVAC. Patients receiving PROSTVAC also received granulocyte macrophage colony-stimulating factor, or GM-CSF, in order to stimulate the production of white blood cells. Placebo patients did not receive GM-CSF. Data showed PROSTVAC immunotherapy was well-tolerated and associated with a 44% reduction in the death rate (hazard ratio, or HR, of 0.56), and an 8.5-month improvement in median OS (P=0.0061). P-value is a conventional statistical method for measuring the significance of clinical results. Typically, a p-value of 0.05 or less represents statistical significance, meaning that there is a 1-in-20 or less statistical probability that the observed results occurred by chance. The HR is the ratio of the hazard rates corresponding to the conditions described by two levels of an explanatory variable. In an immunotherapy trial, the treated population may die at twice the rate per unit time as the control population. The HR would be two, indicating higher hazard of death from the treatment.

Additional clinical trials have been conducted, and while not placebo-controlled, were measured against a validated prognostic indicator of survival. This index, known as the Halabi score, takes into consideration numerous prognostic factors when calculating a predicted survival of a patient.

One such Phase 2 trial was conducted exploring the use of PROSTVAC in 32 men with mCRPC. These men had a median age of 65.6 years, and a predicted OS of 17.4 months based on the Halabi score. Actual median OS for these patients was 26.6 months resulting in an improvement in OS of 9.2 months. The graph below reflects the data from this Phase 2 trial:

An additional Phase 2 trial was conducted in 68 patients with mCRPC with metastatic bone disease. These patients were all receiving Quadramet, or ¹⁵³Sm, an approved radiopharmaceutical for the treatment of bone pain related to metastases. Patients were randomized 1:1 to receive either PROSTVAC in combination with Quadramet, or Quadramet alone. The trials results showed that men receiving Quadramet in combination with PROSTVAC, which is referred to as PSA-TRICOM in

the graph below, saw an increase in time to progression, or TTP, of two months compared to men receiving Quadramet alone. The graph below reflects the data from this trial:

PROSTVAC has been designed to enhance or stimulate the body's immune response, specifically T-cells that will target and kill prostate cancer cells, thereby altering the course of the disease and improving the OS of patients with prostate cancer. In the most comprehensive analysis performed to date, the NCI analyzed the T-cell response induced in patients from six separate clinical trials evaluating PROSTVAC. Published in February 2014, this analysis showed that the majority of the men had a five-fold increase in T-cells recognizing PSA following PROSTVAC treatment. Moreover, the analysis showed an antigen cascade had been induced in 67% of the men treated, demonstrating that PROSTVAC was able to mount a significant and strong T-cell response

against multiple proteins associated with prostate cancer. Below is a summary of T-cell responses from six PROSTVAC clinical trials.

In February 2015, we announced updated and promising OS data from an NCI-sponsored Phase 1 combination trial of PROSTVAC and ipilimumab. Thirty patients with mCRPC were enrolled in the trial at a time when docetaxel was the only FDA-approved treatment that improved OS. The predicted median OS according to the Halabi predicted score was 18.5 months. Patients were treated with PROSTVAC plus escalating doses of ipilimumab. The observed median OS was 31.3 months for all dose cohorts and 37.2 months for patients treated at 10 mg/kg, the highest dose of ipilimumab. Furthermore, approximately 20% of patients at this dose remained alive at 80 months. We believe these data provide a strong rationale to continue to evaluate the combination of PROSTVAC and checkpoint inhibitors in additional clinical trials.

The graph below presents the data from the February 2015 NCI-sponsored Phase 1 combination trial of PROSTVAC and ipilimumab:

The PROSPECT Phase 3 clinical trial is a global randomized, double-blind, placebo-controlled trial in patients with asymptomatic or minimally symptomatic mCRPC. We are conducting the trial under a Special Protocol Assessment agreement, or SPA, with the FDA. An SPA is an agreement between a sponsor of a clinical trial and the FDA that, barring the occurrence of certain circumstances, the proposed design of a Phase 3 trial, including its clinical endpoints and statistical analyses are acceptable for support of regulatory approval after the trial has concluded. The SPA for this trial requires a hazard ratio of 0.82 or less, which is the equivalent of an approximately 18% reduction in risk of death. The trial reached its target enrollment of 1,200 patients in December 2014. As of January 2015, a total of 1,298 patients were enrolled at more than 200 investigative sites in 15 countries. The trial enrolled approximately 36% of the patients at investigative sites in North America and approximately 38% of patients at investigative sites in Western Europe. The remainder of the patients are at investigative sites around the world. This trial consisted of three arms as depicted in the chart below:

The primary objective of the trial is to determine whether the OS of patients receiving PROSTVAC in either of the treatment arms, with or without the addition of GM-CSF, is superior to that of patients receiving placebo; however, three pre-specified interim analyses of data have been integrated into the statistical plan to evaluate whether the trial should continue as planned or potentially be stopped early for efficacy or futility. While the placebo-controlled Phase 2 trial included the use of GM-CSF, additional clinical work has shown that the administration of GM-CSF with PROSTVAC may not be required. The PROSPECT trial is designed to potentially rule out the need for GM-CSF. The final analysis of each treatment arm will occur when a total of 534 deaths have occurred across that treatment arm and placebo. Should the PROSPECT trial prove successful, applications for approval will be made in the United States, the European Union and other territories.

The average number of injections received by each patient participating in the trial is 6.1. The average number of injections received by each patient in the randomized Phase 2 trial for PROSTVAC, which enrolled 122 patients, was 5.4. We believe the increase in the number of injections in this trial compared to the randomized Phase 2 trial will improve the clinical outcome for patients receiving the active drug.

The enrollment criteria for the PROSPECT trial was designed to enroll patients who we believe would most benefit from PROSTVAC. We believe that immunotherapy takes time to demonstrate its beneficial effects, and we therefore enroll patients who we believe have a sufficient life expectancy to benefit from the drug. Using the randomized Phase 2 trial as a guide, certain entry criteria were amended to better identify patients who are hormone refractory, or showing increases in PSA with no evidence of disease progression, with metastatic disease, but with certain limitations with regard to markers known to identify rapid disease progression. Patients were monitored for markers such as PSA doubling time, alkaline phosphatase levels and minimum PSA values in an effort to determine which patients would progress less rapidly and therefore have a better chance of benefiting from our immunotherapy based approach.

The table below compares the inclusion criteria from randomized Phase 2 trial to the Phase 3 PROSPECT trial.

Phase 3 PROSPECT Trial Selects Patients with Less Advanced mCRPC Compared to
the Randomized Phase 2 Trial

The trial is powered to detect a difference in OS between active treatment and placebo at final analysis. Furthermore, three pre-specified interim analyses of data have been integrated into the statistical plan to evaluate whether the trial should continue as planned or potentially be stopped early for efficacy or futility. If stopped early for efficacy, a Biologics License Application, or BLA, may be filed at an earlier stage, potentially shortening the overall development time. The PROSPECT trial is event driven and is fully enrolled as of January 2015. We anticipate reporting top-line data in 2017.

PROSTVAC is currently the subject of seven ongoing or planned NCI-sponsored Phase 2 clinical trials either in combination or expanded disease settings:

CV 301 is a cancer immunotherapy that targets two tumor-associated antigens, CEA and MUC-1, that are over-expressed in major cancer types, including lung, bladder and colorectal cancer. Similar to PROSTVAC, CV 301 uses a vaccinia prime, followed by multiple Fowlpox boosts, and encodes the TRICOM costimulatory molecules. CV 301 and its precursors have been tested in 6 ongoing or completed NCI-sponsored clinical trials in various cancers, and more than 300 patients have been treated with the product candidate. One trial, which investigated the effects of CV 301 in 74 patients with resected metastatic colorectal cancer, showed a significant survival benefit over a set of matched, controlled patients who were treated at Duke University. These matched, controlled patients were not enrolled in the trial, but were colorectal cancer patients undergoing approved therapies, and each group was evaluated to compare how OS differed.

A recent NCI project prioritized 75 cancer antigens by assigning a composite score based upon nine indicative features and found that MUC-1 and CEA were the second and thirteenth of 75 top key cancer antigens. The NCI continues to investigate CV 301 in various clinical settings as part of the CRADA signed in 2011. MUC-1 and CEA are present in 90% of colorectal cancers.

CV 301 is currently undergoing a clinical trial in bladder cancer at the NCI. We have continued to improve the CV 301 construct and expect to initiate production of new clinical trial material in the coming months in colorectal and bladder indications, among others. We plan to replace vaccinia with MVA-BN in an updated formula of CV 301, which we believe will improve its efficacy and production yield.

Combination treatments continue to play an important role in the rapidly changing cancer treatment paradigm. The synergistic clinical benefit seen with PROSTVAC in combination settings is believed also to apply to CV 301. Specifically, recent preclinical data provide a clear rationale for combining CV 301 with checkpoint inhibitors.

Checkpoint inhibitors have shown promising efficacy as single agent treatments in clinical trials in various cancers. However, the majority of cancer patients are not responding to checkpoint inhibitors, and this appears to be related to low or negative expression of programmed death-ligand 1, or PD-L1, a transmembrane protein that has been speculated to play a major role in suppressing the immune system. Low PD-L1 expression is widely defined as <5% PD-L1. This limited response is believed to be due in part to individual patients lacking an immune response to attack the tumors.

We believe CV 301 equips the immune system with the ability to seek out and destroy these tumors. Preclinical data shows the ability to upregulate PD-L1 by mounting an immune response against a tumor target. The upregulation of PD-L1 is a marker indicating the tumor is under attack from T-cells, presenting an opportunity for a greater response in patients who might otherwise not benefit from treatment with a checkpoint inhibitor alone.

Our strategy is to develop CV 301 for use in combination with checkpoint inhibitors. While we have rights to multiple indications for CV 301, the initial target will be NSCLC. Expression levels of CEA and MUC-1 in NSCLC are 70% and greater than 80%, respectively.

Lung cancer is the second most common cancer and is the leading cause of cancer death in the United States. Each year, more people die of lung cancer than of colon, breast and prostate cancers combined. About 85% of lung cancers are NSCLC, which has different subtypes, including squamous cell carcinoma, adenocarcinoma, and large cell carcinoma. Analysts estimate that the global market for NSCLC treatments will increase from $6.9 billion in 2014 to $10.9 billion in 2021.

About 70% of NSCLC patients are reported to have low or negative PD-L1 expression, which is often correlated to a lesser response to checkpoint inhibition. This presents a significant opportunity to deploy optimized combination immunotherapy regimens for broader treatment efficacy.

With this rationale for combining active immunotherapy with checkpoint inhibitors, we have selected NSCLC as the primary indication for the development of a treatment that combines CV 301 with a checkpoint inhibitor such as an anti-PD-1 agent. The objective is to improve the progression-free survival, which offers relatively fast generation of data. We expect to initiate a Phase 1 clinical trial in 2016.

In April 2014, an NCI-sponsored, randomized, prospective Phase 2 trial of CV 301 alone or in combination with Bacillus Calmette-Guerin, or BCG, for the treatment of bladder cancer was initiated.

CV 301 is thought to activate a potent antitumor immune response against bladder cancer cells that express the CEA and MUC-1 antigens.

The trial is designed to enroll 54 patients with high grade non-muscle invasive bladder cancer whose cancer has progressed after initial BCG treatment. The primary endpoint is to determine whether there is an improvement in disease-free survival for patients receiving CV 301 immunotherapy in combination with BCG treatment compared to those receiving BCG treatment alone.

While NSCLC represents the first clinical target in a combination regimen, starting in the second half of 2016 with lung cancer, we plan to initiate no less than three separate Phase 2 trials. We plan to initiate randomized, placebo-controlled studies in NSCLC, bladder cancer and colorectal cancer, in combination with assorted checkpoint inhibitors. These studies will evaluate the efficacy of the individual components, as well as the combination of the vaccine and a checkpoint inhibitor to determine what, if any, synergy can be seen in combination.

MVA-BN Brachyury is a cancer immunotherapy developed using our proprietary validated MVA-BN platform. It is designed to induce a robust T-cell immune response against brachyury. Brachyury, which is not expressed in most normal tissue, is reported to play a key role in the metastasis and progression of tumors. Tumors that overexpress brachyury are believed to be highly resistant to current therapies and are associated with decreased survival rates.

We completed an NCI-sponsored Phase 1 trial of MVA-BN Brachyury in patients with metastatic cancer or chordoma. The trial was an open-label, Phase 1 trial and enrolled 25 patients with metastatic cancer and 13 with chordoma into three cohorts with dose escalation of MVA-BN Brachyury. The initial phase was to establish safety at low doses in a limited number of patients. Once this was established, the remaining patients were enrolled at higher doses. The objective of the trial was to determine the safety and tolerability of escalating doses of MVA-BN Brachyury and to evaluate immunologic responses as measured by an increase in brachyury-specific T-cells. We reported data from this trial in November 2015. Data from this trial demonstrated for the first time that an MVA-BN based vaccine targeting brachyury can induce brachyury-specific T-cell immune responses in advanced cancer patients. MVA-BN Brachyury was well-tolerated with no dose limiting toxicities. The maximum tolerated dose was not reached and no serious adverse vaccine-related events were observed. Immune responses were analyzed in 29 patients. Brachyury-specific T-cell responses were observed at each dose level: more than 66% of patients at dose level 1, more than 80% at dose level 2, and more than 90% at dose level 3. At the two highest dose levels, approximately 80% of the patients that developed brachyury-specific T-cells demonstrated responses in both CD4 and CD8 T-lymphocytes.

As we have done in our other NCI collaborations, we will continue to support our partners in the advancement of this program. There appears to be clinical rationale to explore MVA-BN Brachyury in a number of solid tumor settings, to be used both in monotherapy and in combination therapy. Following the announcement of data from the Phase 1 trial, we look forward to working with the NCI as they develop additional clinical trials in this area. We retain exclusive rights to this program and will determine if and when a corporate partnership is appropriate.

We own and operate a fully integrated, highly scalable live virus vaccine production facility in Kvistgaard, Denmark, which we believe plays a key role in our vaccine production capabilities. In 2006, our approximately 100,000 square foot multiproduct production facility was approved by the European Authorities, specifically the Danish Medicines Agency, for cGMP production, which includes the production of sterile live virus vaccines, QC analysis, release and distribution. We have had numerous inspections by the EMA, NIH and BARDA. Our facility has been inspected by the EMA and the FDA without notice of any material deficiency and is used for the production of all of our current clinical candidates. To date, at our facility, we have produced and delivered 28 million doses of IMVAMUNE/IMVANEX as well as over 2 million doses of our MVA-BN Filo candidate for Ebola.

The plant has been designed and constructed to fulfill the strictest European Union, or EU, and U.S. requirements for the production of sterile live virus vaccines. The facility has also been designed to prevent the pollution of the environment with live virus vaccines through air emissions, water run-off, or by any other means. Our production facility is also approved to handle biosafety level 2, or BSL-2, genetically modified vaccines, such as PROSTVAC.

Our QC laboratory currently performs several of the cGMP regulated QC testing in connection with the production and release and stability testing of bulk drug substances and final drug product in filled, labelled and packaged vials, or FDPs. Moreover, the laboratory performs all environmental monitoring tests including the microbiological testing of water. Currently, the QC labs house approximately 20 laboratories and additional rooms for uses such as sample receipt, incubators, refrigerators and freezers and wash and sterilization.

We are currently implementing a small-scale filling line allowing for fill and pack of clinical trial material and commercial supply for low to mid volume products. The filling machine has a capacity of producing 1,000 vials per hour. This allows us the flexibility to fill smaller batches directly at the facility in Kvistgaard, Denmark, thus reducing the time from raw material to FDP. IDT Biologika, our strategic partner in Dessau, Germany, handles the filling and packing of high volume products such as IMVAMUNE/IMVANEX. We are currently contemplating an expansion of our existing production facility to handle filling and packing of certain products.

We have an approximately 45,000 square foot research and development facility, which is scheduled to increase to approximately 55,000 square feet on January 1, 2016, in Martinsried, Germany, which includes laboratories and the FDA's Good Laboratory Practice, or GLP, compliant animal facility. All laboratories and support areas, such as the bacteriology labs, liquid nitrogen and freezer storage areas, meet the requirements for BSL-2 classification and all equipment meets the requirements for Genetically Modified Organism class 2 specifications, as required by local and national authorities.

The selling and distribution of IMVAMUNE/IMVANEX is carried out by our sales organization in combination with local and regional agents and distributors who possess experience in dealing with contracts with public authorities. As of November 27, 2015, our sales organization consisted of five people, who are based in Kvistgaard, Denmark and Singapore. Our current sales and distribution efforts are primarily directed at ministries of defense and health, which are prepared to update their emergency vaccine stocks. To the extent that PROSTVAC and MVA-BN Filo receive approval by the

applicable regulatory agencies for marketing and distribution, BMS and Janssen, respectively, will be responsible for sales and distribution of those products.

A number of raw materials and sterile single-use devices are used to produce our products and product candidates. Some of the raw materials are biosimilar materials that are also used by other pharmaceutical producers, while others are produced specifically for our use, either due to special quality requirements or to the packaging in which they are supplied. The sterile single-use devices are predominantly custom-made for us.

To the extent possible, we aim to have at least two suppliers of critical raw materials. When this is not possible, the aim is for the raw materials to be produced by an alternative supplier, at some delay, if the primary supplier should fail to deliver. If a primary supplier fails to deliver or delivers less of a critical raw material than agreed, it will typically take three to six months before an alternative supplier will be able to supply raw materials of the same quality. Consequently, supplier failure may cause production delays of three to six months. Where possible, we seek to safeguard against this risk by maintaining fairly large raw material inventories.

Our most critical biosimilar raw material is specific pathogen-free, or SPF, eggs, which are laid by selected chicken strains that are kept disease-free and un-vaccinated. The chicken flock is regularly examined for a number of micro-biological diseases that may be caused by virus, virus bacteria or other microorganisms. The production, shipment, receipt and examination of such SPF eggs is subject to European pharmaceutical legislation. On a global basis, very few egg producers comply with the special SPF requirements. We use three suppliers, two of which are part of the same corporation, which operates chicken farms in both the United States and Europe. The third supplier is a European egg producer. We have verified that eggs from all three suppliers are fully useable for producing the IMVAMUNE/IMVANEX vaccine. In order to further reduce the risk of production delays or stops in case of infections in the stock of chicken, we use eggs from a number of different chicken flocks from two of the three suppliers. We use eggs from different flocks from one production day to the next in order to reduce the risk of losing a product in case of infection in a given flock.

Collaborative agreements with other biopharmaceutical and biotechnology companies and production partners form an integral part of our business. We will endeavor to retain our current partners and enter into new agreements or partnerships. Following is a summary of our outstanding material contracts.

On March 4, 2015, we entered into an option and license agreement with BMS, or the BMS agreement, with BMS obligated to make a $60 million upfront payment to us and subsequent milestone payments to us of up to an aggregate of $915 million. BMS may also be obligated to make royalty payments to us in a percentage ranging from the to potentially the . The BMS agreement provides BMS an exclusive option to license and commercialize PROSTVAC globally.

Under the terms of the BMS agreement, we received an upfront payment of $60 million and could be entitled to a payment of $80 million upon exercise of the option, which BMS may exercise in its sole discretion within a designated time after data from the ongoing Phase 3 trial is available.

In addition, we could be entitled to additional incremental payments starting at $50 million, but with a potential to exceed $230 million should the median OS benefit of PROSTVAC exceed the efficacy seen in Phase 2 results.

Furthermore, we could receive regulatory milestone payments of an aggregate of $110 million, up to an aggregate of $495 million in sales milestones as well as the royalty payments described above on future sales of PROSTVAC.

BMS's royalty obligations under the BMS agreement will terminate when (1) the term during which BMS may exercise its option expires and it cannot be reinstated or (2) on a product-by-product and country-by-country basis, on the latest of (a) the twelfth anniversary of the first commercial sale of such product in such country, (b) the expiration in such country of the last valid claim of the last-to-expire product specific patents that would be infringed by the sale of such product in such country absent a license with respect to such product specific patent and (c) the expiration of applicable regulatory exclusivity as to such product in such country. Certain of BMS's royalty obligations may be automatically extended on a country-by-country basis for the period during which we supply BMS with products under our supply contract with BMS (described below). BMS may terminate the BMS agreement at will or for safety reasons, subject to certain notice requirements. We or BMS may terminate the BMS agreement for material breach or insolvency, subject to certain notice requirements and cure periods.

Prior to BMS's exercise of its option under the BMS agreement, we have agreed to bear patent prosecution costs with respect to the intellectual property governed by such agreement, subject to certain exceptions. Upon and after any exercise by BMS of such option, BMS has agreed to bear the patent prosecution costs with respect to such intellectual property, subject to certain exceptions. BMS's obligation to bear these patent prosecution costs may be delayed if BMS's exercise of its option triggers an obligation to make certain antitrust regulatory filings.

We have also agreed to enter into a supply contract with BMS effective upon BMS's exercise of its option pursuant to which we will undertake the future commercial production of PROSTVAC.

We have also agreed with BMS to perform a trial of the combination of PROSTVAC with one of BMS's cancer immunotherapy candidates following long-term survival data from a combination study of PROSTVAC and ipilimumab, which indicated potential synergy. The trial is anticipated to start by early 2016 and will be conducted by UCSF.

Agreements with Janssen Regarding MVA-BN Filo and Additional Infectious Disease

On October 22, 2014, we entered into a collaboration and license agreement with Crucell Holland B.V., one of the Janssen Pharmaceutical Companies of Johnson & Johnson within the field of Filoviruses, or Janssen. Under the terms of the collaboration and license agreement, we granted Janssen an exclusive license for our multivalent MVA-BN Filo vaccine candidate in combination with Janssen's adenovirus vector based Filo vaccine candidate. We received an upfront payment of $25 million and are entitled to receive up to $20 million in sales, development and regulatory milestones, in addition to potential for royalties on commercial sales at certain price levels outside Africa, where we have elected not to receive royalties. Janssen will be fully responsible for all costs associated with the further development and commercialization of the vaccine candidate.

The collaboration and license agreement and Janssen's royalty obligations under such agreement will terminate on a product-by-product and territory-by-territory basis fifteen years after the first commercial sale of such product in such territory. During development and commercialization, Janssen may terminate the collaboration and license agreement for convenience, subject to a notice requirement. Janssen may elect to terminate the collaboration and license agreement upon a change of control if we are acquired by a competitor of Janssen. If Janssen does not elect to terminate the collaboration and license agreement upon a qualifying change in control, Janssen may terminate certain provisions of the agreement and we are obligated to license the right to manufacture certain of our vaccine vectors to Janssen. We or Janssen may terminate the collaboration and license agreement for material breach, default in the performance of a material obligation, insolvency or bankruptcy, subject to certain notice requirements and cure periods.

Furthermore, pursuant to a development and supply agreement with Janssen, we have agreed to produce bulk vaccine anticipated to yield approximately 2,000,000 doses of MVA-BN Filo based on an agreed number of production batches, for which we have received an initial payment of $71 million and will receive additional $28 million pro rata with deliveries in 2015. The supply agreement automatically terminates upon the completion of the manufacturing plan or the termination of the collaboration and license agreement. Janssen may terminate the supply agreement for convenience, subject to a notice requirement. Janssen may elect to terminate the supply agreement upon a change of control if we are acquired by a competitor of Janssen. We or Janssen may terminate the supply agreement for material breach, default in the performance of a material obligation, insolvency or bankruptcy, subject to certain notice requirements.

Additionally, in connection with the above agreements, Johnson & Johnson Development Corporation made a $43 million equity investment in our company, thus at that time obtaining nearly a 5% ownership in our company.

In emergency outbreak situations such as the recent Ebola outbreak in Western Africa, the collaboration and license agreement does not preclude us from collaborating with other parties in the development and supply of Ebola vaccines for preclinical studies and clinical trials.

We and Janssen subsequently agreed to collaborate on the evaluation of MVA-BN for three additional infectious disease targets. Janssen has been granted the exclusive option to collaborate on one or more of the targets following the preclinical evaluation of MVA-BN-based vaccine candidates, which we will develop.

On December 18, 2015, we entered into a second collaboration and license agreement with Janssen Pharmaceuticals Inc. Under the terms of the collaboration and license agreement, we granted to Janssen exclusive rights to our MVA-BN technology for use in a prime-boost vaccine regimen together with Janssen's adenovirus vector based Filo candidate with the purpose of targeting all cancers induced by human papillomavirus (HPV), one of the three additional infectious disease targets under our material evaluation agreement with Janssen. We are entitled to an initial upfront payment of $9 million. In addition, we are entitled to receive up to $162 million in sales, development and regulatory milestones, in addition to single-digit tiered royalties on commercial sales. Janssen will be responsible for all costs associated with development, subject to certain exceptions. We will undertake all manufacturing related to MVA-BN, subject to certain exceptions. Janssen retains an exclusive option to license MVA-BN for two additional undisclosed infectious disease targets.

The collaboration and license agreement and Janssen's royalty obligations under the agreement will terminate on a product-by-product and territory-by-territory basis twelve years after the first

commercial sale of such product in such territory or the expiration of the patent rights with respect to such product, whichever occurs later. Janssen may terminate the collaboration and license agreement for convenience or serious safety reasons, subject to a notice requirement. Janssen may also terminate our rights and obligations under this agreement, with certain exclusions, in the event we materially breach this agreement, subject to a notice and cure period requirement. We or Janssen may terminate the collaboration and license agreement for material breach, default in the performance of a material obligation, insolvency or bankruptcy, subject to certain notice requirements and cure periods, and upon certain other specified events.

In June 2007, BARDA, a division of the Department of Health and Human Services, or HHS, awarded us a contract, which we refer to as RFP-3, for the production and delivery of, initially, 20 million doses of liquid frozen IMVAMUNE/IMVANEX for the protection of persons considered to be at risk for smallpox. This RFP-3 contract has over the years been amended, expanded and prolonged several times and currently is set to expire on June 3, 2017. As examples of material amendments and modifications, we announced on April 16, 2013 that BARDA had expanded the initial order for 20 million doses of IMVAMUNE/IMVANEX with an additional order for 4 million doses of IMVAMUNE/IMVANEX and an option for additional 4 million doses that was subsequently exercised and announced on September 4, 2014. As of early 2015, we have produced and delivered to BARDA all of the 28 million doses of IMVAMUNE/IMVANEX that have been ordered.

In addition to the production and delivery of the 28 million doses of IMVAMUNE/IMVANEX, the RFP-3 contract also supports the funding of preclinical studies and clinical trials that will be necessary for our BLA submission to the FDA. Furthermore, on July 7, 2015 we announced that BARDA had ordered a bulk supply of IMVAMUNE/IMVANEX, valued at $133 million. Under this new order, which is an extension of the existing RFP-3 contract, we will produce and store a bulk supply of IMVAMUNE/IMVANEX. This bulk material could be converted into a freeze dried formulation of IMVAMUNE/IMVANEX at a later date, once the freeze-drying production process has been transferred to a commercial line, and is approved by the U.S. authorities. This bulk IMVAMUNE/IMVANEX order is expected to be produced and recognized as revenue in 2016 and 2017.

The total value of the RFP-3 contract constitutes $911 million, of which we had received $763 million as of September 30, 2015.

BARDA is entitled to terminate the RFP-3 contract at its convenience in accordance with standard federal acquisition regulation, or FAR, provisions against reimbursement of costs already incurred and as agreed and negotiated by BARDA and us. This is standard in procurement contracts with U.S. authorities and the contract is in general regulated by usual standard FAR provisions.

In November 2009, BARDA awarded us a contract for the development of a freeze dried formulation of IMVAMUNE/IMVANEX with a total prospective initial value of $40 million. The contract provides funds to validate the new freeze dried production process and the associated preclinical studies and clinical trials to support the advanced development of a freeze dried formulation of IMVAMUNE/IMVANEX instead of the existing liquid frozen formulation of IMVAMUNE/IMVANEX.

This contract related to the freeze dried formulation of IMVAMUNE/IMVANEX has over the years been amended, expanded and prolonged several times and is currently having an expiration date of November 15, 2016. As examples of material amendments and modifications we announced in April 2011, that BARDA increased the potential value of the existing contract from $40 million to $94 million. The increased funding supported additional studies and production activities to further advance the development of the freeze dried formulation of IMVAMUNE/IMVANEX by the end of the

contract period. On April 22, 2014 we announced that BARDA had exercised an option at a value of $22 million under the existing contract. This option was exercised in order to fund the transfer of the already validated filling and packaging production process to a commercial production line with a larger capacity.

The total potential value of this contract related to freeze dried IMVAMUNE/IMVANEX constitutes $94 million, of which we had received $60 million as of September 30, 2015.

BARDA is entitled to terminate the contract at its convenience in accordance with standard FAR provisions against reimbursement of costs already incurred and as agreed and negotiated by BARDA and us. This is standard in procurement contracts with U.S. authorities and the contract is in general regulated by usual standard FAR provisions.

In August 2008, we entered into a CRADA with the NCI, pursuant to which we and the NCI will jointly develop new immunotherapies for the prevention and treatment of prostate cancer. Under the CRADA, we have rights to exclusively license intellectual property resulting from this collaboration, subject to a nonexclusive, nontransferable, irrevocable license to the U.S. government to practice throughout the world of research or other U.S. government purposes. The term of the CRADA was initially five years, but has been extended for an additional five years and the agreement now expires on August 12, 2018, unless otherwise agreed. The CRADA may be terminated by mutual consent at any time or by either party. The CRADA may be terminated unilaterally by either party, subject to certain notice requirements. Clinical trials performed under the CRADA are based on a joint development plan between us and the NCI.

In connection with the CRADA, in August 2008, we entered into a license agreement with the PHS under which we were granted a license to certain intellectual property related to the development of PROSTVAC. The license agreement divides the licensed patent portfolio into (i) exclusively and (ii) non-exclusively licensed patents and patent applications. Under the license agreement, we have paid an aggregate of $7 million in license issue payments and sublicensing milestones, and we may be required to pay up to an aggregate of approximately $17 million in future milestone payments. In addition, we may be obligated to pay up to 75% of certain patent prosecution expenses incurred after February 16, 2007. We may also be obligated to make royalty payments to PHS as a percentage of net sales in the single digits. The license agreement will expire upon the expiration of the last patent contained in the licensed patent rights, unless terminated earlier. The PHS may terminate or modify the license agreement in the event of a material breach, including, if we are not executing the commercial development plan, if we do not meet certain milestones by certain dates, if we are unable to satisfy unmet health and safety needs, or upon certain insolvency events that remain uncured, in each case following certain notice periods. We may terminate the license agreement, or any portion thereof, at our sole discretion at any time, subject to certain notice requirements and cure periods. In addition, the PHS has the right to require us to sublicense the rights to the product candidates covered by the license agreement upon certain conditions, including if we are not reasonably satisfying required health and safety needs or if we are not satisfying requirements for public use as specified by federal regulations.

In October 2011, we expanded our scientific partnership with the NCI, entering into a second CRADA. Under the second CRADA, we and the NCI will jointly develop new product candidates for the prevention and treatment of multiple cancer indications, including further development of CV 301 and brachyury.

Under the second CRADA, we and the NCI will collaborate on the preclinical and clinical development of recombinant pox-virus based immunotherapies for the treatment and prevention of breast, lung, ovary, liver, gastric system, bladder, kidney and pancreatic cancer.

Under the second CRADA, we have rights to exclusively license intellectual property that results from this collaboration, subject to a nonexclusive, nontransferable, irrevocable license to the U.S. government to practice throughout the world of research or other U.S. government purposes. The second CRADA runs for an initial period of five years, expiring on October 3, 2016. The second CRADA may be terminated by mutual consent at any time or by either party subject to certain notice requirements. Clinical trials performed under the second CRADA are based on a joint development plan between us and the NCI.

In connection with the second CRADA, in October 2011, we entered into a license agreement with the PHS under which we were granted a license to certain intellectual property rights related to the treatment and prevention of breast, lung, ovary, liver, gastric system, bladder, kidney and pancreatic cancer. The license agreement with the PHS will expire upon the expiration of the last patent contained in the licensed patent rights, unless terminated earlier. The PHS may terminate or modify the license agreement in the event of a material breach, including if we do not meet certain milestones by certain dates, if we are unable to satisfy unmet health and safety needs, or upon certain insolvency events that remain uncured, in each case following certain notice periods and cure periods. We may terminate the license, or any portion thereof, at our sole discretion at any time, subject to certain notice requirements. In addition, the PHS has the right to require us to sublicense the rights to the product candidates covered by the license upon certain conditions, including if we are not reasonably satisfying required health and safety needs or if we are not satisfying requirements for public use as specified by federal regulations.

Furthermore, in May 2013, we entered into an additional license agreement with NIH under which we were granted a license to certain intellectual property rights related to treatment and prevention of colorectal cancer. The license agreement with NIH will expire upon expiration of the last patent contained in the licensed patent rights, unless terminated earlier. The NIH may terminate or modify the license in the event of a material breach, including, if we are not executing the commercial development plan, if we do not meet certain milestones by certain dates, if we are unable to satisfy unmet health and safety needs, or upon certain insolvency events that remain uncured, in each case following certain notice periods. We may terminate the license, or any portion thereof, at our sole discretion at any time, subject to certain notice requirements and cure periods. In addition, the NIH has the right to require us to sublicense the rights to the product candidates covered by the license upon certain conditions, including if we are not reasonably satisfying required health and safety needs or if we are not satisfying requirements for public use as specified by federal regulations.

The license agreements with the PHS and NIH divide the licensed patent portfolio into (i) exclusively and (ii) non-exclusively licensed patents and patent applications. Under the license agreement with PHS, we have paid an aggregate of approximately $3 million in license issue payments and we may be required to pay up to an aggregate of approximately $13 million in future milestone payments. In addition, we may be obligated to pay up to 50% of patent prosecution expenses incurred. We may also be obligated to make royalty payments to PHS as a percentage of net sales in the single digits. Under the license agreement with NIH, we have paid an aggregate of $1 million in license issue payments and we may be required to pay up to an aggregate of approximately $5 million in future milestone payments. In addition, we may be obligated to pay up to 50% of patent prosecution expenses incurred. We may also be obligated to make royalty payments to NIH as a percentage of net sales in the single digits.

The pharmaceutical and biotechnology industries are characterized by rapidly advancing technologies and intense competition. While we believe that our live virus vaccine platform, development expertise, manufacturing experience and scientific knowledge provide us with competitive advantages, we face potential competition from many different sources, including major pharmaceutical, specialty pharmaceutical and biotechnology companies, academic institutions and governmental agencies and public and private research institutions. Any drug candidates that we successfully develop and commercialize will compete with existing drugs and new drugs that may become available in the future.

We compete in the areas of biodefense, commercial vaccines and treatments for infectious disease indications and immunotherapies for the treatment of cancer. Our vaccines and vaccine candidates are protected by intellectual property agreements that we own or license from third parties, and therefore are protected from competition as to the particular vaccines that we produce for the applicable indications that we target for the life of the applicable patent. However, many companies offer pharmaceutical products that may address one or more indications that our vaccines target. Furthermore, many of the companies against which we are competing or against which we may compete in the future have significantly greater financial resources and expertise in research and development, manufacturing, pre-clinical testing, conducting clinical trials, obtaining regulatory approvals and marketing approved drugs than we do. Mergers and acquisitions in the pharmaceutical and biotechnology industries may result in even more resources being concentrated among a smaller number of our competitors. Smaller or early stage companies may also prove to be significant competitors, particularly through collaborative arrangements with large and established companies.

Our commercial opportunities could be reduced or eliminated if our competitors develop and commercialize vaccines that are safer, more effective, have fewer or less severe side effects, are more convenient or are less expensive than any vaccines that we or our collaborators may develop. Our competitors also may obtain FDA or other regulatory approval for their drugs more rapidly than we may obtain approval for ours, which could result in our competitors establishing a strong market position before we or our collaborators are able to enter the market. The key competitive factors affecting the success of all of our drug candidates, if approved, are likely to be their efficacy and safety.

Other companies that compete for government contracts to develop, manufacture and commercialize vaccines for potential bioterror threats include, but are not limited to, AstraZeneca plc, Emergent BioSolutions, Inc., GlaxoSmithKline plc, Merck & Co., Inc., Pfenex Inc. and SIGA Technologies, Inc.

Other companies that compete to develop, manufacture and commercialize vaccines for the prevention and treatment of infectious diseases include, but are not limited to, Johnson & Johnson, Dynavax Technologies Corporation, GenVec, Inc., Genocea Biosciences, Inc., Inovio Pharmaceuticals, Inc., Merck & Co. Inc., Novartis Pharma AG, Novavax, Inc. and Sanofi.

Other companies that compete to develop, manufacture and commercialize immunotherapies for the treatment of cancer include, but are not limited to, Advaxis, Inc., Aduro Biotech, Inc., BMS, Celldex Therapeutics, Inc., Inovio Pharmaceuticals, Inc., Juno Therapeutics, Inc., Merck & Co. Inc., NEON Therapeutics, Novartis AG, Replimune Ltd and Transgene SA.

Our intellectual property assets, or IP, primarily include patents and patent applications, trademarks and trade secrets. It is our continuous objective to manage our IP in line with our overall strategy, which has resulted in the accumulation of a significant patent portfolio directed at the various technologies and products. As our business and technology has matured, our internal organization, with the support of experienced external professionals, has strived to focus the patent portfolio so that it reflects our commercial endeavors.

Our commercial success depends in part on our ability to obtain and maintain proprietary protection for our drug candidates, novel discoveries, product development technologies and other know-how, to operate without infringing on the proprietary rights of others, and to prevent others from infringing our proprietary rights. Our policy is to seek to protect our proprietary position by, among other methods, filing or in-licensing U.S. and foreign patents and patent applications related to our proprietary technology, inventions and improvements that are important to the development and implementation of our business. We also rely on trademarks, trade secrets, know-how, continuing technological innovation and potential in-licensing opportunities to develop and maintain our proprietary position.

While we seek broad coverage under our existing patent applications, there is always a risk that an alteration to the process may provide sufficient basis for a competitor to avoid infringement claims. In addition, patents, if granted, expire and we cannot provide any assurance that any patents will be issued from our pending or any future applications or that any potentially issued patents will adequately protect our intellectual property.

Our IP policy targets the protection of new technologies and products by filing relevant patent applications and by prosecuting these to obtain patent protection in all countries considered major or key markets for the corresponding technology or relevant products. The goal of obtaining and maintaining a commercially strong patent portfolio must be weighed against the often significant expenses involved in obtaining and maintaining patents.

Factors influencing the patent filing decisions include relevant commercial markets and value of the technology and/or products, production possibilities and markets where the technology and/or products are likely to be infringed. Patent applications we prosecute that cover primary technologies and products are therefore filed in most markets. Defensive patenting and applications covering add-on protection to the core patents are usually filed in certain markets only, which markets are selected based on the relevance of protection in the individual market to our overall business. As part of the strategic considerations, we weigh the benefits of seeking patent protection against the benefits of protecting new technologies as trade secrets, or know-how, based on the circumstances.

Individual patents extend for varying periods depending on the date of filing of the patent application or the date of patent issuance and the legal term of patents in the countries in which they are obtained. Generally, patents issued for regularly filed applications in the United States are effective for 20 years from the earliest effective filing date. In addition, in certain instances, a patent term can be extended to recapture a portion of the U.S. Patent and Trademark Office, or the USPTO, delay in issuing the patent as well as a portion of the term effectively lost as a result of the FDA regulatory review period. However, with respect to the FDA component, the restoration period cannot be longer than five years and the total patent term including the restoration period must not exceed 14 years following FDA approval. The duration of foreign patents varies in accordance with provisions of applicable local law, but typically is also 20 years from the earliest effective filing date. In Europe, Supplementary Protection Certificates, or SPCs, extend patent protection for up to five

years to compensate for the years lost in the regulatory process associated with application for marketing authorization, or MA. The actual protection afforded by a patent varies on a product by product basis, from country to country, and depends upon many factors, including the type of patent, the scope of its coverage, the availability of regulatory-related extensions, the availability of legal remedies in a particular country, and the validity and enforceability of the patent.

Furthermore, we rely upon trade secrets, or know-how, and continuing technological innovation to develop and maintain our competitive position. We seek to protect our proprietary information in part using confidentiality agreements with our commercial partners, collaborators, employees and consultants, and invention assignment agreements with our employees. We also have confidentiality agreements or invention assignment agreements with our commercial partners and selected consultants. These agreements are designed to protect our proprietary information and, in the case of the invention assignment agreements, to grant us ownership of technologies that are developed through a relationship with a third party. These agreements may be breached, and we may not have adequate remedies for any breach. In addition, our trade secrets may otherwise become known or be independently discovered by competitors. To the extent that our commercial partners, collaborators, employees and consultants use intellectual property owned by others in their work for us, disputes may arise as to the rights in related or resulting know-how and inventions. For more information, please see "Risk Factors—Risks Related to Our Intellectual Property."

Our commercial success will also depend in part on not infringing upon the proprietary rights of third parties. It is uncertain whether the issuance of any third-party patent would require us to alter our development or commercial strategies, or our drugs or processes, obtain licenses or cease certain activities. Our breach of any license agreements or failure to obtain a license to proprietary rights that we may require to develop or commercialize our future products may have a material adverse impact on us. If third parties prepare and file patent applications in the United States that also claim technology to which we have rights, we may have to participate in interference proceedings in the USPTO, to determine priority of invention. For more information, please see "Risk Factors—Risks Related to Our Intellectual Property."

We have successfully built our patent portfolio on and around our core technology, MVA-BN. The Company has acquired exclusive rights to material IP covering PROSTVAC. Further, we have obtained protection for, and continue to file further applications to protect relevant supporting technologies.

Our patent portfolio consists of more than 60 patent families, which are company-owned or in-licensed, many of which consist of numerous issued/granted patents and pending applications. As of November 24, 2015, the patent portfolio comprises more than 740 granted/issued patents and more than 240 pending patent applications.

Our competitive IP protection gives exclusive rights to produce, sell and market our MVA-based technology globally. Our exclusive rights cover certain aspects of recombinant MVA vaccines for cancer and infectious disease indications created by inserting foreign genes into the MVA genome. In addition, we have acquired exclusive rights to non-MVA technologies, including other viruses and production processes.

Ten U.S. patents have been granted within the patent family covering the MVA virus variant referred to as MVA-BN, with terms expiring between 2020 and 2021, excluding any extensions awarded based on regulatory review. U.S. Patent No. 6,761,893 covers the MVA-BN virus and derivatives thereof, and the use as a vector technology for recombinant MVA-based vaccines.

Together with U.S. Patent No. 6,913,752, this patent family covers the use of the MVA-BN technology for generating immunity in healthy and immunocompromised individuals and priming and boosting vaccination regimes: U.S. Patent No. 7,189,536 relates to prime-boost methods and the use of the virus as an adjuvant composition; U.S. Patent No. 7,335,364 specifies the biological characteristics of the MVA-BN technology; and U.S. Patent No. 7,384,644 relates to the virus and pharmaceutical compositions and methods for the induction of protective immunity against a lethal vaccinia virus infection. U.S. Patent No. 7,459,270 includes claims to methods of generating the MVA-BN virus, to the virus itself and to kits comprising the virus. U.S. Patent No. 8,268,325 further includes claims to a method of generating recombinant MVA-BN viruses and vaccines. Methods of inducing or generating an immune response are included in U.S. Patent Nos. 7,923,017, 7,939,086, and 8,268,329. Corresponding European patent EP 1 335 987 was validated in 25 European countries plus Brunei. There are corresponding patents in Australia, Belarus, Canada, China, Hong Kong, the Czech Republic, Estonia, Hungary, Indonesia, Israel, India, Japan, South Korea, Mexico, New Zealand, the Philippines, Poland, Russia, Singapore, Ukraine, and Vietnam. There are pending applications in Brazil, South Korea, Norway and the United States.

Additional patent protection includes the use of MVA-derived vaccinia viruses for inducing a general immune stimulation, including the use of MVA-BN for protection against smallpox in neonates, or young children with an immature immune system. Patents in this family expire in 2021-2023, excluding any extensions awarded based on regulatory review. Use of MVA-BN and derivatives thereof to induce a rapid immune response has also been patented. Patents in this family expire in 2026, excluding any extensions awarded based on regulatory review. Another patent family relates the insertion of foreign genes into intergenic regions. There are eight issued U.S. patents and several foreign patents relating to this technology. Patents in this family will expire in 2022 to 2024, excluding any extensions awarded based on regulatory review. Another patent family relates to recombinant poxvirus vector capable of expressing two or more homologous foreign sequences, which derive from different variants of a microorganism. This family includes patents expiring in 2022 to 2023, excluding any extensions awarded based on regulatory review. There are issued patents in Australia, Canada, China, Europe, Hong Kong, Indonesia, Israel, India, Japan, Korea, Mexico, Norway, New Zealand, the Philippines, Singapore, Ukraine, the United States, Vietnam, and Eurasia. There are pending applications in Brazil, Canada, Indonesia, the Philippines, Poland, China and Hong Kong.

Methods for the cultivation of primary cells and for the amplification of viruses under serum free conditions have been patented, with terms expiring 2022 to 2025. Another patent family relates to the purification of vaccinia virus based vaccines, with a term expiring in 2028.

Intellectual property relating to MVA-vaccine products includes patent families relating to Ebola and RSV vaccines, including claims directed to heterologous prime boost regimens. One Ebola application was filed jointly with Janssen. If issued, patents resulting from these applications would expire in 2035, excluding any extensions awarded based on regulatory review. RSV patents would expire in 2033, excluding any extensions awarded based on regulatory review.

Cancer vaccines, covering the HER2-Neu DNA AutoVac construct and related technology, include two patent families with terms expiring 2027 to 2033, excluding any extensions awarded based on regulatory review.

Our wholly owned subsidiary in-licensed a number of patents and patent applications pertaining to PROSTVAC owned by the PHS. The licensed territory is worldwide, and the licensed patents are being prosecuted by the PHS in relevant major markets. We will file additional patent applications during the future development cycle when appropriate, which will be owned solely by us or co-owned with the PHS, depending on the circumstances of the particular development efforts. The core PSA patents expire 2015 to 2023, excluding any extensions awarded based on regulatory review.

The core patents relate to the relevant PSA, PSA oligo-epitope peptides and analogs thereof used in PROSTVAC, including various immunogenic compositions comprising the relevant PSAs and pox virus vectors expressing peptide agonists of PSA.

U.S. Patents relate to PSA oligo-epitope peptides and the generation of cellular and humoral immune responses to a mammalian PSA. Specific patents cover a PSA oligo-epitope peptide useful in generating PSA specific T lymphocytes for prevention or treatment of prostate cancer. A PSA epitope peptide which conforms to one or more human leukocyte antigens, or HLA, class I motifs, where the PSA oligo-epitope peptide, in combination with various HLA class I molecules or through interactions with various T-cell receptors, elicits PSA specific cellular immune responses. For example, the PSA oligo-epitope peptide is useful as an immunogen in the prevention or treatment of prostatic cancer, in the inhibition of prostatic cancer cells and in the establishment and characterization of PSA-specific cytotoxic T-cell lines. Another patent family relates to using a recombinant viral vector, preferably a poxvirus vector having at least one insertion site containing a DNA segment encoding PSA or a cytotoxic T-cell eliciting epitope thereof, operably linked to a promoter capable of expression in the host, to generate a specific humoral and cellular immune response to PSA. The method can include introducing a sufficient amount of the recombinant pox virus vector into a host to stimulate the immune response, and contacting the host with additional PSA at periodic intervals thereafter.

Another patent family relates to the generation of immune responses to PSA and includes uses of the vaccination regimen using a prime-boost regime of first administering a first poxvirus vector followed by a second poxvirus vector in a formulation that includes a costimulatory molecule. One patent family relates to peptide agonists of PSA and uses thereof. In various aspects, this family relates to peptides comprising agonist epitopes of the PSA-3 cytotoxic T lymphocyte epitope, and nucleic acids encoding peptides that comprise PSA-3 agonist epitopes. Relevant IP also relates to probes, primers, and vectors comprising these nucleic acids, as well as host cells comprising these vectors and antibodies that bind to the PSA-3 agonist peptides. Diagnostic tests, as well as methods of treatment or prevention of prostate cancer employing such compositions, for example, for peptide-mediated, cell-mediated, and vector-mediated immunotherapies are also covered.

In-licensed core patents include a patent family relating to various recombinant vectors expressing multiple costimulatory molecules and uses thereof, having claims relating to host cells and methods to enhance immune responses. More specifically, the family relates to recombinant poxviruses comprising foreign genes encoding at least the costimulatory molecules: one molecule from the B7 family, LFA-3 and ICAM-1, and optionally a foreign gene encoding at least one target antigen or immunological epitope, and uses as immunogens and vaccines. Another family relates to a composition of a recombinant virus expressing the antigen of the disease causing agent and a recombinant virus expressing an immunostimulatory molecule(s) such as, for example B7.1, B7.2,

IL-2 or GM-CSF for the purpose of generating an enhanced immune response to the disease causing agent.

Our portfolio also consists of several additional non-exclusively licensed patents and patent applications, including a patent family relating to novel insertion sites for introducing DNA into pox vectors, specifically a recombinant poxvirus containing and capable of expressing at least one foreign gene inserted at an insertion site within the poxvirus genome, including orthopox. Another family relates to recombinant poxviruses for immunization against tumor-associated antigens such as those encoded by the neu gene, the ros gene, the trk gene, the kit gene or an immunogenic portion thereof, and to vectors. Recombinant poxviruses capable of expressing cell-encoded, tumor-associated antigens are also disclosed. The recombinant viruses are useful for evoking an immune response against the antigen being expressed. Another family relates to recombinant FPVs capable of expressing immunogenic proteins of fowl pathogens. The recombinant FPV provide live virus vaccines for poultry and other animals.

Our core U.S. trademarks include IMVAMUNE/IMVANEX, the trade name for the smallpox vaccine product, and PROSTVAC the trade name for the prostate cancer vaccine candidate. An application for registration of the trademark PROSTVAC is pending in Europe and other relevant jurisdictions.

The current production process used for our MVA-BN-based vaccines, including the smallpox vaccine production, is primarily protected as a trade secret and is therefore not disclosed to competitors.

We enforced certain intellectual property rights, including the MVA-BN patents, against Acambis in 2005, and in 2007, reached a global settlement, ending the legal disputes on matters relating to smallpox vaccines based on the MVA virus. The settlement involved patent disputes at the U.S. International Trade Commission and the Commercial Court in Vienna, Austria, as well as the conversion, unfair trade acts and unfair competition action at the U.S. Federal District Court of the District of Delaware. Under the agreement, we granted a license to some of our MVA patents in return for Acambis making an undisclosed upfront payment. Acambis will also make royalty and milestones payments should it develop or commercialize certain MVA products in the future. Acambis was later acquired by Sanofi Pasteur.

We subsequently enforced the MVA-BN patents against Oxford BioMedica plc, BioMedica, Inc., and Oxford BioMedica Ltd., in the U.S. District Court of the Southern District of California. We and Oxford BioMedica reached a global settlement in 2010, ending the legal disputes between the parties on matters relating to MVA-BN. Under the agreement, we grant a license to MVA-BN patents in return for Oxford BioMedica making milestone payments and royalties. Further, Oxford BioMedica grants us a license to its heterologous prime-boost patents in return for our making milestone payments and paying royalties and a sub-license on licensed products, under poxvirus patents licensed to Oxford BioMedica by Sanofi-Aventis. Under the settlement, the terms of which are confidential, all pending litigation ceased and all oppositions filed at the European Patent Office by Oxford BioMedica were withdrawn.

Government authorities in the United States at the federal, state and local level and in other countries extensively regulate, among other things, the research, development, testing, production, QC, approval, labeling, packaging, storage, record-keeping, promotion, advertising, distribution, post-approval monitoring and reporting, marketing and export and import of drug and biological products, or biologics, such as our product candidates. Generally, before a new drug or biologic can be marketed, considerable data demonstrating its quality, safety and efficacy must be obtained, organized into a format specific to each regulatory authority, submitted for review and approved by the regulatory authority.

In the United States, the FDA regulates biologics under the Federal Food, Drug, and Cosmetic Act, or FDCA, and the Public Health Service Act, and their implementing regulations. Biologics are also subject to other federal, state and local statutes and regulations. The process of obtaining regulatory approvals and the subsequent compliance with appropriate federal, state, local and foreign statutes and regulations require the expenditure of substantial time and financial resources. Failure to comply with the applicable U.S. requirements at any time during the product development process, approval process or after approval, may subject an applicant to administrative or judicial sanctions. These sanctions could include, among other actions, the FDA's refusal to approve pending applications, withdrawal of an approval, imposition of clinical holds, sending of warning letters, product recalls or withdrawals from the market, product seizures, total or partial suspension of production or distribution injunctions, fines, refusals of government contracts, restitution, disgorgement, or civil or criminal penalties. Any agency or judicial enforcement action could have a material adverse effect on us.

Our product candidates must be approved by the FDA through the BLA process before they may be legally marketed in the United States. The process required by the FDA before a biologic may be marketed in the United States generally involves the following:

A sponsor must submit the results of the preclinical studies, together with production information, analytical data, any available clinical data or literature and a proposed clinical protocol, to the FDA as part of the IND. Long-term nonclinical studies, such as reproductive toxicity and carcinogenity in animals, may continue after an IND is submitted. The IND automatically becomes effective 30 days after receipt by the FDA, unless the FDA raises concerns or questions regarding the proposed clinical trials and places the IND on clinical hold within that 30-day time period. In such a case, the IND sponsor and the FDA must resolve any outstanding concerns before the clinical trial can begin. The FDA may also impose clinical holds on a product candidate at any time before or during clinical trials due to safety concerns or non-compliance.

The clinical stage of development involves the administration of the product candidate to healthy volunteers or patients under the supervision of qualified investigators, generally physicians not employed by or under the trial sponsor's control, in accordance with GCPs, which include the requirement that all research subjects provide their informed consent for their participation in any clinical trial. Clinical trials are conducted under protocols detailing, among other things, the objectives of the clinical trial, dosing procedures, subject selection and exclusion criteria, and the parameters to be used to monitor subject safety and assess efficacy. Each protocol, and any subsequent amendments to the protocol, must be submitted to the FDA as part of the IND. Further, each clinical trial must be reviewed and approved by an independent institutional review board, or IRB, at or servicing each institution at which the clinical trial will be conducted. An IRB is charged with protecting the welfare and rights of trial participants and considers such items as whether the risks to individuals participating in the clinical trials are minimized and are reasonable in relation to anticipated benefits. The IRB also approves the informed consent form that must be provided to each clinical trial subject or his or her legal representative and must monitor the clinical trial until completed. An IRB can suspend or terminate approval of a clinical trial at its institution if the clinical trial is not being conducted in accordance with the IRB's requirements or if the drug has been associated with unexpected serious harm to patients.

There are also requirements governing the reporting of ongoing clinical trials and completed clinical trial results to public registries. Sponsors of certain clinical trials of FDA-regulated products, including biologics, are required to register and disclose specified clinical trial information, which is publicly available at www.clinicaltrials.gov. Information related to the product, patient population, phase of investigation, study sites and investigators, and other aspects of the clinical trial is then made public as part of the registration. Sponsors are also obligated to discuss the results of their clinical trials after completion. Disclosure of the results of these trials can be delayed until the new product or new indication being studied has been approved. However, there are evolving rules and increasing requirements for publication of all trial-related information, and it is possible that data and other information from trials involving drugs and biologics that never garner approval could require disclosure in the future. In addition, publication policies of major medical journals mandate certain registration and disclosures as a pre-condition for potential publication, even if not currently mandated as a matter of law. Competitors may use this publicly available information to gain knowledge regarding the progress of development programs.

Clinical trials are generally conducted in three sequential phases that may overlap, known as Phase 1, Phase 2 and Phase 3 clinical trials. Phase 1 clinical trials generally involve a small number of healthy volunteers who are initially exposed to a single dose and then multiple doses of the product candidate. The primary purpose of these clinical trials is to assess the metabolism, pharmacologic action, side effect tolerability and safety of the product candidate and, if possible, to gain early evidence on effectiveness. Phase 2 clinical trials typically involve studies in disease-affected patients to determine the dose required to produce the desired benefits. At the same time, safety and further pharmacokinetic and pharmacodynamic information is collected, as well as

identification of possible adverse effects and safety risks and preliminary evaluation of efficacy. Phase 3 clinical trials generally involve large numbers of patients at multiple sites, in multiple countries (from several hundred to several thousand subjects) and are designed to provide the data necessary to demonstrate the efficacy of the product for its intended use, its safety in use, and to establish the overall benefit/risk relationship of the product and provide an adequate basis for product approval. Phase 3 clinical trials may include comparisons with placebo and/or other comparator treatments. The duration of treatment is often extended to mimic the actual use of a product during marketing. Generally, two adequate and well-controlled Phase 3 clinical trials are required by the FDA for approval of a BLA.

Post-approval trials, sometimes referred to as Phase 4 clinical trials, may be conducted after initial marketing approval. These trials are used to gain additional experience from the treatment of patients in the intended therapeutic indication. In certain instances, FDA may condition approval of a BLA on the sponsor's agreement to conduct additional clinical trials to further assess the biologic's safety and effectiveness after BLA approval.

Progress reports detailing the results of the clinical trials must be submitted at least annually to the FDA and written IND safety reports must be submitted to the FDA and the investigators for serious and unexpected suspected adverse, findings from other studies suggesting a significant risk to humans exposed to the drug, findings from animal or in vitro testing suggesting a significant risk to humans, and any clinically important rate increase of a serious suspected adverse reaction over that listed in the protocol or investigator brochure. Additionally, some clinical trials are overseen by an independent group of qualified experts organized by the clinical trial sponsor, known as a data safety monitoring board or committee. This group operates according to a charter and may advise the sponsor whether or not a trial should move forward at designated intervals based on access to certain data from the trial. We may also suspend or terminate a clinical trial based on evolving business objectives and/or competitive climate. Concurrent with clinical trials, companies usually complete additional animal studies and must also develop additional information about the chemistry and physical characteristics of the product candidate as well as finalize a process for producing the product in commercial quantities in accordance with cGMP requirements. The production process must be capable of consistently producing quality batches of the product candidate and, among other things, must develop methods for testing the identity, strength, quality and purity of the final product. Additionally, appropriate packaging must be selected and tested and stability studies must be conducted to demonstrate that the product candidate does not undergo unacceptable deterioration over its shelf life.

Following trial completion, trial data is analyzed to assess safety and efficacy. The results of nonclinical studies and clinical trials are then submitted to the FDA as part of a BLA, along with proposed labeling for the product and information about the production process and facilities that will be used to ensure product quality, results of analytical testing conducted on the chemistry of the product candidate, and other relevant information. The BLA must contain proof of safety, purity, potency and efficacy, which is demonstrated by extensive preclinical and clinical testing. The application must include all data relating to preclinical studies and clinical trials. To support marketing approval, the data submitted must be sufficient in quality and quantity to establish the safety and efficacy of the investigational product to the satisfaction of the FDA. FDA approval of a BLA must be obtained before a biologic may be marketed in the United States.

Under the Prescription Drug User Fee Act, or PDUFA, as amended, each BLA must be accompanied by a significant user fee, which is adjusted on an annual basis. PDUFA also imposes an annual product fee for human drugs and an annual establishment fee on facilities used to produce prescription drugs. Fee waivers or reductions are available in certain circumstances, including a waiver of the application fee for the first application filed by a small business.

The FDA has 60 days from its receipt of a BLA to determine whether the application will be accepted for filing based on the agency's threshold determination that it is sufficiently complete to permit substantive review. Once the submission is accepted for filing, the FDA begins an in depth review. The FDA has agreed to certain performance goals in the review of BLAs. Most such applications for standard review products are reviewed within ten to twelve months, while most priority review applications are reviewed in six to eight months. Priority review can be applied to drugs that the FDA determines offer major advances in treatment, or provide a treatment where no adequate therapy exists. For biologics, priority review is further limited only for products intended to treat a serious or life threatening disease relative to currently approved products. The review process for both standard and priority review may be extended by the FDA for three additional months to consider certain late submitted information, or information intended to clarify information already provided in the submission.

After the BLA submission is accepted for filing, the FDA reviews the BLA to determine, among other things, whether the proposed product candidate is safe and effective for its intended use, and whether the product candidate is being produced in accordance with cGMP to assure and preserve the product candidate's identity, strength, quality, purity and potency. The FDA may refer applications for novel drug product candidates or drug product candidates which present difficult questions of safety or efficacy to an advisory committee, typically a panel that includes clinicians and other experts, for review, evaluation and a recommendation as to whether the application should be approved and under what conditions. The FDA is not bound by the recommendations of an advisory committee, but it considers such recommendations carefully when making decisions. The FDA will likely re-analyze the clinical trial data, which could result in extensive discussions between the FDA and us during the review process. The review and evaluation of a BLA by the FDA is extensive and time-consuming and may take longer than originally planned to complete, and we may not receive a timely approval, if at all.

Before approving a BLA, the FDA will conduct a pre-approval inspection of the production facilities for the new product to determine whether they comply with cGMPs. The FDA will not approve the product unless it determines that the production processes and facilities are in compliance with cGMP requirements and adequate to assure consistent production of the product within required specifications. In addition, before approving a BLA, the FDA may also audit data from clinical trials to ensure compliance with GCP requirements. After the FDA evaluates the application, production process and production facilities, it may issue an approval letter or a Complete Response Letter. An approval letter authorizes commercial marketing of the product with specific prescribing information for specific indications. A Complete Response Letter indicates that the review cycle of the application is complete and the application will not be approved in its present form. A Complete Response Letter usually describes all of the specific deficiencies in the BLA identified by the FDA. The Complete Response Letter may require additional clinical data and/or an additional pivotal Phase 3 clinical trial(s), and/or other significant and time-consuming requirements related to clinical trials, preclinical studies or production. If a Complete Response Letter is issued, the applicant may either resubmit the BLA, addressing all of the deficiencies identified in the letter, or withdraw the application. Even if such data and information is submitted, the FDA may ultimately decide that the BLA does not satisfy the criteria for approval. Data obtained from clinical trials are not always conclusive and the FDA may interpret data differently than we interpret the same data.

There is no assurance that the FDA will ultimately approve a product for marketing in the United States and we may encounter significant difficulties or costs during the review process. If a product receives marketing approval, the approval may be significantly limited to specific populations, severities of allergies, and dosages or the indications for use may otherwise be limited, which could restrict the commercial value of the product. Further, the FDA may require that certain

contraindications, warnings or precautions be included in the product labeling or may condition the approval of the BLA on other changes to the proposed labeling, development of adequate controls and specifications, or a commitment to conduct post-market testing or clinical trials and surveillance to monitor the effects of approved products. For example, the FDA may require Phase 4 testing which involves clinical trials designed to further assess the product's safety and effectiveness and may require testing and surveillance programs to monitor the safety of approved products that have been commercialized. The FDA may also place other conditions on approvals including the requirement for a Risk Evaluation and Mitigation Strategy, or REMS, to assure the safe use of the product. If the FDA concludes a REMS is needed, the sponsor of the BLA must submit a proposed REMS. The FDA will not approve the BLA without an approved REMS, if required. A REMS could include medication guides, physician communication plans, or elements to assure safe use, such as restricted distribution methods, patient registries and other risk minimization tools. Any of these limitations on approval or marketing could restrict the commercial promotion, distribution, prescription or dispensing of products. Product approvals may be withdrawn for non-compliance with regulatory standards or if problems occur following initial marketing.

A sponsor may request an SPA, the purpose of which is to reach agreement with the FDA on the design of the Phase 3 clinical trial protocol and analysis that will form the primary basis of an efficacy claim. If such an agreement is reached, it will be documented and made part of the administrative record, and it will be binding on the FDA and may not be changed unless the sponsor fails to follow the agreed-upon protocol, data supporting the request are found to be false or incomplete, or the FDA determines that a substantial scientific issue essential to determining the safety or effectiveness of the drug was identified after the testing began. Even if an SPA is agreed to, approval of the BLA is not guaranteed because a final determination that an agreed-upon protocol satisfies a specific objective, such as the demonstration of efficacy, or supports an approval decision, will be based on a complete review of all the data in the BLA.

The Commissioner of the FDA, under delegated authority from the Secretary of the HHS may, under certain circumstances, issue an EUA that permits the use of an unapproved drug product or unapproved use of an approved drug product. Before an EUA may be issued, the Secretary must declare an emergency based on one of the following grounds:

In order to be the subject of an EUA, the FDA Commissioner must conclude that, based on the totality of scientific evidence available, it is reasonable to believe that the product may be effective in diagnosing, treating or preventing a disease attributable to the agents described above; that the

product's potential benefits outweigh its potential risks; and that there is no adequate, approved alternative to the product.

Although an EUA cannot be issued until after an emergency has been declared by the Secretary of HHS, the FDA strongly encourages an entity with a possible candidate product, particularly one at an advanced stage of development, to contact the FDA center responsible for the candidate product before a determination of actual or potential emergency.

Following approval of a new product, a producer and the approved product are subject to continuing regulation by the FDA, including, among other things, monitoring and recordkeeping activities, reporting to the applicable regulatory authorities of adverse experiences with the product, providing the regulatory authorities with updated safety and efficacy information, product sampling and distribution requirements, and complying with promotion and advertising requirements, which include, among others, standards for direct-to-consumer advertising, restrictions on promoting products for uses or in patient populations that are not described in the product's approved labeling (known as "off-label use"), limitations on industry-sponsored scientific and educational activities, and requirements for promotional activities involving the internet. Although physicians may prescribe legally available drugs and biologics for off-label uses, producers may not market or promote such off-label uses. Modifications or enhancements to the product or its labeling or changes of the site of production are often subject to the approval of the FDA and other regulators, which may or may not be received or may result in a lengthy review process. Prescription drug promotional materials must be submitted to the FDA in conjunction with their first use. Any distribution of prescription drug products and pharmaceutical samples must comply with the U.S. Prescription Drug Marketing Act, a part of the FDCA.

In the United States, once a product is approved, its production is subject to comprehensive and continuing regulation by the FDA. The FDA regulations require that products be produced in specific approved facilities and in accordance with cGMP. We rely, and expect to continue to rely, on third parties for the production of clinical and commercial quantities of our products in accordance with cGMP regulations. cGMP regulations require, among other things, QC and quality assurance as well as the corresponding maintenance of records and documentation and the obligation to investigate and correct any deviations from cGMP. Producers and other entities involved in the production and distribution of approved products are required to register their establishments with the FDA and certain state agencies, and are subject to periodic unannounced inspections by the FDA and certain state agencies for compliance with cGMP and other laws. Accordingly, producers must continue to expend time, money, and effort in the area of production and QC to maintain cGMP compliance. These regulations also impose certain organizational, procedural and documentation requirements with respect to production and quality assurance activities. BLA holders using contract manufacturers, laboratories or packagers are responsible for the selection and monitoring of qualified firms, and, in certain circumstances, qualified suppliers to these firms. These firms and, where applicable, their suppliers are subject to inspections by the FDA at any time, and the discovery of violative conditions, including failure to conform to cGMP, could result in enforcement actions that interrupt the operation of any such facilities or the ability to distribute products produced, processed or tested by them. Discovery of problems with a product after approval may result in restrictions on a product, producers, or holder of an approved BLA, including, among other things, recall or withdrawal of the product from the market.

The FDA is required to facilitate the development, and expedite the review, of drugs and biologics that are intended for the treatment of a serious or life threatening disease or condition for

which there is no effective treatment and which demonstrates the potential to address unmet medical needs for the condition. Under the fast track program, a sponsor may request that the FDA grant fast track designation to the product candidate for a specific indication concurrent with, or after, the submission of the IND for the product candidate. The FDA must determine if the product candidate qualifies for fast track designation within 60 days of receipt of the sponsor's request.

Under the FDA's accelerated approval regulations, the FDA may approve a drug or biologic for a serious or life threatening illness that provides meaningful therapeutic benefit to patients over existing treatments based upon a surrogate endpoint that is reasonably likely to predict clinical benefit, or on a clinical endpoint that can be measured earlier than irreversible morbidity or mortality, that is reasonably likely to predict an effect on irreversible morbidity or mortality or other clinical benefit, taking into account the severity, rarity, or prevalence of the condition and the availability or lack of alternative treatments.

In clinical trials, a surrogate endpoint is a measurement of laboratory or clinical signs of a disease or condition that substitutes for a direct measurement of how a patient feels, functions, or survives. Surrogate endpoints can often be measured more easily or more rapidly than clinical endpoints. A product candidate approved on this basis is subject to rigorous post marketing compliance requirements, including the completion of Phase 4 or post approval clinical trials to confirm the effect on the clinical endpoint. Failure to conduct required post approval studies, or confirm a clinical benefit during post marketing studies, will allow the FDA to withdraw the product from the market on an expedited basis. All promotional materials for product candidates approved under accelerated regulations are subject to prior review by the FDA.

In addition to other benefits such as the ability to use surrogate endpoints and engage in more frequent interactions with the FDA, the FDA may initiate review of sections of a fast track product candidate's NDA or BLA before the application is complete. This rolling review is available if the applicant provides, and the FDA approves, a schedule for the submission of the remaining information and the applicant pays applicable user fees. However, the FDA's time period goal for reviewing an application does not begin until the last section of the application is submitted. Additionally, the fast track designation may be withdrawn by the FDA if the FDA believes that the designation is no longer supported by data emerging in the clinical trial process.

Depending upon the timing, duration and specifics of FDA approval of our product candidates, some of our U.S. patents may be eligible for limited patent term extension under the Drug Price Competition and Patent Term Restoration Act of 1984, referred to as the Hatch-Waxman Amendments. The Hatch-Waxman Amendments permit a patent restoration term of up to five years as compensation for patent term lost during product development and the FDA regulatory review process. However, patent term restoration cannot extend the remaining term of a patent beyond a total of 14 years from the product's approval date. The patent term restoration period is generally one-half the time between the effective date of an IND, and the submission date of a BLA, plus the time between the submission date of a BLA and the approval of that application. Only one patent applicable to an approved biologic is eligible for the extension, and the extension must be applied for prior to expiration of the patent. The USPTO, in consultation with the FDA, reviews and approves the application for any patent term extension or restoration.

Under the Pediatric Research Equity Act, or PREA, BLAs or supplements must contain data to assess the safety and effectiveness of the biologic for the claimed indications in all relevant pediatric subpopulations and to support dosing and administration for each pediatric subpopulation for which

the product is safe and effective. The FDA may grant full or partial waivers, or deferrals, for submission of data. Unless otherwise required by regulation, PREA does not apply to any biologic for an indication for which orphan designation has been granted.

In the European Union, our product candidates are also subject to extensive regulatory requirements. As in the United States, pharmaceuticals which are referred to as medicinal products can only be marketed if an MA from the competent regulatory agencies has been obtained.

Similar to the United States, the various phases of preclinical and clinical research in the European Union are subject to significant regulatory controls. Although the EU Clinical Trials Directive 2001/20/EC has sought to harmonize the EU clinical trials regulatory framework, setting out common rules for the control and authorization of clinical trials in the European Union, the European Union Member States have transposed and applied the provisions of the Directive differently. This has led to significant variations in the Member State regimes. To improve the current system, a new Regulation No. 536/2014 on clinical trials on medicinal product candidates for human use, which repealed Directive 2001/20/EC, was adopted on April 16, 2014 and published in the European Official Journal on May 27, 2014. The new Regulation aims at harmonizing and streamlining the clinical trials authorization process, simplifying adverse event reporting procedures, improving the supervision of clinical trials, and increasing their transparency. The new Regulation entered into force on June 16, 2014 but will apply not earlier than May 28, 2016. Until then the Clinical Trials Directive 2001/20/EC will still apply. In addition, the transitory provisions of the new Regulation offer the sponsors the possibility to choose between the requirements of the Directive and the Regulation for one year from the entry into application of the Regulation.

Under the current regime, before a clinical trial can be initiated it must be approved in each of the European Union countries where the trial is to be conducted by two distinct bodies: the National Competent Authority, or NCA, and one or more Ethics Committees, or ECs. Under the current regime all suspected unexpected serious adverse reactions to the investigated drug that occur during the clinical trial have to be reported to the NCA and ECs of the Member State where they occurred.

In the European Economic Area, or EEA (which is comprised of the 28 Member States of the EU plus Norway, Iceland and Liechtenstein), medicinal products can only be commercialized after obtaining an MA. There are two types of MAs:

The Community MA, which is issued by the European Commission through the Centralized Procedure, based on the opinion of the Committee for Medicinal Products for Human Use of the EMA, and which is valid throughout the entire territory of the EEA. The Centralized Procedure is mandatory for certain types of products, such as biotechnology medicinal products, orphan medicinal products, and medicinal products containing a new active substance indicated for the treatment of AIDS, cancer, neurodegenerative disorders, diabetes, auto-immune and viral diseases. The Centralized Procedure is optional for products containing a new active substance not yet authorized in the EEA, or for products that constitute a significant therapeutic, scientific or technical innovation or which are in the interest of public health in the European Union.

National MAs, which are issued by the competent authorities of the Member States of the EEA and only cover their respective territory, are available for products not falling within the mandatory scope of the Centralized Procedure. Where a product has already been authorized for marketing in a Member State of the EEA, this National MA can be recognized in another Member States through

the Mutual Recognition Procedure. If the product has not received a National MA in any Member State at the time of application, it can be approved simultaneously in various Member States through the Decentralized Procedure. Under the Decentralized Procedure an identical dossier is submitted to the competent authorities of each of the Member States in which the MA is sought, one of which is selected by the applicant as the Reference Member State, or RMS. The competent authority of the RMS prepares a draft assessment report, a draft summary of the product characteristics and a draft of the labeling and package leaflet, which are sent to the other Member States (referred to as the Concerned Member States, or CMSs) for their approval. If the CMSs raise no objections, based on a potential serious risk to public health, to the assessment, the draft summary of the product characteristics, labeling, or packaging proposed by the RMS, the product is subsequently granted a National MA in all the Member States (i.e. in the RMS and the CMSs).

Under the above described procedures, before granting the MA, the EMA or the competent authorities of the Member States of the EEA make an assessment of the risk-benefit balance of the product on the basis of scientific criteria concerning its quality, safety and efficacy.

Our current and future operations may be subject to additional health care regulation and enforcement by the federal government and by authorities in the states and foreign jurisdictions particularly after our product candidates are approved. Such laws may include:

The United States and some foreign jurisdictions are considering or have enacted a number of legislative and regulatory proposals to change the healthcare system in ways that could affect our ability to sell our products profitably. Among policy makers and payors in the United States and elsewhere, there is significant interest in promoting changes in healthcare systems with the stated goals of containing health care costs, improving quality or expanding access.

By way of example, in March 2010, the Patient Protection and Affordable Care Act, or the ACA, was signed into law, which intended to broaden access to health insurance, reduce or constrain the growth of healthcare spending, enhance remedies against fraud and abuse, add transparency requirements for the healthcare and health insurance industries, impose taxes and fees on the health industry and impose additional health policy reforms. Among the provisions of the ACA of importance to our business are:

We expect that the ACA, as well as other healthcare reform measures that may be adopted in the future, may result in more rigorous coverage criteria and lower reimbursement, and in additional downward pressure on the price that we receive for any approved product. Any reduction in reimbursement from Medicare or other government-funded programs may result in a similar reduction in payments from private payors. The implementation of cost containment measures or other healthcare reforms may prevent us from being able to generate revenue, attain profitability or commercialize our drugs.

Moreover, we cannot predict what healthcare reform initiatives may be adopted in the future. Further federal, state and foreign legislative and regulatory developments are likely, and we expect ongoing initiatives to increase pressure on drug pricing. Such reforms could have an adverse effect on anticipated revenues from product candidates that we may successfully develop and for which we may obtain regulatory approval and may affect our overall financial condition and ability to develop product candidates.

Significant uncertainty exists as to the coverage and reimbursement status of any product candidates for which we or our collaborators obtain regulatory approval, and also with regard to coverage and reimbursement going forward of our approved products. In the United States and markets in other countries, sales of any products for which we or our collaborators receive regulatory approval for commercial sale will depend, in part, on the extent to which third-party payors provide coverage and establish adequate reimbursement levels for such drug products.

In the United States, third-party payors include federal and state healthcare programs, government authorities, private managed care providers, private health insurers and other organizations. Third-party payors are increasingly challenging the price, examining the medical necessity and reviewing the cost-effectiveness of medical drug products and medical services, in addition to questioning their safety and efficacy. Such payors may limit coverage to specific drug products on an approved list, also known as a formulary, which might not include all of the FDA-approved drugs for a particular indication. We or our collaborators may need to conduct expensive pharmaco-economic studies in order to demonstrate the medical necessity and cost-effectiveness of our products, in addition to the costs required to obtain the FDA approvals. Nonetheless, our product candidates may not be considered medically necessary or cost-effective.

Moreover, the process for determining whether a third-party payor will provide coverage for a drug product may be separate from the process for setting the price of a drug product or for establishing the reimbursement rate that such a payor will pay for the drug product. A payor's decision to provide coverage for a drug product does not imply that an adequate reimbursement rate will be approved. Further, one payor's determination to provide coverage for a drug product does not assure that other payors will also provide coverage for the drug product. Adequate third-party reimbursement may not be available to enable us to maintain price levels sufficient to realize an appropriate return on our investment in product development.

Different pricing and reimbursement schemes exist in other countries. In the European Union, governments influence the price of pharmaceutical products through their pricing and reimbursement rules and control of national health care systems that fund a large part of the cost of those products to consumers. Some jurisdictions operate positive and negative list systems under which products may only be marketed once a reimbursement price has been agreed. To obtain reimbursement or pricing approval, some of these countries may require the completion of clinical trials that compare the cost-effectiveness of a particular drug candidate to currently available therapies. Other member states allow companies to fix their own prices for medicines, but monitor and control company

profits. The downward pressure on health care costs in general, particularly prescription drugs, has become very intense. As a result, increasingly high barriers are being erected to the entry of new products. In addition, in some countries, cross-border imports from low-priced markets exert a commercial pressure on pricing within a country.

The marketability of any product candidates for which we or our collaborators receive regulatory approval for commercial sale may suffer if the government and third-party payors fail to provide adequate coverage and reimbursement. In addition, emphasis on managed care in the United States has increased and we expect will continue to increase the pressure on pharmaceutical pricing. Coverage policies and third-party reimbursement rates may change at any time. Even if favorable coverage and reimbursement status is attained for one or more products for which we or our collaborators receive regulatory approval, less favorable coverage policies and reimbursement rates may be implemented in the future.

As of December 31, 2015, we had approximately 400 employees. We consider our labor relations to be positive.

We were incorporated on July 1, 1992 as a private limited liability company (DK: anpartsselskab, or ApS) under Danish law and we are registered with the Danish Business Authority (DK: Erhvervsstyrelsen) in Copenhagen, Denmark under registration number (CVR) no. 16271187. On September 3, 1994, our company was converted into a public limited liability company (DK: aktieselskab, or A/S).

We have a two-tier governance structure consisting of a board of directors and executive management. Below is a summary of relevant information concerning our board of directors and executive management, as well as a brief summary of certain significant provisions of Danish corporate law and the articles of association that will be in effect upon the closing of this offering, which relate to our board of directors.

The following table sets forth information with respect to each of our board members and their respective ages as of December 31, 2015. The terms of office of all our board members expire at the next annual general meeting to be held in 2016. All board members are eligible for re-election.

The business address of our board members is our registered office address at Hejreskovvej 10A, DK-3490 Kvistgaard, Denmark.


Name of Board Member	Age	Position(s)
Gerard van Odijk	58	Chairman
Anders Gersel Pedersen	64	Deputy Chairman
Claus Braestrup	70	Board Member
Erik Gregers Hansen	63	Board Member
Peter Kürstein	59	Board Member
Frank Verwiel	53	Board Nominee

The following is a brief summary of the business experience of our non-employee board members.

Dr. van Odijk has been the chairman of our board of directors since April 2014 as well as a member of the board of directors since April 2008. He was re-elected in 2015 for a one-year term. Our board of directors has assessed that Dr. van Odijk is independent under Nasdaq Copenhagen listing standards. Dr. van Odijk is also currently an independent advisor for the pharmaceutical industry and a member of the board of directors of UDG Healthcare plc. Dr. van Odijk was formerly president and chief executive officer of Teva Pharmaceuticals Europe B.V. He received his M.D. from the University of Utrecht in the Netherlands.

Dr. Pedersen has been deputy chairman of our board of directors since April 2014 as well as a member of the board of directors since April 2010. He was re-elected in 2015 for a one-year term. Our board of directors has assessed that Dr. Pedersen is independent under Nasdaq Copenhagen listing standards. Dr. Pedersen is also currently an executive vice president of research and development at H. Lundbeck A/S, a deputy chairman of the board of directors of Genmab A/S and a member of the board of directors of ALK-Abelló A/S.

Dr. Braestrup has been a member of the board of directors since April 2008. He was re-elected in 2015 for a one-year term. Our board of directors has assessed that Dr. Braestrup is independent under Nasdaq Copenhagen listing standards. Dr. Braestrup is also currently the chairman of the board of directors of Saniona AB and a member of the board of directors of Evolva Holding SA, Gyros AB and Evotec AG. He is also an executive of Kastan ApS. He was formerly president and chief executive officer of H. Lundbeck A/S. He received his doctorate in medicine from the University of Copenhagen.

Mr. Hansen has been a member of the board of directors since April 2010. He was re-elected in 2015 for a one-year term. Our board of directors has assessed that Mr. Hansen is independent under Nasdaq Copenhagen listing standards. Mr. Hansen is also currently a chairman of the board of directors of Polaris Management A/S, TTIT A/S and TTiT Ejendomme A/S; deputy chairman of the board of directors of Bagger-Sørensen & Co. A/S, Bagger-Sørensen Foundation, Gumlink A/S and Fertin Pharma A/S; and a member of the board of directors of Lesanco ApS, Ecco Sko A/S, OKONO A/S, Wide Invest ApS, 4 Best Invest ApS, Vecata Ejendomme A/S, Bagger-Sørensen Invest A/S and Aser Ltd. He is also an executive of Rigas Invest ApS, BFB ApS, Tresor Asset Advisers ApS, Tresor ApS, Berco ApS, Polaris Invest II ApS and Hansen Advisers ApS. Mr. Hansen holds an MSc in finance and accounting from Aarhus University, in Aarhus, Denmark.

Mr. Kürstein has been a member of the board of directors since April 2012. He was re-elected in 2015 for a one-year term. Our board of directors has assessed that Mr. Kürstein is independent under Nasdaq Copenhagen listing standards. Mr. Kürstein is also currently the chairman of the board of directors of Radiometer Medical ApS; deputy chairman of the board of directors of FOSS A/S; and a member of the board of directors of N. Foss & Co. A/S, Den Ehrvervsdrivende Fond GI. Strand, Copenhagen capital section under the Confederation of Danish Industries and Danske BorneAstma Center. Mr. Kürstein is also the chairman of the board of directors of the Danish-American Business Forum and the Committee on Health Care and Life Science under the Confederation of Danish Industries and an executive officer at ApS Mijimax. Mr. Kürstein has served previously as the chairman of the board of directors of Radiometer Finans ApS and the committee on Health Care and Life Science under the Confederation of Danish Industries; and as a member of the board of directors of H. Lundbeck A/S. Additionally, Mr. Kürstein served previously as the chief executive officer of Danrad Holding ApS and Radiometer Medical ApS; and as an executive officer of Danrad ApS. Mr. Kürstein holds an MBA from Harvard Business School in Boston, USA.

Dr. Verwiel was appointed as an observer of the board of directors in August 2015. The board of directors expects to nominate Dr. Verwiel for election to the board of directors at the annual general meeting in 2016. Dr. Verwiel currently serves as a member of the board of directors of Achillion Pharmaceuticals Inc. Dr. Verwiel served as a member of the board of directors of Aptalis Holdings Inc. and certain of its affiliates and MPEX Pharmaceuticals Inc., among others from 2005 to 2014, until the sale of Aptalis Pharma Inc. to Forest Laboratories Inc. in March of 2014. In the same period Dr. Verwiel also served as the president and chief executive officer of Aptalis Pharma Inc. From 1996 to 2005, Dr. Verwiel served in various roles at Merck & Co. including vice president, Hypertension, Worldwide Human Health Marketing and as a member of Merck's worldwide hypertension business strategy team. Dr. Verwiel was a member of the board of directors of

InterMune Inc. from 2012 to 2014. Dr. Verwiel received his M.D. from Erasmus University in Rotterdam, the Netherlands. Dr. Verwiel also holds an MBA from INSEAD in Fontainebleau, France.

The following table sets forth information with respect to each of the members of our executive management, their respective ages and their positions as of December 31, 2015. The business address of these members of our executive management is our registered office address at Hejreskovvej 10A, DK-3490 Kvistgaard, Denmark.

The following is a brief summary of the business experience of our executive management.

Mr. Chaplin has served as our president and chief executive officer since June 2014. Mr. Chaplin joined our subsidiary, Bavarian Nordic GmbH, in 1999 and was appointed executive vice president in 2004. Prior to joining Bavarian Nordic GmbH, Mr. Chaplin worked for several years both in the United Kingdom and Australia developing vaccines against infectious diseases. Mr. Chaplin is co-chair of the Alliance for BioSecurity. Mr. Chaplin holds a Ph.D. in Immunology from Bristol University.

Mr. Larsen has served as our executive vice president and chief financial officer since he joined the company in July 2008 from Nordisk Film, where he served as chief financial officer and worked since August 2004. Mr. Larsen holds a M.Sc. in economics and business administration from Copenhagen Business School.

The board of directors is responsible for our overall strategic management and the financial and managerial supervision, as well as for regular evaluation of the work of the executive management. In addition, the board of directors supervises our affairs in a general sense and ensures that they are managed in an adequate manner and in accordance with applicable law and our articles of association.

The board of directors performs its duties in accordance with our rules of procedure of the board of directors. The rules of procedure are reviewed and updated by all members of the board of directors. Under our articles of association, the board of directors may consist of three to six external members elected by the shareholders at the annual general meeting for terms of one year with possibility for re-election. Our board of directors currently consists of five board members and we plan to elect a sixth board member at our next annual general meeting. In addition, the employees may, pursuant to the statutory rules regarding representation of the employees on the board of directors, elect employee representatives to the board of directors. Currently the board of directors has no employee representation. The board of directors elects a chairman from among its members. All of our board members and our board nominee are independent under the corporate governance standards of The NASDAQ Global Select Market and Nasdaq Copenhagen.

Members of the executive management are appointed by the board of directors, which lays down the terms and conditions of their employment and the framework for their duties. The executive management is responsible for our day-to-day management in compliance with the guidelines and directions issued by the board of directors. Our day-to-day operations do not include transactions of an unusual nature or of material importance to the affairs of the company.

Upon the closing of this offering, we will have a finance, risk and audit committee, and a nomination and remuneration committee. We have adopted a charter for each of these committees. Under Danish corporate law, it is not possible to delegate the decision making authority of the entire board of directors to board committees.

We have set up a finance, risk and audit committee, or audit committee, consisting of Erik Gregers Hansen and Anders Gersel Pedersen and chaired by Erik Gregers Hansen. The audit committee reviews and discusses the accounting, audit and the regulatory control with our auditors elected at the general meeting and the executive management in accordance with the working terms of reference of the audit committee. Upon the closing of this offering, our audit committee will consist of Erik Gregers Hansen and Anders Gersel Pedersen. Each member satisfies the independence requirements of the corporate governance standards of The NASDAQ Global Select Market, and Erik Gregers Hansen qualifies as an "audit committee financial expert," as defined in NASDAQ Rule 5605(c)(2)(A) and as determined by our board of directors. Provided he is elected to the board at the annual general meeting in the spring of 2016, Frank Verwiel is also expected to be appointed as a member of the audit committee. Our audit committee will oversee our accounting and financial reporting processes and the audits of our consolidated financial statements. Until such third director is appointed to the audit committee, we will not be in compliance with the composition requirement of NASDAQ Rule 5605(c)(2)(A), which requires that the audit committee consist of three members. We intend to rely on the cure period provided in NADSAQ Rule 5605(c)(4)(B), which allows us to comply with the composition requirement of NASDAQ Rule 5605(c)(2)(A) by the earlier of our next annual general meeting of shareholders or one year from the consummation of this offering. Our audit committee will be responsible for, among other things:

Upon the closing of this offering, our nomination and remuneration committee will consist of Gerard van Odijk, Claus Braestrup and Peter Kürstein, and will be chaired by Gerard van Odijk. Each member satisfies the independence requirements of the corporate governance standards of The NASDAQ Global Select Market. Our nomination and remuneration committee will assist our board of directors in selecting individuals qualified to become our board members, determining the composition of the board of directors and its committees, and reviewing and approving or recommending our compensation structure, including all forms of compensation relating to our board of directors and the executive management. Our nomination and remuneration committee will be responsible for, among other things:

We have adopted a code of business conduct and ethics that applies to all of our employees, members of our executive management and members of our board of directors responsible for financial reporting. Following the closing of this offering, the code of business conduct and ethics will be available on our website at www.bavarian-nordic.com. We expect that any amendments to the code, or any waivers of its requirements, will be disclosed on our website. The information on, or that can be accessed through, our website is not part of and should not be incorporated by reference into this prospectus.

The Sarbanes-Oxley Act of 2002, or the Sarbanes-Oxley Act, as well as related rules subsequently implemented by the Securities and Exchange Commission, or SEC, requires foreign private issuers, including our company, to comply with various corporate governance practices. In addition, The NASDAQ Global Select Market rules provide that foreign private issuers may follow home country practice in lieu of The NASDAQ Global Select Market corporate governance standards, subject to certain exceptions and except to the extent that such exemptions would be contrary to U.S. federal securities laws. The home country practices followed by our company in lieu of The NASDAQ Global Select Market rules are described below:

Because we are a foreign private issuer, our members of our board of directors and executive management are not subject to short-swing profit and insider trading reporting obligations under section 16 of the Securities Exchange Act of 1934, as amended, or the Exchange Act. They will, however, be subject to the obligations to report changes in share ownership under section 13 of the Exchange Act and related SEC rules.

In 2015, the aggregate remuneration paid to our board of directors was DKK 2,130,000 ($319,820). The members of the board of directors did not receive any other remuneration from the Company in 2015.

No member of the board of directors is entitled to any kind of remuneration upon retirement from his or her position as a member of the board of directors. We have not allocated funds for any pension benefits, severance schemes or similar measures, or undertaken any other obligations to do so on behalf of the board of directors, and we have no obligation to do so.

For the financial year ended December 31, 2015, the aggregate remuneration to our executive management was DKK 13,424,497 ($2.0 million). This amount includes executive bonuses, which are expected to be paid in March 2016. The final amount of executive bonuses to be paid has not yet been determined.

The board of directors has adopted a Remuneration Policy, including the General Guidelines for Incentive Remuneration, of the Board of Directors and Executive Management in the Company, which was approved by our shareholders at our annual general meeting on April 23, 2015. No member of our board of directors and executive management has received or will receive separate remuneration in connection with this offering.

Compensation of Members of Our Board of Directors and Executive Management

During 2015, our board of directors granted the following warrants to members of our board of directors and executive management:

We have entered into employment or service agreements with our executive management consisting of our president and chief executive officer, Mr. Chaplin, and our executive vice president and chief financial officer, Ole Larsen. Our executive management can terminate their employment with the company by giving six months' notice, and we can terminate the employment by giving 18 months' notice to Mr. Chaplin and 12 months' notice to Mr. Larsen. The remuneration to the executive management consists of a base salary including standard benefits (such as a company car, personal and health insurance, company-paid telephone and computer), cash bonus, phantom shares and warrants. The cash bonus is conditional upon the fulfilment of certain predefined bonus targets relating to both company and individual performance. The cash bonus cannot exceed 50% of the executive management's base salary. However, our board of directors may decide to postpone for three years all or part of the payment of a cash bonus awarded to a member of the executive management, converting the postponed bonus into a number of Restricted Stock Units, or RSUs. Further, the board may decide to grant up to one additional matching share for each two acquired RSUs. Warrants and phantom shares are granted to the executive management under our warrant program and phantom share program, both of which are further described below. In addition, Mr. Larsen receives an annual pension contribution of 10% of his annual base salary.

In addition to the benefits described above, we will cover Mr. Chaplin's accommodation expenses, exclusive of electricity and heating expenses, until May 28, 2017. Also, reasonable relocation expenses, including, but not limited to, house-hunting trips, moving expenses and reasonable school fees for admitting the children to an international school in Denmark will be reimbursed by us. Further, we entered into a long-term incentive agreement with Mr. Chaplin in 2009, when he served as our executive vice president, Division President Infectious Diseases. The incentive scheme offered one-off payments ranging from 150 thousand euros up to 1.5 million euros. The one-off payments were subject to achievement of various milestones and were furthermore conditioned upon continued employment, irrespective of the position held, with us at the time of the achievement of the respective milestone event. The long-term incentive scheme ceased to be effective as of December 31, 2015. In connection with Mr. Chaplin's appointment as president and chief executive officer, it was extraordinarily decided by our board of directors to let him continue his participation in the long-term incentive scheme. However, his participation was modified such that Mr. Chaplin in the period from his appointment could not receive payments under the long-term incentive scheme which, together with any change of control bonus (as further described below), would exceed one year's base salary. We had no obligation to continue with other similar programs after December 31, 2015 and no such programs have been implemented thus far in 2016.

In the event that (i) a controlling interest in us is transferred, (ii) we cease to exist by merger with a third party, (iii) we divest all or significant parts of our assets to a third party, or (iv) we divest all or significant parts of our assets related to our infectious diseases business or our cancer immunotherapy business to a third party, our executive management will be entitled to receive a transaction bonus corresponding to 12 months' base salary. It is a condition for payment of the transaction bonus that the relevant member of the executive management has not given notice of resignation prior to completion of the relevant event and that we have not terminated the employment with the notice period expiring prior to completion of the relevant event. Further, if a member of our executive management's employment is terminated by us within 12 months after completion of an event triggering the transaction bonus, and provided the termination is not due to breach by said member, the notice of termination on the part of the company will be extended to 24 months.

Mr. Chaplin and Mr. Larsen are both subject to non-competition clauses applicable during the employment and for a period of 18 and 12 months, respectively, following each of their resignations.

Other than as set out above, the members of the executive management are not entitled to any kind of remuneration upon termination of employment other than salary during the notice period, post-employment compensation to an executive's dependents in the event of the executive's death and in certain circumstances for disability, compensation for non-competition clauses and possible transaction bonus as described above. Except for an allocation for payments under non-competition clauses with the executive management, neither we nor our subsidiaries have allocated funds for any pension benefits or similar measures or undertaken any other obligations to or on behalf of the executive management and we are under no obligation to do so.

We and our subsidiaries have not granted any loans, issued any guarantees or undertaken any other obligations to do so on behalf of our executive management.

For further details on the terms and conditions of the warrants, see "Warrant Incentive Program." See also "Phantom Share Programs" for a description of our phantom share scheme.

Other than as set out above, no exceptional or extraordinary agreements, including agreements regarding bonus schemes, except ordinary incentive schemes and remuneration of the executive management implying financial obligations for us, have been concluded between us and members of our executive management.

The board of directors has been granting warrants to our management and selected employees of the company and our subsidiaries. Until 2013, members of our board of directors were also granted warrants. Beginning in 2014, the remuneration structure for our board of directors was changed allowing the board of directors to be remunerated only by payment of fixed cash fees.

Warrants have been granted pursuant to authorization given to our board of directors by the shareholders in our articles of association. In accordance with the authorization, our board of directors has fixed the terms of the warrants, including the exercise price and the size of the grants, taking into account the limitations in the authorization from the shareholders, our guidelines for incentive pay in force at the time of grant, as well as the need to motivate and retain the warrant holders. Warrants have been granted free of charge and will typically become exercisable approximately three years after the date of grant and may be exercised to subscribe for shares in a number of pre-defined exercise windows against payment of the exercise price. Unexercised warrants will lapse approximately four and a half years after the date of grant. Granted warrants are subject to provisions reflecting the principles of the Danish Stock Option Act (in Danish: Aktieoptionsloven), which allow for the forfeiture of unexercised warrants if the grantee separates from the company or one of our subsidiaries under circumstances in which the warrant holder is considered a "bad-leaver." Such circumstances include the warant holder being dismissed for cause. Warrant holders are allowed to maintain all granted warrants if they separate from the company or one of our subsidiaries under circumstances where they are considered as "good-leavers." Such circumstances include the warrant holders being dismissed without cause.

As of December 31, 2015, the material terms of our outstanding warrants and the holders of such warrants may be summarized as follows:

In 2013, we established a three-year phantom share program (2014-2017 program) under which all employees in the group receive up to six phantom shares free of charge for each month of employment during the period from January 1, 2014 to December 31, 2016. The phantom shares are granted at the end of each month conditioned upon continued employment at the date of grant. Each employee who is a full-time employee during the term of the program will be eligible to receive a maximum of 216 phantom shares. Part-time employees will receive a pro rata number of phantom shares. Each phantom share entitles the holder to a cash payment in January 2017, calculated as the difference between (i) the average share price for the Company's share in a period of 15 business days prior to the establishment of the phantom share program plus a 15% premium (the exercise price) and (ii) the average closing price on Nasdaq Copenhagen of our shares during a period of 10 business days before January 16, 2017. However, payment is conditional upon the difference between the exercise price and the average closing price being at least 10%.

In 2014, we established a three-year phantom share program (2015-2018 program) under which all employees in the group receive up to six phantom shares free of charge for each month of employment during the period from January 1, 2015 to December 31, 2017. The phantom shares are granted at the end of each month conditional upon continued employment at the date of grant. Each employee who is a full-time employee during the term of the program will be eligible to receive a maximum of 216 phantom shares. Part-time employees will receive a pro rata number of phantom shares. Each phantom share entitles the holder to a cash payment in January 2018, calculated as the difference between (i) the average closing price on Nasdaq Copenhagen of our shares in the period 15 trading days prior to November 13, 2014 plus 15% (the exercise price) and (ii) the average closing price on Nasdaq Copenhagen of our shares during a period of 10 trading days before January 15, 2018. However, payment is conditional upon the difference between the exercise price and the average closing price being at least DKK 5 ($1).

In 2015, we established a three-year phantom share program (2016-2019 program) under which all employees in the group receive up to six phantom shares free of charge for each month of employment during the period from January 1, 2016 to December 31, 2018. The phantom shares are granted at the end of each month conditional upon continued employment at the date of grant. Each employee who is a full-time employee during the term of the program will be eligible to receive a maximum of 216 phantom shares. Part-time employees will receive a pro rata number of phantom shares. The exercise price is DKK 366.85 and has been established as the average share price for the Company's share in a period of 15 business days prior to the establishment of the phantom share program plus a 15% premium. The phantom shares may be exercised in January 2019, only if the Company's share price by then exceeds the exercise price by at least DKK 5. In that case, each employee in the program will receive a cash bonus per phantom share equivalent to DKK 1 per point the share price of the Company's shares exceeds the exercise price.

All of our phantom share programs include provisions allowing for an earlier settlement of the phantom shares in the event of inter alia a change of control in the company, a merger or demerger of the company or the company's delisting. Moreover, both phantom share programs include provisions allowing for adjustments in the terms of the phantom shares if our capital structure is changed.

The awarded phantom shares and phantom shares expected to be awarded under the phantom share programs described above are as follows:

According to the Danish Companies Act, the general meeting is allowed to discharge our board members and members of our executive management from liability for any particular financial year based on a resolution relating to the period covered by the financial statement for the previous financial year. This discharge means that the general meeting will relieve such board members and members of our executive management from liability to our company. However, the general meeting cannot discharge any claims by individual shareholders or other third parties.

Additionally, we have entered into agreements with our board members and members of our executive management pursuant to which, subject to limited exceptions, we will agree to indemnify such board members and members of our executive management from civil liability, including: (i) any reasonably incurred damages or fines payable by them as a result of an act or failure to act in the exercise of their duties performed before or after the date of the indemnification agreement; (ii) any reasonable costs of conducting a defense against a claim; and (iii) any reasonable costs of appearing in other legal proceedings in which such individuals are involved as current or former board members or members of our executive management. The indemnification agreements entered into with our board members are conditional on approval by stockholders at our annual general meeting scheduled on April 20, 2016.

There is a risk that such agreements will be deemed void under Danish law, either because the agreements are deemed contrary to the rules on discharge of liability in the Danish Companies Act (in Danish: Selskabsloven) as set forth above, because the agreements are deemed contrary to sections 19 and 23 of the Danish Liability and Compensation Act (in Danish: Erstatningansvarsloven), which contain mandatory provisions on recourse claims between an employee (including members of our executive management) and the company, or because the

agreements are deemed contrary to the general provisions of the Danish Contracts Act (in Danish: Aftaleloven).

In addition to such indemnification, we provide our board members and executive management with directors' and officers' liability insurance.

Insofar as indemnification of liabilities arising under the Securities Act of 1933, as amended, or the Securities Act, may be permitted to board members and executive management or persons controlling us pursuant to the foregoing provisions, we have been informed that, in the opinion of the SEC, such indemnification is against public policy in the United States as expressed in the Securities Act and is therefore unenforceable.

In December 2009, we obtained full ownership of our subsidiary, Bavarian Nordic Inc. (f/k/a BN Immuno Therapeutics Inc.), a Delaware corporation, or BNI, by purchasing shares in BNI from the chief executive officer and president of BNI, Reiner Laus, who was also our executive vice president at the time. The consideration to Mr. Laus was paid in part in our shares and in part with a number of future milestone payments that are triggered upon the successful completion of a number of pre-defined development milestones. The total remaining consideration to Mr. Laus amounts to a maximum of $4 million (DKK 25 million), of which up to $3 million (DKK 20 million) may be paid in shares. A separate agreement regarding cancellation of certain contractual rights regarding BNI entitles Mr. Laus to a maximum consideration of $5 million (DKK 35 million) upon successful achievement of certain pre-defined milestones.

We have entered into employment agreements with, and issued warrants to, the members of our executive management. See "Management—Compensation" and "Management—Warrant Incentive Program" for more information.

We intend to enter into indemnification agreements with our board members and the members of our executive management. See "Management—Insurance and Indemnification" for a description of these indemnification agreements.

The following table sets forth information relating to the beneficial ownership of our shares as of December 31, 2015 by:

The number of shares beneficially owned by each entity, person, member of or nominee to our board of directors or executive management is determined in accordance with the rules of the SEC, and the information is not necessarily indicative of beneficial ownership for any other purpose. Under such rules, beneficial ownership includes any shares over which the individual has sole or shared voting power or investment power as well as any shares that the individual has the right to subscribe for within 60 days of December 31, 2015 through the exercise of any warrants or other rights. Except as otherwise indicated, and subject to applicable community property laws, the persons named in the table have sole voting and investment power with respect to all shares owned by that person.

The percentage of shares beneficially owned is computed on the basis of 28,019,671 shares outstanding as of December 31, 2015. Shares for which a person has the right to subscribe within 60 days of December 31, 2015 are deemed outstanding for purposes of computing the percentage ownership of the person holding such rights, but are not deemed outstanding for purposes of computing the percentage ownership of any other person. There were no shares for which a person has the right to subscribe within 60 days of December 31, 2015. Additionally, a person is considered to have the right to subscribe for shares which are subject to outstanding warrants and vested within 60 days of December 31, 2015, although such warrants may only be exercised in two annual exercise periods. See "Description of Share Capital—Our Warrants—Exercise Periods" for more

information. Unless otherwise indicated below, the address for each beneficial owner listed is c/o Bavarian Nordic A/S, at Hejreskovvej 10A, DK-3490 Kvistgaard, Denmark.

As of December 31, 2015, there were 27,614 holders of record entered in our share register, of which 155 were U.S. residents, holding 14.67% of our outstanding shares. The number of individual holders of record is based exclusively upon our share register and does not address whether a share or shares may be held by the holder of record on behalf of more than one person or institution who may be deemed to be the beneficial owner of a share or shares in our company.

Set forth below is a summary of certain information concerning our share capital as well as a description of certain provisions of our articles of association and relevant provisions of the Danish Companies Act. The summary includes certain references to and descriptions of material provisions of our articles of association to be effective in connection with the consummation of this offering and Danish law in force as of the date of this prospectus. The summary below contains only material information concerning our share capital and corporate status and does not purport to be complete and is qualified in its entirety by reference to our articles of association and applicable Danish law. Further, please note that as an American Depositary Share, or ADS, holder you will not be treated as one of our shareholders and will not have any shareholder rights.

Our company was incorporated on July 1, 1992 as a private limited liability company (in Danish: Anpartsselskab, or ApS) under Danish law and is registered with the Danish Business Authority (in Danish: Erhvervsstyrelsen) in Copenhagen, Denmark under registration number (CVR) no. 16271187. On September 3, 1994, our company was converted into a public limited liability company (in Danish: Aktieselskab, or A/S). Our company's headquarters and registered office is Hejreskovvej 10A, DK-3490 Kvistgaard, Denmark and our telephone number is +45 33 26 83 83. Our website address is www.bavarian-nordic.com. The information on, or that can be accessed through, our website is not part of and should not be incorporated by reference into this prospectus. We have included our website address as an inactive textual reference only.

As of December 31, 2015 our registered, issued and outstanding share capital was DKK 280,196,710 distributed on 28,019,671 shares of nominal value DKK 10 each, and excludes up to 1,624,605 shares that may be issued upon the exercise of outstanding warrants. For a description of the terms of our outstanding warrants, see "—Warrant Incentive Program." The development of our share capital since our inception is set forth in the table below.

The new shares issued according to the authorizations listed above will rank pari passu with our existing shares in accordance with our articles of association, including that the new shares shall be negotiable instruments, shall be registered in the name of the shareholder, shall be entered in our register of shareholders, no restrictions shall apply to the transferability of the new shares, and no shareholder shall be obliged to have his shares redeemed. The new shares will confer on the holders the same right to receive dividends and other rights in the company as our existing shares.

Further, our board of directors is authorized on behalf of the Company to acquire its own shares for a total nominal value of up to 10% of our share capital for the time being. The remuneration paid for the shares may not deviate by more than 10% from the bid rate established by Nasdaq Copenhagen at the time of acquisition. The bid rate shall be the closing rate at Nasdaq Copenhagen—all trades at 5:00 PM CET.

As of December 31, 2015 our registered, issued and outstanding share capital was DKK 280,196,710, and excludes up to 1,624,605 shares that may be issued upon the exercise of outstanding warrants. For a description of the terms of our outstanding warrants, see "—Warrant Incentive Program." As of December 31, 2015, our share capital consisted of 28,019,671 shares of nominal value DKK 10 each, and excludes up to 1,624,605 shares that may be issued upon the exercise of outstanding warrants. In connection with this offering, we intend to issue up to ADSs representing shares excluding the underwriters' option to purchase up to additional ADSs. Each ADS will represent one-third of a share. We have applied to have the ADSs

listed on The NASDAQ Global Select Market under the symbol "BAVN." The underlying shares will continue to be listed on Nasdaq Copenhagen under the symbol "BAVA."

Initial settlement of the ADSs issued in this offering will take place on the consummation date of this offering through The Depository Trust Company, or DTC, in accordance with its customary settlement procedures for equity securities. Each person owning ADSs held through DTC must rely on the procedures thereof and on institutions that have accounts therewith to exercise any rights of a holder of the ADSs.

If our shareholders at a general meeting resolve to increase the share capital of the company by a cash contribution, section 162 of the Danish Companies Act will apply. Under that section, shareholders have a pre-emptive right to subscribe for new shares in proportion to their existing shareholdings. However, the pre-emptive right may be derogated from by a majority comprising at least two-thirds of the votes cast as well as at least two-thirds of the share capital represented at the general meeting, provided the share capital increase takes place at market price or nine-tenths of the votes cast as well as at least nine-tenths of the share capital represented at the general meeting if the share capital increase takes place below market price. Further, the pre-emptive rights may be derogated from by an exercise of the board of directors of a valid authorization in our articles of association, provided that the share capital increase takes place at or above market price.

We are obligated to maintain a shareholders' register (in Danish: Ejerbog). The owners' register is maintained by Computershare A/S, Kongevejen 418, Øverød, DK-2840 Holte, Denmark, our Danish share registrar and transfer agent. It is mandatory that the shareholders' register is maintained within the European Union and that it is available to public authorities.

Pursuant to the Danish Companies Act (in Danish: Selskabsloven), public and private limited liability companies are required to register with the Danish Business Authority information regarding shareholders who own at least 5% of the share capital or the voting rights. Pursuant to this provision, we file registrations with the Danish Public Shareholders' Register of the Danish Business Authority. Shareholders that exceed the ownership threshold must notify us and we will subsequently file the information with the Danish Business Authority. Reporting is further required upon reaching thresholds of 10%, 15%, 20%, 25%, 33 1/3%, 50%, 66 2/3%, 90%, and 100%. This also applies to holders of our ADSs.

With respect to our articles of association, the following should be emphasized:

The objectives for which our company has been established are to carry out research, trade, manufacture and any other related activities, primarily within the pharmaceutical industry. See article 2 of our articles of association.

Summary of Provisions Concerning Members of the Board of Directors and the Executive Management

Our company shall be managed by a board of directors of three to six members to be elected for one year at a time by the shareholders at the (annual) general meeting. Retiring directors shall be eligible for re-election. Members that are to be elected pursuant to the statutory rules regarding representation of the employees on the board of directors shall be elected as well. The shareholders

at the general meeting shall determine the remuneration of the board of directors. See article 17 of the articles of association.

The proceedings at meetings of our board of directors will be recorded in the minutes to be signed by the attending members. The board of directors shall elect its own chairman and deputy-chairman and may furthermore grant individual or joint powers of procuration. The board of directors shall draw up its own rules of procedure governing the performance of its duties. See article 18 of the articles of association.

We shall be bound by the joint signatures of the chairman of the board of directors and that of either any one member of the executive management or any two members of the board of directors, or by the joint signatures of any two members of the board of directors and a member of the executive management. See article 19 of the articles of association.

No share shall carry any special rights. See article 7 of the articles of association.

Each share of nominal value DKK 10 shall carry one vote at general meetings. See article 11 of the articles of association.

The shares are negotiable instruments and no restrictions shall apply to the transferability of the shares. See article 6 of the articles of association.

No shareholder shall be obliged to let his shares be redeemed in full or in part by us or by any other party, except as provided in the Danish Companies Act. See article 7 of the articles of association.

All shares shall be registered in the names of the holders and shall be entered in our shareholders' register. See article 6 of the articles of association. On the annual general meeting held on April 23, 2015, the annual general meeting resolved that shares issued on or after April 23, 2015 may no longer be issued to the bearer. Thus, shares issued before said date may have been issued to the bearer.

All resolutions put to the vote of shareholders at general meetings shall be subject to adoption by a simple majority of votes, unless the Danish Companies Act (in Danish: Selskabsloven) or our articles of association prescribes other requirements. Unless a greater majority or unanimity is required pursuant to Danish legislation, the adoption of resolutions regarding amendment of our articles of association, the dissolution of the company or its merger or amalgamation with another company or business, is subject to such resolution being adopted by not less than 2/3 of all the votes cast as well as of the votes represented at the relevant general meeting. See article 16 of the articles of association.

General meetings shall be held in the municipality of our registered office or in the Capital Region of Denmark (in Danish: Region Hovedstaden). General meetings shall be convened by the board of directors giving not less than three weeks' and not more than five weeks' notice. General meetings shall be convened by publication in the IT information system of the Danish Business Authority and on our website. Our board of directors may resolve that notice to convene the general meeting shall be published in a leading newspaper. Furthermore, all shareholders registered in our shareholders' register, who have so requested, shall be convened by letter. The notice shall set out the agenda of the general meeting. The notice shall specify whether any proposal requiring a special majority of votes is to be considered, including the essential contents of such proposal. See article 10 of the articles of association.

Any shareholder shall be entitled to attend general meetings, provided he or she has requested an admission card from our office not later than three days prior to the relevant meeting. His or her capacity as a shareholder shall be documented by his or her title having been entered in our shareholders' register no later than one week prior to the general meeting or by our having received

his or her application for entry of the title in our register of shareholders before this date. The shareholder may attend in person or be represented by proxy, and a shareholder shall be entitled to attend together with an advisor. The attorney must provide a dated instrument of proxy issued to a person who need not be a shareholder in the company. Unless containing a provision to the contrary, instruments of proxy shall be deemed to be in force until revoked in writing by notification to us. However, instruments of proxy issued to our board of directors may not be issued for a period of more than 12 months and may only be issued in respect of a specific general meeting for which the agenda is known in advance. See article 11 of the articles of association.

Extraordinary general meetings shall be held as directed by the shareholders at the general meeting, the board of directors or an auditor, or upon a written request to the board of directors by shareholders holding not less than one twentieth of the share capital. Shareholder requests must contain a specification of the business to be considered at the general meeting. The general meeting shall be convened not later than 14 days after the appropriate request having reached our board of directors. See article 13 of the articles of association and "Risk Factors—You may not be able to exercise your right to vote the shares underlying your ADSs."

Provisions as to the Level of Equity Investments to be Notified to Us and the Danish Authorities

Pursuant to section 29 of the Danish Securities Trading Act (in Danish: Værdipapirhandelsloven), shareholders in a company incorporated in Denmark with its shares admitted to trading and official listing are required to immediately (meaning within the same trading day as the transaction) and simultaneously notify the Company and the Danish Financial Supervisory Authority, or FSA, when the shareholder's stake (i) represents 5% or more of the voting rights in the Company or the nominal value of its share capital, and (ii) when a change in a holding already notified implies that the limits of 5%, 10%, 15%, 20%, 25%, 50% or 90% and the limits of one-third and two-thirds of the voting rights or the nominal value are reached or are no longer reached or the change implies that the limits stated in (i) are no longer reached. This duty to notify also applies to anyone, who directly or indirectly holds (a) financial instruments that afford the holder a right to purchase existing shares, e.g., share options; and/or (b) financial instruments based on existing shares and with an economic effect equal to that of the financial instruments mentioned under (a), regardless of them not affording the right to purchase existing shares, e.g., our ADSs or, under the circumstances, cash-settled derivatives linked to the value of our shares or ADSs. Holding these kinds of financial instruments counts towards the thresholds mentioned above and may thus trigger a duty to notify by themselves or when accumulated with a holding of shares or ADSs. The notifications must comply with the requirements for the contents thereof set out in sections 16 and 17 of the Danish executive order on major shareholders (in Danish: Storaktionærbekendtgørelsen), including the identity of the shareholder and the date when a limit is reached or no longer reached. Failure to comply with the duties of disclosure is punishable by fine or suspension of voting rights in instances of gross or repeated non-compliance. The FSA will in certain cases publish information concerning sanctions imposed, including, as a general rule, the name of the shareholder in question, as a consequence of non-compliance with the above rules. When we receive such notification, we must publish its contents as soon as possible. Furthermore, the general duty of notification pursuant to the Danish Companies Act applies, which implies that shareholders must notify the Company when the limit of 100% of the voting rights or nominal value of the shares is reached or no longer reached. This also applies to holders of our ADSs.

Danish Rules Intended to Prevent Market Abuse, Such as Insider Trading, Tipping and Market Manipulation

Part 10 of the Danish Securities Trading Act, which purpose is to prevent market abuse, apply to us and dealings concerning our shares and will likewise apply to our ADSs. As we prior to our application for the listing of ADSs on The NASDAQ Global Select Market already are subject to Danish and U.S. securities laws, we intend to revise our internal code on possession and handling of inside information and with respect to our board of directors', executive management's and employees' dealings in our shares or in financial instruments the value of which is determined by the value of our shares so that it also covers our ADSs. Furthermore, we have drawn up a list of those persons working for us who could have access to inside information on a regular or incidental basis and have informed such persons of the rules on insider trading and market manipulation, including the sanctions, which can be imposed in the event of a violation of those rules. As of 3 July 2016 EU Regulation No 596/2014 on market abuse, will enter into force, and Part 10 of the Danish Securities Trading Act will likely be repealed, and replaced by the provisions found in EU Regulation No 596/2014.

The EU Short Selling Regulation (EU Regulation 236/2012) Includes Certain Notification Requirements in connection with Short Selling of Shares Admitted to Trading on a Trading Venue (including Nasdaq Copenhagen) and Securities or Derivatives that Relate to Such Shares (including the ADSs).

When a natural or legal person reaches or falls below a net, short position of 0.2% of the issued share capital of a company that has shares admitted to trading on a trading venue, such person shall notify the relevant competent authority, which in Denmark is the Danish FSA. The obligation to notify, moreover, applies in each case where the short position reaches 0.1% above the 0.2% threshold. In addition, when a natural or legal person reaches or falls below a net short position of 0.5% of the issued share capital of a company that has shares admitted to trading on a trading venue and each 0.1% above that, such person shall make a public announcement of its net short position.

Under Danish law, members of the board of directors or executive management may be held liable for damages in the event that loss is caused due to their negligence. They may be held jointly and severally liable for damages to the company and to third parties for acting in violation of the articles of association and Danish law.

Comparison of Danish Corporate Law and Our Articles of Association and Delaware Corporate Law

The following comparison between Danish corporate law, which applies to us, and Delaware corporate law, the law under which many publicly listed companies in the United States are incorporated, discusses additional matters not otherwise described in this prospectus. This summary is subject to Danish law, including the Danish Companies Act, and Delaware corporate law, including the Delaware General Corporation Law. Further, please note that as an ADS holder you will not be treated as one of our shareholders and will not have any shareholder rights.

Denmark. Public limited liability companies in Denmark are usually subject to a two-tier governance structure with the board of directors having the ultimate responsibility for the overall supervision and strategic management of the company in question and with an executive management being responsible for the day-to-day operations. Each board member and member of

the executive board/management is under a fiduciary duty to act in the interest of the company, but shall also take into account the interests of the creditors and the shareholders. Under Danish law, the members of the board of directors and executive management of a limited liability company are liable for losses caused by negligence whether shareholders, creditors or the company itself suffers such losses. They may also be liable for wrongful information given in the annual financial statements or any other public announcements from the company. An investor suing for damages is required to prove its claim with regard to negligence and causation. Danish courts, when assessing negligence, have been reluctant to impose liability unless the directors and officers neglected clear and specific duties. This is also the case when it comes to liability with regard to public offerings or liability with regard to any other public information issued by the company.

Delaware. The board of directors bears the ultimate responsibility for managing the business and affairs of a corporation. In discharging this function, directors of a Delaware corporation owe fiduciary duties of care and loyalty to the corporation and to its stockholders. Delaware courts have decided that the directors of a Delaware corporation are required to exercise informed business judgment in the performance of their duties. Informed business judgment means that the directors have informed themselves of all material information reasonably available to them. Delaware courts have also imposed a heightened standard of conduct upon directors of a Delaware corporation who take any action designed to defeat a threatened change in control of the corporation. In addition, under Delaware law, when the board of directors of a Delaware corporation approves the sale or break-up of a corporation, the board of directors may, in certain circumstances, have a duty to obtain the highest value reasonably available to the stockholders.

Denmark. Under Danish law, the members of the board of directors of a limited liability company are generally appointed for an individual term of one year. There is no limit on the number of consecutive terms the board members may serve. Pursuant to our articles of association, our board members are appointed by the general meeting of shareholders for a term of one year and are eligible for re-election. Election of board members is, according to our articles of association, an item that shall be included on the agenda for the annual general meeting.

At the general meeting, shareholders are entitled at all times to dismiss a board member by a simple majority vote.

Delaware. The Delaware General Corporation Law generally provides for a one-year term for directors, but permits directorships to be divided into up to three classes, of relatively equal size, with up to three-year terms, with the years for each class expiring in different years, if permitted by the certificate of incorporation, an initial bylaw or a bylaw adopted by the stockholders. A director elected to serve a term on a "classified" board may not be removed by stockholders without cause. There is no limit in the number of terms a director may serve.

Denmark. Under Danish law, new board members are elected by the shareholders in a general meeting also in the event of vacancies. A general meeting will thus have to be convened in order to fill a vacancy on the board of directors. However, the board of directors may choose to wait to fill vacancies until the next annual general meeting of the company, provided that the number of the remaining board members is more than two. It is only a statutory requirement to convene a general meeting to fill vacancies if the number of remaining members on the board is less than three.

Delaware. The Delaware General Corporation Law provides that vacancies and newly created directorships may be filled by a majority of the directors then in office (even though less than a quorum) unless (1) otherwise provided in the certificate of incorporation or bylaws of the corporation or (2) the certificate of incorporation directs that a particular class of stock is to elect such director, in which case any other directors elected by such class, or a sole remaining director elected by such class, will fill such vacancy.

Denmark. Under Danish law, board members may not take part in any matter or decision-making that involves a subject or transaction in relation to which the board member has a conflict of interest with us.

Delaware. The Delaware General Corporation Law generally permits transactions involving a Delaware corporation and an interested director of that corporation if:

Denmark. In the event that a board member in a Danish limited liability company is unable to participate in a board meeting, the elected alternate, if any, shall be given access to participate in the board meeting. Our board of directors does not have elected alternates. In a Danish limited liability company, unless the board of directors has decided otherwise, or as otherwise is set out in the articles of association, the board member in question may grant a power of attorney to another board member, provided that this is considered safe considering the agenda in question.

Delaware. A director of a Delaware corporation may not issue a proxy representing the director's voting rights as a director.

Denmark. According to the Danish Companies Act, general meetings in listed limited liability companies shall be convened by the board of directors with a minimum of three weeks' notice and a maximum of five weeks' notice as set forth in the articles of association. A convening notice shall also be forwarded to shareholders recorded in our shareholders' register, who have requested such notification. There are specific requirements as to the information and documentation required to be disclosed in connection with the convening notice.

Delaware. Under Delaware law, unless otherwise provided in the certificate of incorporation or bylaws, written notice of any meeting of the stockholders must be given to each stockholder entitled to vote at the meeting not less than 10 nor more than 60 days before the date of the meeting and shall specify the place, date, hour, and purpose or purposes of the meeting.

Denmark. Each share confers the right to cast one vote at the general meeting of shareholders, unless the articles of association provide otherwise. Each holder of shares may cast

as many votes as it holds shares. Voting instructions may be given only in respect of a number of ADSs representing an integral number of shares or other deposited securities. Shares that are held by us or our direct or indirect subsidiaries do not confer the right to vote.

Delaware. Under the Delaware General Corporation Law, each stockholder is entitled to one vote per share of stock, unless the certificate of incorporation provides otherwise. In addition, the certificate of incorporation may provide for cumulative voting at all elections of directors of the corporation, or at elections held under specified circumstances. Either the certificate of incorporation or the bylaws may specify the number of shares and/or the amount of other securities that must be represented at a meeting in order to constitute a quorum, but in no event can a quorum consist of less than one-third of the shares entitled to vote at a meeting.

Stockholders as of the record date for the meeting are entitled to vote at the meeting, and the board of directors may fix a record date that is no more than 60 nor less than 10 days before the date of the meeting, and if no record date is set then the record date is the close of business on the day next preceding the day on which notice is given, or if notice is waived then the record date is the close of business on the day next preceding the day on which the meeting is held. The determination of the stockholders of record entitled to notice or to vote at a meeting of stockholders shall apply to any adjournment of the meeting, but the board of directors may fix a new record date for the adjourned meeting.

Denmark. According to the Danish Companies Act, extraordinary general meetings of shareholders will be held whenever our board of directors or our appointed auditor requires. In addition, one or more shareholders representing at least 5% of the registered share capital of the company may, in writing, require that a general meeting be convened. If such a demand is forwarded, the board of directors shall convene the general meeting within two weeks thereafter.

All shareholders have the right to present proposals for adoption at the annual general meeting, provided that the proposals are forwarded at the latest six weeks prior thereto. In the event that the request is made at a later date, the board of directors decides whether the proposals have been forwarded in due time to be included on the agenda.

Delaware. Delaware law does not specifically grant stockholders the right to bring business before an annual or special meeting of stockholders. However, if a Delaware corporation is subject to the SEC's proxy rules, a stockholder who owns at least $2,000 in market value, or 1% of the corporation's securities entitled to vote, may propose a matter for a vote at an annual or special meeting in accordance with those rules.

Denmark. Under Danish law, it is permissible for shareholders to take action and pass resolutions by written consent in the event of unanimity. However, this will normally not be the case in listed companies and for a listed company, this method of adopting resolutions is generally not feasible.

Delaware. Although permitted by Delaware law, publicly listed companies do not typically permit stockholders of a corporation to take action by written consent.

Denmark. The concept of appraisal rights does not exist under Danish law, except in connection with statutory redemptions rights according to the Danish Companies Act.

According to Section 73 of the Danish Companies Act, a minority shareholder may require a majority shareholder that holds more than 90% of the company's registered share capital to redeem his or her shares. Similarly, a majority shareholder holding more than 90% of the company's share capital may, according to Section 70 of the same act, squeeze out the minority shareholders. In the event that the parties cannot agree to the redemption squeeze out price, this shall be determined by an independent evaluator appointed by the court. Additionally, there are specific regulations in Sections 249, 267, 285 and 305 of the Danish Companies Act that require compensation in the event of national or cross-border mergers and demergers. Moreover, shareholders who vote against a cross-border merger or demerger are, according to Sections 286 and 306 of the Danish Companies Act, entitled to have their shares redeemed.

Delaware. The Delaware General Corporation Law provides for stockholder appraisal rights, or the right to demand payment in cash of the judicially determined fair value of the stockholder's shares, in connection with certain mergers and consolidations.

Denmark. Under Danish law, only a company itself can bring a civil action against a third party; an individual shareholder does not have the right to bring an action on behalf of a company. However, if shareholders representing at least 10% of the share capital at a general meeting have opposed a decision to grant discharge to a member of our board of directors or our executive management or refrain from bringing law suits against, among other persons, a member of our board of directors or executive management, a shareholder may bring a derivative action on behalf of our Company against, among other persons, a member of our board of directors or executive management. An individual shareholder may, in its own name, have an individual right to take action against such third party in the event that the cause for the liability of that third party also constitutes a negligent act directly against such individual shareholder.

Delaware. Under the Delaware General Corporation Law, a stockholder may bring a derivative action on behalf of the corporation to enforce the rights of the corporation. An individual also may commence a class action suit on behalf of himself and other similarly situated stockholders where the requirements for maintaining a class action under Delaware law have been met. A person may institute and maintain such a suit only if that person was a stockholder at the time of the transaction

which is the subject of the suit. In addition, under Delaware case law, the plaintiff normally must be a stockholder at the time of the transaction that is the subject of the suit and throughout the duration of the derivative suit. Delaware law also requires that the derivative plaintiff make a demand on the directors of the corporation to assert the corporate claim before the suit may be prosecuted by the derivative plaintiff in court, unless such a demand would be futile.

Denmark. Danish limited liability companies may not subscribe for newly issued shares in their own capital. Such company may, however, according to the Danish Companies Act Sections 196-201, acquire fully paid shares of its own company, provided that the board of directors has been authorized to do so by the shareholders at a general meeting. Such authorization can only be given for a maximum period of five years and the authorization shall fix (i) the maximum value of the shares and (ii) the minimum and the highest amount that the company may pay for the shares. Such purchase of shares may generally only be acquired using distributable reserves.

Delaware. Under the Delaware General Corporation Law, a corporation may purchase or redeem its own shares unless the capital of the corporation is impaired or the purchase or redemption would cause an impairment of the capital of the corporation. A Delaware corporation may, however, purchase or redeem out of capital any of its preferred shares or, if no preferred shares are outstanding, any of its own shares if such shares will be retired upon acquisition and the capital of the corporation will be reduced in accordance with specified limitations.

Denmark. Under Danish law, it is possible to implement limited protective anti-takeover measures. Such provisions may include, among other things, (i) different share classes with different voting rights and (ii) notification requirements concerning participation in general meetings. We have currently not adopted any such provisions.

Delaware. In addition to other aspects of Delaware law governing fiduciary duties of directors during a potential takeover, the Delaware General Corporation Law also contains a business combination statute that protects Delaware companies from hostile takeovers and from actions following the takeover by prohibiting some transactions once an acquirer has gained a significant holding in the corporation.

Section 203 of the Delaware General Corporation Law prohibits "business combinations," including mergers, sales and leases of assets, issuances of securities and similar transactions by a corporation or a subsidiary with an interested stockholder that beneficially owns 15% or more of a corporation's voting stock, within three years after the person becomes an interested stockholder, unless:

A Delaware corporation may elect not to be governed by Section 203 by a provision contained in the original certificate of incorporation of the corporation or an amendment to the original certificate of incorporation or to the bylaws of the company, which amendment must be approved by a majority of the shares entitled to vote and may not be further amended by the board of directors of the corporation. Such an amendment is not effective until 12 months following its adoption.

Denmark. According to Section 150 of the Danish Companies Act, a shareholder may, at the annual general meeting or at a general meeting whose agenda includes such item, request an inspection of the company's books regarding specific issues concerning the management of the company or specific annual reports. If approved by shareholders with a simple majority, one or more investigators are elected. If the proposal is not approved by a simple majority but 25% of the share capital votes in favor of the proposal, then the shareholder can request the court to appoint an investigator.

Delaware. Under the Delaware General Corporation Law, any stockholder may inspect certain of the corporation's books and records, for any proper purpose, during the corporation's usual hours of business.

Denmark. As a general rule, shareholders of the company are entitled to subscribe for new shares in proportion to their existing shareholdings in the event of a cash increase of the share capital. Such a cash increase of the share capital can be resolved by the general meeting by at least two-thirds of the votes cast as well as at least two-thirds of the share capital represented at the general meeting.

However, in the below-mentioned scenarios, the general meeting may resolve to depart from the shareholders' right to proportionate subscription if the following voting requirements are met:

The board of directors may resolve to increase our share capital without pre-emptive subscription rights for existing shareholders pursuant to the authorizations described above under the caption "Authorizations to the Board of Directors."

Unless future issuances of new shares are registered under the Securities Act or with any authority outside Denmark, U.S. shareholders and shareholders in jurisdictions outside Denmark may be unable to exercise their pre-emptive subscription rights under U.S. securities law.

Delaware. Under the Delaware General Corporation Law, stockholders have no pre-emptive rights to subscribe for additional issues of stock or to any security convertible into such stock unless, and to the extent that, such rights are expressly provided for in the certificate of incorporation.

Denmark. Under Danish law, the distribution of ordinary and extraordinary dividends requires the approval of a company's shareholders at a company's general meeting. In addition the shareholders may authorize the board of directors to distribute extraordinary dividends. The shareholders may not resolve to the distribution of dividends in excess of the recommendation from the board of directors and we may only pay out dividends from our distributable reserves, which are defined as results from operations carried forward and reserves that are not bound by law after deduction of loss carried forward. It is possible under Danish law to pay out interim dividends. The decision to pay out interim dividends shall be accompanied by a balance sheet, and the board of directors determines whether it will be sufficient to use the statement of financial position from the annual report or if an interim statement of financial position for the period from the annual report period until the interim dividend payment shall be prepared. If interim dividends are paid out later than six months following the end of the financial year for the latest annual report, an interim balance sheet showing that there are sufficient funds shall always be prepared.

Delaware. Under the Delaware General Corporation Law, a Delaware corporation may pay dividends out of its surplus (the excess of net assets over capital), or in case there is no surplus, out of its net profits for the fiscal year in which the dividend is declared and/or the preceding fiscal year (provided that the amount of the capital of the corporation is not less than the aggregate amount of the capital represented by the issued and outstanding stock of all classes having a preference upon the distribution of assets). In determining the amount of surplus of a Delaware corporation, the assets of the corporation, including stock of subsidiaries owned by the corporation, must be valued at their fair market value as determined by the board of directors, without regard to their historical book value. Dividends may be paid in the form of shares, property or cash.

Denmark. Under Danish law, all amendments to the articles of association shall be approved by the general meeting of shareholders with a minimum of two-thirds of the votes cast and two-thirds of the represented share capital. The same applies to solvent liquidations, mergers with the company as the discontinuing entity, mergers with the company as the continuing entity if shares are issued in connection therewith and demergers. Under Danish law, it is debatable whether the shareholders must approve a decision to sell all or virtually all of the company's business/assets.

Delaware. Under the Delaware General Corporation Law, the vote of a majority of the outstanding shares of capital stock entitled to vote thereon generally is necessary to approve a merger or consolidation or the sale of all or substantially all of the assets of a corporation. The Delaware General Corporation Law permits a corporation to include in its certificate of incorporation a provision requiring for any corporate action the vote of a larger portion of the stock or of any class or series of stock than would otherwise be required. However, under the Delaware General Corporation Law, no vote of the stockholders of a surviving corporation to a merger is needed, unless required by the certificate of incorporation, if (1) the agreement of merger does not amend in any respect the certificate of incorporation of the surviving corporation, (2) the shares of stock of the surviving corporation are not changed in the merger and (3) the number of shares of common stock

of the surviving corporation into which any other shares, securities or obligations to be issued in the merger may be converted does not exceed 20% of the surviving corporation's common stock outstanding immediately prior to the effective date of the merger. In addition, stockholders may not be entitled to vote in certain mergers with other corporations that own 90% or more of the outstanding shares of each class of stock of such corporation, but the stockholders will be entitled to appraisal rights.

Denmark. All resolutions made by the general meeting may be adopted by a simple majority of the votes, subject only to the mandatory provisions of the Danish Companies Act and the articles of association. Resolutions concerning all amendments to the articles of association must be passed by two-thirds of the votes cast as well as two-thirds of the share capital represented at the general meeting. Certain resolutions, which limit a shareholder's ownership or voting rights, are subject to approval by a nine-tenth majority of the votes cast and the share capital represented at the general meeting. Decisions to impose any or increase any obligations of the shareholders towards the company require unanimity.

Delaware. Under the Delaware General Corporation Law, a corporation's certificate of incorporation may be amended only if adopted and declared advisable by the board of directors and approved by a majority of the outstanding shares entitled to vote, and the bylaws may be amended with the approval of a majority of the outstanding shares entitled to vote and may, if so provided in the certificate of incorporation, also be amended by the board of directors.

The transfer agent and registrar for our shares is Computershare A/S, Kongevejen 418, Øverød, DK-2840 Holte, Denmark. Deutsche Bank Trust Company Americas will serve as the depositary for our ADSs.

Deutsche Bank Trust Company Americas, as depositary, will register and deliver our ADSs. Each ADS will represent one-third of a share (or a right to receive one-third of an ordinary share) deposited with Danske Bank A/S, or any successor, as custodian for the depositary. Each ADS will also represent any other securities, cash or other property which may be held by the depositary in respect of the deposited shares. The depositary's corporate trust office at which the ADSs will be administered is located at 60 Wall Street, New York, New York 10005, USA. The depositary's principal executive office is located at 60 Wall Street, New York, New York 10005, USA.

You may hold ADSs either: (1) directly (a) by having an American Depositary Receipt, also referred to as an ADR, which is a certificate evidencing a specific number of ADSs, registered in your name, or (b) by having ADSs registered in your name in the Direct Registration System; or DRS, or (2) indirectly by holding a security entitlement in ADSs through your broker or other financial institution. If you hold ADSs directly, you are a registered ADS holder, also referred to as an ADS holder. This description assumes you are an ADS holder. If you hold the ADSs indirectly, you must rely on the procedures of your broker or other financial institution to assert the rights of ADS holders described in this section. You should consult with your broker or financial institution to find out what those procedures are.

The DRS is a system administered by the DTC pursuant to which the depositary may register the ownership of uncertificated ADSs, which ownership is confirmed by periodic statements sent by the depositary to the registered holders of uncertificated ADSs. ADSs will be issued through DRS unless you specifically request certificated ADRs.

As an ADS holder, you will not be treated as one of our shareholders and you will not have shareholder rights. Danish law governs shareholder rights. The depositary will be the holder of the shares underlying your ADSs. As a holder of ADSs, you will have ADS holder rights. A deposit agreement among us, the depositary and you, as an ADS holder, and all beneficial owners of ADSs sets out ADS holder rights as well as the rights and obligations of the depositary. New York law governs the deposit agreement and the ADSs.

We currently maintain a Level 1 American Depositary Receipt program in the United States sponsored by the depositary, through which our outstanding ADSs are traded over-the-counter in the United States under the symbol "BVNRY." As of December 30, 2015, the depositary has informed us that there were 31,417 ADSs outstanding. Upon approval (if granted) of our application to list the ADSs offered hereby on The NASDAQ Global Select Market, the outstanding ADSs will also be uplisted to The NASDAQ Global Select Market, and will thereafter trade alongside the ADSs offered hereby under the symbol "BAVN" upon commencement of trading on The NASDAQ Global Select Market, which is anticipated to commence at the opening of such exchange immediately following the pricing of this offering.

The following is a summary of the material provisions of the deposit agreement. For more complete information, you should read the entire deposit agreement and the form of American Depositary Receipt. For directions on how to obtain copies of those documents see the section of this Prospectus titled "Where You Can Find Additional Information."

The depositary has agreed to pay you the cash dividends, share distributions or the proceeds of other distributions it or the custodian receives on shares, after deducting its fees and expenses. You will receive these distributions in proportion to the number of shares your ADSs represent.

Cash. After completion of this offering, we do not expect to declare or pay any cash dividends or cash distributions on our shares for the foreseeable future. The depositary will convert any cash dividend or other cash distribution we pay on the shares or any net proceeds from the sale of any shares, rights, securities or other entitlements in any foreign currency, including Danish kroner, into U.S. dollars if it can do so on a practicable basis, and can transfer the U.S. dollars to the United States. If that is not practical or lawful or if any government approval is needed and is denied or is not obtainable at a reasonable cost and within a reasonable period, the deposit agreement allows the depositary to distribute the foreign currency to the ADS holders or to hold the foreign currency for the account of the ADS holders, in which case it will not invest the foreign currency and it will not be liable for any interest. Before making a distribution, any taxes or other governmental charges, together with fees and expenses of the depositary that must be paid, will be deducted. See "Certain Material U.S. Federal Income Tax Considerations" and "Certain Material Danish Tax Considerations." The depositary will distribute only whole U.S. dollars and cents and will round fractional cents to the nearest whole cent. Before making a distribution, any taxes or other governmental charges, together with fees and expenses of the depositary, that must be paid, will be deducted. If the exchange rates fluctuate during a time when the depositary cannot convert the foreign currency, you may lose some or all of the value of the distribution.

Shares. The depositary may distribute additional ADSs representing any shares we distribute as a dividend or free distribution to the extent reasonably practicable and permissible under law. The depositary will only distribute whole ADSs. It will sell shares which would require it to deliver a fractional ADS and distribute the net proceeds in the same way as it does with cash. If the depositary does not distribute additional ADSs, the outstanding ADSs will, to the extent permissible by law, also represent the new shares. The depositary may also sell all or a portion of the shares that it has not distributed, and distribute the net proceeds in the same way as it does with cash. In addition, the depositary may sell all or a portion of the distributed shares sufficient to pay its fees and expenses and any taxes and governmental charges in connection with that distribution.

Elective Distributions in Cash or Shares. If we offer holders of our shares the option to receive dividends in either cash or shares, the depositary will make the distribution to ADS holders pro rata in the manner that we indicate is the default option for shareholders who fail to make such an election.

Rights to Purchase Additional Shares. If we offer holders of our shares any rights to subscribe for additional shares or any other rights, the depositary may, if it determines it is lawful and reasonably practicable to do so, endeavour to sell the rights and distribute the proceeds in the same way as it does with cash distributions. The depositary will allow rights that are not distributed or sold to lapse. In that case, you will receive no value for them.

The depositary may sell a portion of the distributed rights sufficient to pay its fees and expenses, and any taxes and governmental charges, in connection with that distribution.

Other Distributions. The depositary will endeavor to sell any other property delivered by us to our shareholders, and distribute the net proceeds to ADS holders, in the same way as it does with cash. If the depositary is unable to sell what we distributed, it may dispose of such property in any way it deems reasonably practicable under the circumstances for nominal or no consideration. In

addition, the depositary may sell a portion of the distributed securities or property sufficient to pay its fees and expenses and any taxes and governmental charges in connection with that distribution.

The depositary will deliver ADSs if you or your broker deposits shares or evidence of rights to receive shares with the custodian. Upon payment of its fees and expenses and of any taxes or charges, such as stamp taxes or share transfer taxes or fees, and delivery of any required endorsements, certifications or other instruments of transfer required by the depositary, the depositary will register the appropriate number of ADSs in the names you request and will deliver the ADSs to or upon the order of the person or persons entitled thereto.

You may surrender your ADSs at the depositary's principal office. Upon payment of its fees and expenses and of any taxes or charges, such as stamp taxes or share transfer taxes or fees, the depositary will transfer and deliver the shares and any other deposited securities underlying the ADSs to you or a person designated by you at the office of the custodian or through a book-entry delivery. Alternatively, at your request, risk and expense, the depositary will transfer and deliver the deposited securities at its principal office, to the extent permitted by law. If you withdraw the deposited securities underlying the ADSs, you will not be eligible to re-convert such securities into ADSs.

How can ADS holders interchange between certificated ADSs and uncertificated ADSs?

You may surrender your ADRs to the depositary for the purpose of exchanging your ADRs for uncertificated ADSs. The depositary will cancel the ADRs and will send you a statement confirming that you are the owner of uncertificated ADSs. Alternatively, upon receipt by the depositary of a proper instruction from a registered holder of uncertificated ADSs requesting the exchange of uncertificated ADSs for certificated ADSs, the depositary will execute and deliver to you an ADR evidencing those ADSs.

ADS holders may only exercise voting rights with respect to the shares underlying their respective ADSs in accordance with the provisions of the deposit agreement, which provides that a holder may vote the shares underlying the ADSs for any particular matter to be voted on by our shareholders either by withdrawing the shares underlying the ADSs, or, to the extent permitted by applicable law and as permitted by the depositary, by requesting a temporary registration as shareholder and authorizing the depositary to act as proxy. To the extent permitted by applicable law and as permitted by the depositary, a temporary registration entails that you will be treated as having requested a temporary individual registration in the share register only with effect for the general meeting in question. The temporary registration will be deleted from the share register immediately after the general meeting. A temporary registration will entail that you may attend and vote at the general meeting in question, or appoint the depositary as a proxy to vote on your behalf thereat. Such withdrawal or temporary registration procedure would be necessary for you to vote the shares underlying your ADSs at our 2016 annual general meeting.

Absent withdrawal or, to the extent permitted by applicable law and as permitted by the depositary, temporary registration and proxy, Danish law prevents the depositary from differentiated voting at our general meetings unless our articles of association specifically allow for this, which is

currently not the case, meaning that all votes on the shares held by the depositary, including those underlying the ADSs issued in this offering, would need to be cast either in favor of or against any proposal at our general meetings, if such shares are voted at all. Our board of directors is committed to using reasonable efforts to work towards removing this restriction at our 2016 annual general meeting. If this restriction is removed, the depositary would be able to vote the shares registered in its name that underlie the ADSs to more closely reflect the votes of the ADS holders, thereby effectively permitting pass-through voting by ADS holders who indicate their voting preference to the depositary in accordance with and subject to the depositary's procedures.

Thereafter, you may instruct the depositary to vote the number of whole deposited shares or other deposited securities your ADSs represent. If we ask for your instructions and upon timely notice from us as described in the deposit agreement, the depositary will notify you of the upcoming vote and arrange to deliver our voting materials to you by regular, ordinary mail delivery, or by electronic transmission. The materials will (1) describe the matters to be voted on and (2) explain how you may instruct the depositary to vote the shares or other deposited securities underlying your ADSs as you direct. For instructions to be valid, they must reach the depositary by a date set by the depositary. The depositary will try, as far as practical, and subject to applicable law and the provisions of the deposit agreement, the deposited securities and our constituent documents, to vote or to cause its custodian to vote the shares or other deposited securities as instructed by ADS holders.

We cannot assure you that you will receive the voting materials in time to ensure that you can instruct the depositary to vote the shares underlying your ADSs. In addition, the depositary and its agents are not responsible for failing to carry out voting instructions or for the manner in which such vote is cast or the effect of any such vote. This means that you may not be able to exercise your right to vote and you may have no recourse if the shares underlying your ADSs are not voted as you requested.

In order to give you a reasonable opportunity to instruct the depositary as to the exercise of voting rights relating to deposited securities, if we request the depositary to act, we will try to give the depositary notice of any such meeting and details concerning the matters to be voted upon sufficiently in advance of the meeting date.

As an ADS holder, you will be required to pay the following service fees to the depositary and certain taxes and governmental charges (in addition to any applicable fees, expenses, taxes and other governmental charges payable on the deposited securities represented by any of your ADSs):

In addition, ADS holders, beneficial owners of ADSs, persons depositing shares and persons surrendering ADSs for cancellation and withdrawal of deposited securities will be required to pay the following charges:

The depositary fees payable upon the issuance and cancellation of ADSs are typically paid to the depositary bank by the brokers (on behalf of their clients) receiving the newly issued ADSs from the depositary bank and by the brokers (on behalf of their clients) delivering the ADSs to the depositary bank for cancellation. The brokers in turn charge these fees to their clients. Depositary fees payable in connection with distributions of cash or securities to ADS holders and the depositary services fee are charged by the depositary bank to the holders of record of ADSs as of the applicable ADS record date.

The depositary fees payable for cash distributions are generally deducted from the cash being distributed or by selling a portion of distributable property to pay the fees. In the case of distributions other than cash (i.e., share dividends or rights), the depositary bank charges the applicable fee to the ADS record date holders concurrent with the distribution. In the case of ADSs registered in the name of the investor (whether certificated or uncertificated in direct registration), the depositary bank sends invoices to the applicable record date ADS holders. In the case of ADSs held in brokerage and custodian accounts (via DTC), the depositary bank generally collects its fees through the systems provided by DTC (whose nominee is the registered holder of the ADSs held in DTC) from the brokers and custodians holding ADSs in their DTC accounts. The brokers and custodians who hold their clients' ADSs in DTC accounts in turn charge their clients' accounts the amount of the fees paid to the depositary banks.

In the event of refusal to pay the depositary fees, the depositary bank may, under the terms of the deposit agreement, refuse the requested service until payment is received or may set off the amount of the depositary fees from any distribution to be made to the ADS holder.

You will be responsible for any taxes or other governmental charges payable on your ADSs or on the deposited securities represented by any of your ADSs. The depositary may refuse to register or transfer your ADSs or allow you to withdraw the deposited securities represented by your ADSs until such taxes or other charges are paid. It may apply payments owed to you or sell deposited securities represented by your ADSs to pay any taxes owed and you will remain liable for any deficiency. If the depositary sells deposited securities, it will, if appropriate, reduce the number of ADSs registered in your name to reflect the sale and pay you any net proceeds, or send you any property, remaining after it has paid the taxes. You agree to indemnify us, the depositary, the custodian and each of our and their respective agents, directors, employees and affiliates for, and hold each of them harmless from, any claims with respect to taxes and additions to tax (including applicable interest and penalties thereon) arising from any refund of taxes, reduced rate of withholding at source or other tax benefit obtained for or by you. Your obligations under this paragraph shall survive any transfer of ADRs, any surrender of ADRs and withdrawal of deposited securities or the termination of the deposit agreement.

The depositary is under no obligation to provide the holders and beneficial owners of ADSs with any information about the tax status of our company and shall not incur any liability for any tax consequences that may be incurred by holders and beneficial owners on account of their ownership of the ADSs, including, without limitation, tax consequences resulting from our company (or any of our subsidiaries) being treated as a "Passive Foreign Investment Company" (as defined in the U.S. Internal Revenue Code and the regulations issued thereunder) or otherwise.

Upon any change in our par value, split-up, subdivision cancellation, consolidation or any other reclassification of our shares, or upon any recapitalization, reorganization, merger, amalgamation or consolidation or sale of assets affecting us or to which we otherwise are a party, any securities which shall be received by the depositary or a custodian in exchange for, or in conversion of or replacement or otherwise in respect of, our shares shall, to the extent permitted by law, be treated as new deposited securities under the deposit agreement, and the ADRs shall, subject to the provisions of the deposit agreement and applicable law, evidence ADSs representing the right to receive such additional securities. Alternatively, the depositary may, with our approval, which approval shall not be unreasonably withheld, and shall, if we shall so request, subject to the terms of the deposit agreement and receipt of an opinion of our counsel satisfactory to the depositary that such distributions are not in violation of any applicable laws or regulations, execute and deliver additional ADRs as in the case of a stock dividend on our shares, or call for the surrender of outstanding ADRs to be exchanged for new ADRs, in either case, as well as in the event of newly deposited shares, with necessary modifications to the form of ADR specifically describing such new deposited securities and/or corporate change. Notwithstanding the foregoing, in the event that any security so received may not be lawfully distributed to some or all ADS holders, the depositary may, with our approval, which approval shall not be unreasonably withheld, and shall if we request, subject to receipt of an opinion from our counsel satisfactory to the depositary that such distributions are not in violation of any applicable laws or regulations, sell such securities at public or private sale, at such place or places and upon such terms as it may deem proper and may allocate the net proceeds of such sales (net of fees and charges of, and expenses incurred by, the depositary and taxes and governmental charges) for the account of the ADS holders otherwise entitled to such securities upon an averaged or other practicable basis without regard to any distinctions among such ADS holders and distribute the net proceeds so allocated to the extent practicable as in the case of a distribution received in cash pursuant to the deposit agreement. In accordance with the provisions of the deposit agreement, neither we nor the depositary are responsible for (i) any failure to determine that it may be lawful or feasible to make such securities available to ADS holders in general or any ADS holder in particular, (ii) any foreign exchange exposure or loss incurred in connection with such sale, or (iii) any liability to the purchaser of such securities.

We may agree with the depositary to amend the deposit agreement and the ADRs without your consent for any reason. If an amendment adds or increases fees or charges, except for taxes and other governmental charges, charges in connection with foreign exchange control regulations, delivery charges or similar items, or materially prejudices a substantial existing right of ADS holders, it will not become effective for outstanding ADSs until 30 days after the depositary notifies ADS holders of the amendment. At the time an amendment becomes effective, you are considered, by continuing to hold your ADSs, to agree to the amendment and to be bound by the ADRs and the deposit agreement as amended. If any new laws are adopted which would require the deposit agreement to be amended in order to comply therewith, we and the depositary may amend the

deposit agreement in accordance with such laws and such amendment may become effective before notice thereof is given to ADS holders.

The depositary will terminate the deposit agreement at our direction by mailing notice of termination to the ADS holders then outstanding at least 90 days prior to the date fixed in such notice for such termination. The depositary may also terminate the deposit agreement by mailing a notice of termination to us and the ADS holders if 90 days have passed since the depositary told us it wants to resign or since we notified the depositary that it is being removed, but a successor depositary has not been appointed and accepted its appointment. In either such case, the depositary must notify you at least 30 days before termination.

After termination, the depositary and its agents will do the following under the deposit agreement, but nothing else: collect distributions on the deposited securities, sell rights and other property and deliver shares and other deposited securities upon cancellation of ADSs after payment of any fees, charges, taxes or other governmental charges. Six months after termination, the depositary may sell any remaining deposited securities by public or private sale. After that, the depositary will hold the money it received on the sale, as well as any other cash it is holding under the deposit agreement for the pro rata benefit of the ADS holders that have not surrendered their ADSs. It will not invest the money and has no liability for interest. The depositary's only obligations will be to account for the money and other cash. After termination, we will have no obligations under the deposit agreement except for our obligations to the depositary.

The depositary will maintain ADS holder records at its depositary office. You may inspect such records at such office during regular business hours, but solely for the purpose of communicating with other holders in the interest of the business of our company or matters relating to the ADSs or the deposit agreement.

The depositary will maintain facilities in New York to record and process the issuance, cancellation, combination, split-up and transfer of ADRs.

These facilities may be closed from time to time, to the extent not prohibited by law or if any such action is deemed necessary or advisable by the depositary or us, in good faith, at any time or from time to time because of any requirement of law, any government or governmental body or commission or any securities exchange on which the ADRs or ADSs are listed, or under any provision of the deposit agreement or provisions of, or governing, the deposited securities, or any meeting of our shareholders or for any other reason.

Limits on our obligations and the obligations of the depositary; limits on liability to holders of ADSs

The deposit agreement expressly limits our obligations and the obligations of the depositary. It also limits our liability and the liability of the depositary and its directors, officers, affiliates, employees and agents. We and the depositary and each of our and their respective directors, officers, affiliates, employees and agents:

We and the depositary, each of our and the depositary's controlling persons and agents, and the custodian may rely and shall be protected in acting upon any written notice, request, opinion or other document believed by it to be genuine and to have been signed or presented by the proper party.

In addition, we, the depositary and the custodian are not liable to ADS holders, beneficial owners of ADSs or any third parties:

Neither we, the depositary or the custodian are liable for the failure by any ADS holder or beneficial owner to obtain the benefits of credits on the basis of non-U.S. tax paid against such ADS holder's or beneficial owner's income tax liability. The depositary and any of its agents also disclaim any liability for any failure to carry out any instructions to vote, the manner in which any vote is cast, provided that any such action or omission is in good faith, or the effect of any vote, or any failure to determine that any distribution or action may be lawful or reasonably practicable or for allowing any rights to lapse in accordance with the provisions of the deposit agreement, the failure or timeliness of any notice from us, the content of any information submitted to it by us for distribution to you or for any inaccuracy of any translation thereof, any investment risk associated with the acquisition of an interest in the deposited securities, the validity or worth of the deposited securities, the credit

worthiness of any third party, or for any tax consequences that may result from ownership of ADSs, shares or deposited securities. The depositary and its agents shall not be liable for any acts or omissions made by a successor depositary whether in connection with a previous act or omission of the depositary or in connection with any matter arising wholly after the removal or resignation of the depositary, provided that in connection with the issue out of which such potential liability arises the depositary performed its obligations without gross negligence or willful misconduct while it acted as depositary. The depositary and its directors, officers, employees, agents and affiliates shall not be liable for any indirect, special, punitive or consequential damages to us the holders or beneficial owners of ADSs or any other person.

In addition, the deposit agreement provides that each party to the deposit agreement, including each holder, beneficial owner and holder of interests in the ADRs, irrevocably waives, to the fullest extent permitted by applicable law, any right it may have to a trial by jury in any lawsuit or proceeding against the depositary or our company related to our shares, the ADSs or the deposit agreement.

In the deposit agreement, we and the depositary agree to indemnify each other under certain circumstances.

Before the depositary will issue, deliver or register a transfer of an ADS, split-up, subdivide or combine ADSs, make a distribution on an ADS, or permit withdrawal of shares, the depositary may require:

The depositary may refuse to deliver ADSs or register transfers of ADSs generally when the transfer books of the depositary or our transfer books are closed or at any time if the depositary or we think it is necessary or advisable to do so.

ADS holders have the right to cancel their ADSs and withdraw the underlying shares at any time except:

This right of withdrawal may not be limited by any other provision of the deposit agreement.

The deposit agreement permits the depositary to deliver ADSs before deposit of the underlying shares. This is called a pre-release of the ADSs. The depositary may also deliver shares upon cancellation of pre-released ADSs, even if the ADSs are cancelled before the pre-release transaction has been closed out. A pre-release is closed out as soon as the underlying shares are delivered to the depositary.

The depositary may receive ADSs instead of shares to close out a pre-release. The depositary may pre-release ADSs only under the following conditions: (1) before or at the time of the pre-release, the person to whom the pre-release is being made (a) represents to the depositary in writing that it or its customer owns the shares or ADSs to be deposited, (b) agrees to indicate the depositary as owner of such shares or ADSs in its records and to hold such shares or ADSs in trust for the depositary until such shares or ADSs are delivered to the depositary or the custodian, (c) unconditionally guarantees to deliver such shares or ADSs to the depositary or the custodian, as the case may be, and (d) agrees to any additional restrictions or requirements that the depositary deems appropriate; (2) the pre-release is fully collateralized with cash, U.S. government securities or other collateral that the depositary considers appropriate; (3) the depositary must be able to close out the pre-release on not more than five business days' notice; and (4) the pre-release is subject to such further indemnities and credit regulations as the depositary deems appropriate. In addition, the depositary will normally limit the number of ADSs that may be outstanding at any time as a result of pre-release to 30% of the aggregate number of ADSs then outstanding, although the depositary may disregard the limit from time to time, if it thinks it is appropriate to do so.

The deposit agreement provides that, to the extent available by the depositary, ADSs shall be evidenced by ADRs issued through DRS/Profile unless certificated ADRs are specifically requested by the ADS holder. DRS is the system administered by DTC under which the depositary may register the ownership of uncertificated ADSs and such ownership will be evidenced by periodic statements sent by the depositary to the registered holders of uncertificated ADSs. Profile is a required feature of DRS that allows a DTC participant, claiming to act on behalf of a registered holder of ADSs, to direct the depositary to register a transfer of those ADSs to DTC or its nominee and to deliver those ADSs to the DTC account of that DTC participant without receipt by the depositary of prior authorization from the ADS holder to register that transfer.

In connection with and in accordance with the arrangements and procedures relating to DRS/Profile, the parties to the deposit agreement understand that the depositary will not verify, determine or otherwise ascertain whether the DTC participant that is claiming to be acting on behalf of an ADS holder in requesting registration of transfer and delivery described in the paragraph above has the actual authority to act on behalf of the ADS holder, notwithstanding any requirements under the Uniform Commercial Code.

Shareholder Communications; Inspection of Register of Holders of ADSs; ADS Holder Information

The depositary will make available for your inspection during normal business hours at its principal office all reports and communications that it receives from us as a holder of deposited securities that we make generally available to holders of deposited securities. The depositary will send you copies of those communications if we ask it to.

Our shares are admitted to trading and official listing on Nasdaq Copenhagen and our ADSs have been, until shortly before the consummation of this offering, traded in the over-the-counter market in the United States. Future sales of our shares or ADSs, including shares issued upon the exercise of outstanding warrants, in the public market after this offering, or the perception that those sales may occur, could cause the prevailing market price for our ADSs to fall or impair our ability to raise equity capital in the future.

Based on the number of shares outstanding as of December 31, 2015 and assuming (1) no exercise of the underwriters' option to purchase additional ADSs and (2) no exercise of any of our other outstanding warrants, we will have outstanding an aggregate of shares. All of our outstanding shares are freely tradeable on Nasdaq Copenhagen, all of the ADSs to be sold in this offering (representing shares) and any ADSs sold upon exercise of the underwriters' option to purchase additional ADSs, will be freely tradeable in the U.S. public market without restriction or further registration under the Securities Act, unless the ADSs are held by any of our "affiliates" as such term is defined in Rule 144 of the Securities Act (subject, in each case, to the terms of the lock-up agreements referred to below, as applicable). The number of ADSs available for sale immediately after this offering will be the number sold in this offering plus the number of ADSs available prior to this offering (reflecting any split or combination effected in conjunction with this offering) less any ADSs held by our directors and officers, who will be subject to lockup agreements for 90 days after the date of this prospectus.

In connection with this offering, we, our board members and our executive management have agreed, subject to certain exceptions, with the underwriters not to dispose of or hedge any of our or their ADSs, shares or securities convertible into or exchangeable for ADSs or shares during the period from the date of the lock-up agreement continuing through the date 90 days after the date of this prospectus, except with the prior written consent of the representatives of the underwriters. See "Underwriting—Lock-up Agreements." Following the lock-up periods set forth in the agreements described above, and assuming that the underwriters do not release any parties from these agreements, all of the ADSs and shares that are held by our "affiliates" as of the date of this prospectus will be eligible for sale in the public market in compliance with Rule 144 under the Securities Act.

Rule 144 provides an exemption from the registration requirements of the Securities Act for restricted securities and securities held by certain affiliates of an issuer being sold in the United States, to U.S. persons or through U.S. securities markets. In general, under Rule 144, as currently in effect, once we have been subject to the public company reporting requirements of the Exchange Act for at least 90 days, a person (or persons whose securities are required to be aggregated) who is not deemed to have been one of our "affiliates" for purposes of Rule 144 at any time during the three months preceding a sale, and who has beneficially owned restricted securities within the meaning of Rule 144 for at least six months, including the holding period of any prior owner other than one of our "affiliates," is entitled to sell such securities in the U.S. public market (subject to the lock-up agreements referred to above, if applicable) without complying with the manner of sale, volume limitations or notice provisions of Rule 144, but subject to compliance with the public information requirements of Rule 144. If such a person has beneficially owned the securities proposed to be sold for at least one year, including the holding period of any prior owner other than "affiliates," then such person is entitled to sell such securities in the public market without complying

with any of the requirements of Rule 144 (subject to the lock-up agreement referred to above, if applicable). In general, under Rule 144, as currently in effect, once we have been subject to the public company reporting requirements of the Exchange Act for at least 90 days, our "affiliates," as defined in Rule 144, who have beneficially owned the securities proposed to be sold for at least six months are entitled to sell in the public market, upon expiration of any applicable lock-up agreements and within any three-month period, a number of those securities that does not exceed the greater of:

Such sales under Rule 144 by our "affiliates" or persons selling ADSs on behalf of our "affiliates" are also subject to certain manner of sale provisions, notice requirements and to the availability of current public information about us.

The following is a summary of certain material U.S. federal income tax considerations relating to the ownership and disposition of ADSs by a U.S. holder (as defined below). This summary addresses only the U.S. federal income tax considerations for U.S. holders that are initial purchasers of the ADSs pursuant to this offering and that will hold such ADSs as capital assets. This summary does not address all U.S. federal income tax matters that may be relevant to a particular U.S. holder. This summary does not address tax considerations applicable to a holder of ADSs that may be subject to special tax rules including, without limitation, the following:

Further, this summary does not address the U.S. federal estate, gift, or alternative minimum tax considerations, or any U.S. state, local, or non-U.S. tax considerations of the acquisition, ownership and disposition of the ADSs.

This description is based on the U.S. Internal Revenue Code of 1986, as amended or the Code, existing, proposed and temporary U.S. Treasury Regulations promulgated thereunder and administrative and judicial interpretations thereof, in each case as in effect and available on the date hereof. All of the foregoing is subject to change, which change could apply retroactively, and to differing interpretations, all of which could affect the tax considerations described below. There can be no assurances that the U.S. Internal Revenue Service or the IRS, will not take a position concerning the tax consequences of the acquisition, ownership and disposition of the ADSs that is contrary to the tax treatment described herein or that such a position would not be sustained by a court.

For the purposes of this summary, a "U.S. holder" is a beneficial owner of ADSs that is (or is treated as), for U.S. federal income tax purposes:

If a partnership (or any other entity treated as a partnership for U.S. federal income tax purposes) holds ADSs, the U.S. federal income tax consequences relating to an investment in the ADSs will depend in part upon the status of the partner and the activities of the partnership. Such a partner or partnership should consult its tax advisor regarding the U.S. federal income tax considerations of acquiring, owning and disposing of the ADSs in its particular circumstances.

Persons considering an investment in the ADSs should consult their own tax advisors as to the particular tax consequences applicable to them relating to the acquisition, ownership and disposition of the ADSs, including the applicability of U.S. federal, state and local tax laws and non-U.S. tax laws.

Distributions. Subject to the discussion under "Passive Foreign Investment Company Considerations" below, the gross amount of any distribution (including any amounts withheld in respect of foreign tax) actually or constructively received by a U.S. holder with respect to ADSs will be taxable to the U.S. holder as a dividend to the extent of the U.S. holder's pro rata share of our current or accumulated earnings and profits as determined under U.S. federal income tax principles. Distributions in excess of earnings and profits will be non-taxable to the U.S. holder to the extent of, and will be applied against and reduce, the U.S. holder's adjusted tax basis in the ADSs. Distributions in excess of earnings and profits and such adjusted tax basis will generally be taxable to the U.S. holder as either long-term or short-term capital gain depending upon whether the U.S. holder has held the ADSs for more than one year as of the time such distribution is received. However, since we do not calculate our earnings and profits under U.S. federal income tax principles, it is expected that any distribution will be reported as a dividend, even if that distribution would otherwise be treated as a non-taxable return of capital or as capital gain under the rules described above. Non-corporate U.S. holders may qualify for the preferential rates of taxation with respect to dividends on ADSs applicable to long-term capital gains (i.e., gains from the sale of capital assets held for more than one year) applicable to qualified dividend income (as discussed below) if we are a "qualified foreign corporation" and certain other requirements (discussed below) are met. A non-U.S. corporation (other than a corporation that is classified as a passive foreign investment company, or PFIC, for the taxable year in which the dividend is paid or the preceding taxable year) generally will be considered to be a qualified foreign corporation (a) if it is eligible for the benefits of a comprehensive tax treaty with the United States which the Secretary of Treasury of the United States determines is satisfactory for purposes of this provision and which includes an exchange of information provision, or (b) with respect to any dividend it pays on ADSs which are readily tradable on an established securities market in the United States. The ADSs are expected to be listed on The NASDAQ Global Select Market, which is an established securities market in the

United States, and we expect the ADSs to be readily tradable on The NASDAQ Global Select Market. There can be no assurance, however, that the ADSs will be considered readily tradable on an established securities market in the United States for purposes of the definition of a qualified foreign corporation. The Company, which is incorporated under the laws of Denmark, believes that it qualifies as a resident of Denmark for purposes of, and is eligible for the benefits of, the Convention between the Government of the United States of America and the Government of the Kingdom of Denmark for the Avoidance of Double Taxation and the Prevention of Fiscal Evasion with Respect to Taxes on Income, signed August 19, 1999, or the Treaty, although there can be no assurance in this regard. Further, the IRS has determined that the Treaty is satisfactory for purposes of the qualified dividend rules and that it includes an exchange-of-information program. Therefore, subject to the discussion under "Passive Foreign Investment Company Considerations" below, such dividends will generally be "qualified dividend income" in the hands of individual U.S. holders, provided that a holding period requirement (more than 60 days of ownership, without protection from the risk of loss, during the 121-day period beginning 60 days before the ex-dividend date) and certain other requirements are met. The dividends will not be eligible for the dividends-received deduction generally allowed to corporate U.S. holders. A U.S. holder generally may claim the amount of any Danish withholding tax as either a deduction from gross income or a credit against U.S. federal income tax liability. However, the foreign tax credit is subject to numerous complex limitations that must be determined and applied on an individual basis. Generally, the credit cannot exceed the proportionate share of a U.S. holder's U.S. federal income tax liability that the attributable taxable income bears to such U.S. holder's worldwide taxable income. In addition, this limitation is calculated separately with respect to specific categories of income. The amount of a distribution with respect to the ADSs that is treated as a "dividend" may be lower for U.S. federal income tax purposes than it is for Danish income tax purposes, potentially resulting in a reduced foreign tax credit for the U.S. holder. Each U.S. holder should consult its own tax advisors regarding the foreign tax credit rules.

In general, distributions paid to a U.S. holder in a foreign currency will, for U.S. income tax purposes, be translated at the spot exchange rate on the day the U.S. holder receives the distribution, regardless of whether the foreign currency is converted into U.S. dollars at that time. Any foreign currency gain or loss a U.S. holder realizes on a subsequent conversion of foreign currency into U.S. dollars will be U.S. source ordinary income or loss. If dividends received in a foreign currency are converted into U.S. dollars on the day they are received, a U.S. holder should not be required to recognize foreign currency gain or loss in respect of the dividend.

Sale, Exchange or Other Taxable Disposition of the ADSs. A U.S. holder will generally recognize gain or loss for U.S. federal income tax purposes upon the sale, exchange or other taxable disposition of ADSs in an amount equal to the difference between the U.S. dollar value of the amount realized from such sale or exchange and the U.S. holder's tax basis for those ADSs. Subject to the discussion under "Passive Foreign Investment Company Considerations" below, this gain or loss will generally be a capital gain or loss. The adjusted tax basis in the ADSs generally will be equal to the cost of such ADSs. Capital gain from the sale, exchange or other taxable disposition of ADSs of a non-corporate U.S. holder is generally eligible for a preferential rate of taxation applicable to capital gains, if the non-corporate U.S. holder's holding period determined at the time of such sale, exchange or other taxable disposition for such ADSs exceeds one year (i.e., such gain is long-term taxable gain). The deductibility of capital losses for U.S. federal income tax purposes is subject to limitations under the Code. Any such gain or loss that a U.S. holder recognizes generally will be treated as U.S. source income or loss for foreign tax credit limitation purposes.

Medicare Tax. Certain U.S. holders that are individuals, estates or trusts are subject to a 3.8% tax on all or a portion of their "net investment income," which may include all or a portion of their dividend income and net gains from the disposition of ADSs. Each U.S. holder that is an individual,

estate or trust is urged to consult its tax advisors regarding the applicability of the Medicare tax to its income and gains in respect of its investment in the ADSs.

Passive Foreign Investment Company Considerations. If we are classified as a PFIC in any taxable year, a U.S. holder would be subject to special rules generally intended to reduce or eliminate any benefits from the deferral of U.S. federal income tax that a U.S. holder could derive from investing in a non-U.S. company that does not distribute all of its earnings on a current basis.

A corporation organized outside the United States generally will be classified as a PFIC for U.S. federal income tax purposes in any taxable year in which, after applying certain look-through rules with respect to the income and assets of its subsidiaries, either: (i) at least 75% of its gross income is "passive income" or (ii) at least 50% of the average quarterly value of its total gross assets (which would generally be measured by fair market value of our assets, and for which purpose the total value of our assets may be determined in part by the market value of the ADSs and our shares, which are subject to change) is attributable to assets that produce "passive income" or are held for the production of "passive income."

Passive income for this purpose generally includes dividends, interest, royalties, rents, gains from commodities and securities transactions, the excess of gains over losses from the disposition of assets which produce passive income, and includes amounts derived by reason of the temporary investment of funds raised in offerings of the ADSs. If a non-U.S. corporation owns directly or indirectly at least 25% by value of the stock of another corporation, the non-U.S. corporation is treated for purposes of the PFIC tests as owning its proportionate share of the assets of the other corporation and as receiving directly its proportionate share of the other corporation's income. If we are classified as a PFIC in any year with respect to which a U.S. holder owns the ADSs, we will continue to be treated as a PFIC with respect to such U.S. holder in all succeeding years during which the U.S. holder owns the ADSs, regardless of whether we continue to meet the tests described above, subject to the application of the elections described below.

The value of our assets may be determined in large part by reference to the market price of the ADSs and our shares, which is likely to fluctuate after this offering. In addition, the composition of our income and assets will be affected by how, and how quickly, we use the cash proceeds from this offering in our business. Whether we are a PFIC for any taxable year will depend on our assets and income in each year, and because this is a factual determination made annually after the end of each taxable year, there can be no assurance that we will not be considered a PFIC in any taxable year. Based on the composition of our gross income and assets in 2014, certain estimates of our gross income and assets for 2015, and the nature of our business, we do not believe that we were characterized as a PFIC in our 2014 taxable year and do not expect to be characterized as a PFIC for our taxable year ending December 31, 2015. However, there can be no assurance that we will not be considered a PFIC for any future taxable year, and our U.S. tax counsel has not provided any opinion regarding our PFIC status.

If we are a PFIC, and you are a U.S. holder, then unless you make one of the elections described below, a special tax regime will apply to both (a) any "excess distribution" by us to you (generally, your ratable portion of distributions in any year which are greater than 125% of the average annual distribution received by you in the shorter of the three preceding years or your holding period for the ADSs) and (b) any gain realized on the sale or other disposition of the ADSs. Under this regime, any excess distribution and realized gain will be treated as ordinary income and will be subject to tax as if (a) the excess distribution or gain had been realized ratably over your holding period, (b) the amount deemed realized in each year had been subject to tax in each year of that holding period at the highest marginal rate for such year (other than income allocated to the

current period or any taxable period before we became a PFIC, which would be subject to tax at the U.S. holder's regular ordinary income rate for the current year and would not be subject to the interest charge discussed below), and (c) the interest charge generally applicable to underpayments of tax had been imposed on the taxes deemed to have been payable in those years. In addition, dividend distributions made to you will not qualify for the lower rates of taxation applicable to long-term capital gains discussed above under "Distributions."

Certain elections exist that may alleviate some of the adverse consequences of PFIC status and would result in an alternative treatment (such as mark-to-market treatment) of the ADSs. If a U.S. holder makes the mark-to-market election, the U.S. holder generally will recognize as ordinary income any excess of the fair market value of the ADSs at the end of each taxable year over their adjusted tax basis, and will recognize an ordinary loss in respect of any excess of the adjusted tax basis of the ADSs over their fair market value at the end of the taxable year (but only to the extent of the net amount of income previously included as a result of the mark-to-market election). If a U.S. holder makes the election, the U.S. holder's tax basis in the ADSs will be adjusted to reflect these income or loss amounts. Any gain recognized on the sale or other disposition of ADSs in a year when we are a PFIC will be treated as ordinary income and any loss will be treated as an ordinary loss (but only to the extent of the net amount of income previously included as a result of the mark-to-market election). The mark-to-market election is available only if we are a PFIC and the ADSs are "regularly traded" on a "qualified exchange." The ADSs will be treated as "regularly traded" in any calendar year in which more than a de minimis quantity of the ADSs are traded on a qualified exchange on at least 15 days during each calendar quarter (subject to the rule that trades that have as one of their principal purposes the meeting of the trading requirement as disregarded). The NASDAQ Global Select Market is a qualified exchange for this purpose and, consequently, if the ADSs are regularly traded, the mark-to-market election will be available to a U.S. holder. U.S. holders should consult their tax advisors to determine whether this election would be available and if so, what the consequences of the alternative treatments would be in their particular circumstances.

We do not currently intend to provide the information necessary for U.S. holders to make qualified electing fund elections if we were treated as a PFIC for any taxable year.

If we are determined to be a PFIC, the general tax treatment for U.S. Holders described in this section would apply to indirect distributions and gains deemed to be realized by U.S. Holders in respect of any of our subsidiaries that also may be determined to be PFICs.

If a U.S. holder owns ADSs during any taxable year in which we are a PFIC, the U.S. holder generally will be required to file an IRS Form 8621 (Information Return by a Shareholder of a Passive Foreign Investment Company or Qualified Electing Fund) with respect to the company, generally with the U.S. holder's federal income tax return for that year. If our company were a PFIC for a given taxable year, then you should consult your tax advisor concerning your annual filing requirements.

The U.S. federal income tax rules relating to PFICs are complex. Prospective U.S. investors are urged to consult their own tax advisers with respect to the acquisition, ownership and disposition of the ADSs, the consequences to them of an investment in a PFIC, any elections available with respect to the ADSs and the IRS information reporting obligations with respect to the acquisition, ownership and disposition of the ADSs.

Backup Withholding and Information Reporting. U.S. holders generally will be subject to information reporting requirements with respect to dividends on ADSs and on the proceeds from the sale, exchange or disposition of ADSs that are paid within the United States or through U.S.-related

financial intermediaries, unless the U.S. holder is an "exempt recipient." In addition, U.S. holders may be subject to backup withholding on such payments, unless the U.S. holder provides a taxpayer identification number and a duly executed IRS Form W-9 or otherwise establishes an exemption. Backup withholding is not an additional tax, and the amount of any backup withholding will be allowed as a credit against a U.S. holder's U.S. federal income tax liability and may entitle such holder to a refund, provided that the required information is timely furnished to the IRS.

Certain Reporting Requirements With Respect to Payments of Offer Price. U.S. holders paying more than U.S. $100,000 for the ADSs generally may be required to file IRS Form 926 reporting the payment of the offer price for the ADSs to us. Substantial penalties may be imposed upon a U.S. holder that fails to comply. Each U.S. holder should consult its own tax advisor as to the possible obligation to file IRS Form 926.

Foreign Asset Reporting. Certain individual U.S. holders are required to report information relating to an interest in the ADSs, subject to certain exceptions (including an exception for shares held in accounts maintained by U.S. financial institutions) by filing IRS Form 8938 (Statement of Specified Foreign Financial Assets) with their federal income tax return. U.S. holders are urged to consult their tax advisors regarding their information reporting obligations, if any, with respect to their ownership and disposition of the ADSs.

THE DISCUSSION ABOVE IS A GENERAL SUMMARY. IT DOES NOT COVER ALL TAX MATTERS THAT MAY BE OF IMPORTANCE TO A PROSPECTIVE INVESTOR. EACH PROSPECTIVE INVESTOR IS URGED TO CONSULT ITS OWN TAX ADVISOR ABOUT THE TAX CONSEQUENCES TO IT OF AN INVESTMENT IN ADSS IN LIGHT OF THE INVESTOR'S OWN CIRCUMSTANCES.

The following is a summary of certain material Danish tax considerations relating to the ownership and disposition of ADSs. The summary is for general information purposes only and does not constitute exhaustive tax or legal advice.

It is noted specifically that the summary does not address all possible tax consequences relating to the ownership and disposition of ADSs. The summary does accordingly not apply to investors to whom special tax rules apply, and, therefore, may not be relevant, for example, to investors subject to the Danish Tax on Pension Yields Act (i.e., pension savings), professional investors, certain institutional investors, insurance companies, pension companies, banks, stockbrokers and investors with tax liability on return on pension investments. The summary does further not apply to non-Danish tax resident investors that carry on business activities in Denmark through a permanent establishment.

In the context of the following section, "companies" mean entities that are treated as separate taxable entities under Danish domestic tax laws.

The summary is based solely on the tax laws of Denmark in effect on the date of this prospectus. Danish tax laws may be subject to change, potentially with retroactive effect.

Potential investors in the ADSs are advised to consult their tax advisors regarding the applicable tax consequences of ownership and disposition of the ADSs based on their particular circumstances.

It is currently not clear under Danish tax legislation or case law how ADSs are to be treated for Danish tax purposes.

This summary assumes that the ADS holder in respect of the ADSs is treated as the direct owner of the shares underlying the ADSs and accordingly as the shareholder for Danish domestic tax law purposes, and that the ADS holder is deemed the beneficial owner of any dividend distributed on the underlying shares for Danish domestic tax law purposes as well as any under any applicable tax treaty.

Therefore, the following deals with certain material Danish tax considerations relating to the ownership and disposition of shares.

Gains from the sale of shares realized by Danish tax resident individuals are taxed as share income at a rate of 27% on the first DKK 50,600 ($7,598) (for cohabiting spouses, a total of DKK 101,200 ($15,195)) and at a rate of 42% on share income exceeding DKK 50,600 ($7,598) (for cohabiting spouses over DKK 101,200 ($15,195)) in 2016. The thresholds are subject to annual adjustments and include all share income included in the calculation (i.e., all capital gains and dividends derived by the individual or cohabiting spouses, respectively).

Gains and losses on the sale of shares are calculated as the difference between the purchase price and the sales price. The purchase price is based on the average purchase price paid for the shares in the company (i.e., not the purchase price paid for each share).

Losses on the sale of listed shares can only be offset against other share income deriving from listed shares (i.e., dividends and capital gains on the sale of listed shares). Unused losses will automatically be offset against a cohabiting spouse's share income deriving from listed shares and any additional losses can be carried forward and offset against future share income deriving from listed shares.

Dividends paid to Danish tax resident individuals are included in the individual's share income and taxed as such, as outlined above. Dividends paid to Danish tax resident individuals are generally subject to withholding tax at the rate of 27%.

Non-Danish tax resident individuals, including individuals tax resident in the United States, are generally not taxed in Denmark on gains realized on the sale of sales.

Dividends paid to non-Danish tax resident individuals, including individuals tax resident in the United States, are generally subject to withholding tax at the rate of 27%. No additional tax will be imposed.

In the event that the shareholder is tax resident in a state with which Denmark has entered into a tax treaty and is entitled to benefits under such tax treaty, the shareholder may seek a refund from the Danish Tax Administration of the tax withheld in excess of the applicable treaty rate (Danish tax treaties typically provide for a 15% tax rate). Denmark has entered into tax treaties with approximately 80 countries, including the United States and almost all EU member states. The treaty between Denmark and the United States generally provides for a 15% tax rate.

Similarly, Danish domestic tax law provides for a 15% tax rate, if the shareholder holds less than 10% of the share capital in the company and is tax resident in a state that is obligated to exchange information with Denmark under a tax treaty or an international agreement, convention or other administrative agreement on assistance in tax matters. If the shareholder is tax resident outside the EU, it is an additional requirement for application of the 15% tax rate that the shareholder together with related shareholders holds less than 10% of the share capital of the company.

Any reduced tax rate according to an applicable tax treaty and/or Danish domestic tax law will not affect the withholding rate (27%). In order to receive a refund (from 27% to e.g. 15%), the shareholder must make a claim for such refund through certain certification procedures.

As a general rule, the refund shall be paid within six months following the Danish Tax Administration's receipt of the refund claim. If the refund is paid later than six months after the receipt of the claim, interest will be calculated on the amount of refund. For 2016 and subsequent years, the rate per month will be 0.4% plus a premium fixed annually. The six-month deadline can be suspended by the Danish Tax Administration, if the Tax Administration is unable to determine whether the taxpayer is entitled to a refund based on the taxpayer's affairs. If the deadline is suspended accordingly, computation of interest is also suspended.

On August 25, 2015, the Danish Tax Administration announced that payment of refunds has been temporarily put on hold pending investigations on potential fraudulent refund claims. The Tax

Administration has further announced that payment of refunds will be resumed as soon as possible. The six-month deadline applies irrespective of this announcement, but the deadline can be suspended as described above.

The Danish Tax Administration is currently working on the implementation of a new procedure for processing refund claims. The Tax Administration has announced that it expects that this new procedure will be in place in the first quarter of 2016 and, following the implementation of this new procedure, that refunds in general will be payable within the six-month deadline.

For the purpose of taxation of sales of shares made by corporate shareholders (and dividends received by corporate shareholders, see below), a distinction is made between:

"Subsidiary Shares," which are generally defined as shares owned by a shareholder holding at least 10% of the share capital of the issuing company;

"Group Shares," which are generally defined as shares in a company in which the shareholder of the company and the issuing company are subject to Danish joint taxation or satisfy the requirements for international joint taxation under Danish law;

"Tax-Exempt Portfolio Shares," which are generally defined as unlisted shares owned by a shareholder holding less than 10% of the share capital of the issuing company; and

"Taxable Portfolio Shares," which are defined as shares that do not qualify as Subsidiary Shares, Group Shares or Tax-Exempt Portfolio Shares.

Gains and losses on disposal of Subsidiary Shares and Group Shares and Tax-Exempt Portfolio Shares realized by Danish tax resident companies are generally not included in the taxable income of the shareholder, subject to certain anti-avoidance rules.

Capital gains from the sale of Taxable Portfolio Shares are taxable at the general corporate tax rate of 22% and losses on such shares are generally deductible. Gains and losses on listed Taxable Portfolio Shares are taxed under the mark-to-market principle (i.e., each year's taxable gain or loss is calculated as the difference between the market value of the shares at the beginning and end of the tax year).

Dividends received on Subsidiary Shares and Group Shares are generally tax-exempt, subject to certain anti-avoidance rules.

Dividends received on Taxable Portfolio Shares are taxable at the general corporate tax rate of 22% and tax is generally withheld similarly at 22%.

Non-Danish tax resident companies, including companies tax resident in the United States, are generally not taxed in Denmark on gains realized on the sale of sales, subject to certain anti-avoidance rules.

Dividends received on Subsidiary Shares are exempt from Danish withholding tax provided that taxation shall be waived or reduced under the Parent-Subsidiary Directive (2011/96/EEC) or under an applicable tax treaty. Similarly, dividends received on Group Shares, which are not Subsidiary Shares, are exempt from Danish withholding tax if the shareholder is resident in the EU or the EEA and provided that taxation shall be waived or reduced under the Parent-Subsidiary Directive (2011/96/EEC) or under an applicable tax treaty had the shares been Subsidiary Shares.

In other cases, including in respect of dividends received on Tax-Exempt and Taxable Portfolio Shares, dividends will generally be subject to withholding tax at a rate of 27%. No additional tax will be imposed. The government has recently published a draft legislative proposal pursuant to which the dividend tax rate will be reduced to 22%, but this reduction will not affect the withholding rate that will remain 27%. If the proposal is passed unchanged, all foreign corporate shareholders receiving taxable dividends from Danish companies will thus be able to ask for a refund—pursuant to the procedures described below—of at least 5% of the total dividend.

Further, in the event that the shareholder is tax resident in a state with which Denmark has entered into a tax treaty and is entitled to the benefits under such tax treaty, the shareholder may seek a refund from the Danish Tax Administration of the tax withheld in excess of the applicable treaty rate (Danish tax treaties typically provide for a 15% tax rate). Denmark has entered into tax treaties with approximately 80 countries, including the United States and almost all EU member states. The treaty between Denmark and the United States generally provides for a 15% tax rate.

Similarly, Danish domestic tax law provides for an applicable 15% tax rate, if the shareholder holds less than 10% of the share capital in the company and is tax resident in a state that is obligated to exchange information with Denmark under a tax treaty or an international agreement, convention or other administrative agreement on assistance in tax matters. If the shareholder is tax resident outside the EU, it is an additional requirement for eligibility for the 15% tax rate that the shareholder together with related shareholders holds less than 10% of the nominal share capital of the company.

Any reduced tax rate according to an applicable tax treaty (and/or the 15% tax rate provided for under Danish domestic tax law) will not affect the withholding rate (27%). In order to receive a refund (from 27% to e.g. 15%), the shareholder must make a claim for such refund through certain certification procedures.

On August 25, 2015, the Danish Tax Administration announced that payment of refunds has been temporarily put on hold pending investigations on potential fraudulent refund claims. The Tax Administration has further announced that payment of refunds will be resumed as soon as possible. The six-month deadline applies irrespective of this announcement, but the deadline can be suspended as described above.

We and the underwriters for this offering named below have entered into an underwriting agreement with respect to the ADSs being offered. Subject to the terms and conditions of the underwriting agreement, each underwriter has severally agreed to purchase from us the number of ADSs set forth opposite its name below. Cowen and Company, LLC and Piper Jaffray & Co. are the representatives of the underwriters.

The underwriting agreement provides that the obligations of the underwriters are subject to certain standard conditions precedent (including approval of legal matters by their counsel) and that the underwriters have agreed, severally and not jointly, to purchase all of the ADSs sold under the underwriting agreement if any of these ADSs are purchased, other than those ADSs covered by the overallotment option described below. If an underwriter defaults, the underwriting agreement provides that the purchase commitments of the non-defaulting underwriters may be increased, additional underwriters may be added to fulfill the purchase commitment of the defaulting underwriter or the underwriting agreement may be terminated.

We have agreed to indemnify the underwriters against specified liabilities, including liabilities under the Securities Act and to contribute to payments the underwriters may be required to make in respect thereof.

The underwriters are offering the ADSs, subject to prior sale, when, as and if issued to and accepted by them. The underwriters reserve the right to withdraw, cancel or modify offers to the public and to reject orders in whole or in part.

The address of Cowen and Company, LLC is 599 Lexington Avenue, New York, NY 10022, and the address of Piper Jaffray & Co. is 800 Nicollet Mall, Suite 1000, Minneapolis, MN 55402.

We have granted to the underwriters an option to purchase up to additional ADSs at the same price per ADS paid for the ADSs offered hereby, less the underwriting commission. This option is exercisable for a period of 30 days. The underwriters may exercise this option solely for the purpose of covering overallotments, if any, made in connection with the sale of ADSs offered hereby. To the extent that the underwriters exercise this option, the underwriters will purchase additional ADSs from us in approximately the same proportion as shown in the table following the first paragraph of this section.

The following table shows the public offering price, underwriting commission and proceeds, before expenses, to us. These amounts are shown assuming both no exercise and full exercise of the underwriters' option to purchase additional ADSs.

We estimate that our total expenses of this offering, excluding the underwriting commission, will be approximately $ million and have been paid or are payable by us. We have also agreed to reimburse the underwriters for certain of their expenses, in an amount of up to $35,000, that may be incurred in connection with the review by the Financial Industry Regulatory Authority, Inc., or FINRA, of the terms of the ADSs offered hereby, as set forth in the underwriting agreement.

The underwriters propose to offer the ADSs to the public at the public offering price set forth on the cover of this prospectus. The underwriters may offer the ADSs to securities dealers at the public offering price less a concession fee not in excess of $ per ADS. If all of the ADSs are not sold at the public offering price, the underwriters may change the offering price and other selling terms. Certain of the underwriters may sell shares to the public, both in and outside of the United States, through one or more of their affiliates as selling agents.

The underwriters do not intend to confirm sales of the ADSs to any accounts over which they have discretionary authority.

Prior to this offering, neither our shares nor our ADSs have been listed for trading on an exchange in the United States. However, our shares are listed on the Nasdaq Copenhagen exchange under the symbol "BAVA," and we have a sponsored Level 1 American Depositary Receipt program in the United States, through which our Level 1 American Depositary Shares, or the Level 1 ADSs, are traded on the U.S. over-the-counter market under the ticker symbol "BVNRY." The public offering price will be determined by negotiations between us and the representatives of the underwriters. In addition to prevailing market conditions, the factors to be considered in these negotiations include:

We have applied to list our ADSs on The NASDAQ Global Select Market under the symbol "BAVN."

An active trading market for the ADSs may not develop on The NASDAQ Global Select Market, or if such a market develops, may not be sustained. It is also possible that, after this offering, the ADSs will not trade in the public market at or above the public offering price.

In connection with this offering, the underwriters may engage in stabilizing transactions, overallotment transactions, syndicate covering transactions, penalty bids and purchases to cover positions created by short sales, for up to 30 days from the date of this prospectus. Cowen and Company, LLC or its agents shall act as the stabilizing manager.

These stabilizing transactions, syndicate covering transactions and penalty bids may have the effect of raising or maintaining the market price of our ADSs or preventing or retarding a decline in the market price of our ADSs. As a result, the price of our ADSs in the open market may be higher than it would otherwise be in the absence of these transactions. Neither we nor the underwriters make any representation or prediction as to the effect that the transactions described above may have on the price of ADSs. These transactions may be effected on The NASDAQ Global Select Market, in the over-the-counter market or otherwise and, if commenced, may be discontinued at any time.

In order to be exempt from the prohibition against naked short positions under EU Regulation 236/2012 on short selling and certain aspects of credit default swaps, short positions must be carried out as part of stabilization transactions in compliance with Chapter III of EU Regulation No. 2273/2003 on exemptions for buy-back programs and stabilization of financial instruments.

Pursuant to certain "lock-up" agreements, we and our executive officers and directors, or the Locked-Up Parties, have agreed, subject to certain exceptions, not to offer, sell, contract to sell, assign, transfer, pledge, or otherwise dispose of, or announce the intention to otherwise dispose of, or enter into any swap, hedge or similar agreement or arrangement that transfers, in whole or in part, the economic risk of ownership of, directly or indirectly, or make any demand or request for or exercise any right with respect to the registration of, or engage in any short selling of, or file with the SEC a registration statement under the Securities Act relating to any of our shares, our ADSs or our Level 1 ADSs, or securities convertible into or exchangeable or exercisable for any of our shares, our ADSs or our Level 1 ADSs, without the prior written consent of both of the representatives of the underwriters, for a period of 90 days after the date of this prospectus.

This lock-up provision applies to our shares, our ADSs and our Level 1 ADSs and to securities convertible into or exchangeable or exercisable for such securities together, the Locked-Up Securities. The exceptions to the lock-up for the Locked-Up Parties include: (a) transfers made as a bona fide gift to any member of the immediate family of the Locked-Up Party or to a trust, the beneficiaries of which are exclusively the Locked-Up Party or members of the Locked-Up Party's immediate family; (b) transfers made by will or intestate succession upon the death of the Locked-Up Party; (c) transfers made as a bona fide gift to a charity or educational institution; (d) if the Locked-Up Party is a corporation, partnership, limited liability company or other business entity, any transfers to any stockholder, partner or member of, or owner of a similar equity interest in, the Locked-Up Party, as the case may be, if, in any such case, such transfer is not for value; (e) if the Locked-Up Party is a corporation, partnership, limited liability company or other business entity, any transfer made by the Locked-Up Party (i) in connection with the sale or other bona fide transfer in a single transaction of all or substantially all of the Locked-Up Party's capital stock, partnership interests, membership interests or other similar equity interests, as the case may be, or all or substantially all of the Locked-Up Party's assets, in any such case not undertaken for the purpose of avoiding the restrictions imposed by this Agreement, or (ii) to another corporation, partnership, limited liability company or other business entity so long as the transferee is an affiliate of the Locked-Up Party and such transfer is not for value; (f) any transactions by the Locked-Up Party related to Locked-Up Securities which were acquired in an open market transaction; (g) the establishment of a trading plan pursuant to Rule 10b5-1 under the Exchange Act for the transfer of Locked-Up Securities, provided that such plan does not provide for the transfer of Locked-Up Securities during the Lock-Up Period; (h) transfers by operation of law or by order of a court of competent jurisdiction, such as pursuant to a qualified domestic order or in connection with a divorce settlement; (i) transfers to us (A) upon a vesting event of our securities for full or partial payment of taxes or tax withholding obligations required to be paid in connection with such vesting, (B) in full or partial payment of the exercise price for warrants, or (C) for full or partial payment of taxes or tax withholding obligations required to be paid upon the exercise of warrants; (j) transfers of Locked-Up Securities to us in connection with the cashless exercise of warrants; and (k) sales of Locked-Up Securities in the open market as are necessary to cover any individual tax obligations resulting from the exercise of warrants by the Locked-Up Party. The exceptions to the lock-up for us are (i) our sale of ADSs in this offering and (ii) the issuance of Locked-Up Securities pursuant to the conversion or exercise of existing securities.

The representatives may, in their sole discretion and at any time or from time to time before the termination of the lock-up period, release all or any portion of the securities subject to lock-up agreements; provided, however, that, subject to limited exceptions, at least three business days before the release or waiver or any lock-up agreement with one of our officers or directors, the representatives must notify us of the impending release or waiver and we will announce the

impending release or waiver through a major news service at least two business days before the effective date of the release or waiver.

A prospectus in electronic format may be made available on the websites maintained by one or more of the underwriters or selling group members, if any, participating in this offering and one or more of the underwriters participating in this offering may distribute prospectuses electronically. The representatives may agree to allocate a number of ADSs to underwriters and selling group members for sale to their online brokerage account holders. Internet distributions will be allocated by the underwriters and selling group members that will make Internet distributions on the same basis as other allocations. Other than the prospectus in electronic format, the information on these websites is not part of this prospectus or the registration statement of which this prospectus forms a part, has not been approved or endorsed by us or any underwriter in its capacity as underwriter, and should not be relied upon by investors.

Certain of the underwriters and their affiliates have provided, and may in the future provide, various investment banking, commercial banking and other financial services for us and our affiliates for which they have received, and may in the future receive, customary fees.

In addition, in the ordinary course of their business activities, the underwriters and their affiliates may make or hold a broad array of investments and actively trade debt and equity securities (or related derivative securities) and financial instruments (including bank loans) for their own account and for the accounts of their customers. Such investments and securities activities may involve securities and/or instruments of ours or our affiliates. The underwriters and their affiliates may also make investment recommendations and/or publish or express independent research views in respect of such securities or financial instruments and may hold, or recommend to clients that they acquire, long and/or short positions in such securities and instruments.

No action has been taken in any jurisdiction except the United States that would permit a public offering of our ADSs, or the possession, circulation or distribution of this prospectus or any other material relating to us or our ADSs in any jurisdiction where action for that purpose is required. Accordingly, the ADSs may not be offered or sold, directly or indirectly, and neither this prospectus nor any other offering material or advertisements in connection with the ADSs may be distributed or published, in or from Denmark or any other country or jurisdiction except in compliance with any applicable rules and regulations of any such country or jurisdiction.

The securities may be sold in Canada only to purchasers purchasing, or deemed to be purchasing, as principal that are accredited investors, as defined in National Instrument 45-106 Prospectus Exemptions or subsection 73.3(1) of the Securities Act (Ontario), and are permitted clients, as defined in National Instrument 31-103 Registration Requirements, Exemptions and Ongoing Registrant Obligations. Any resale of the securities must be made in accordance with an exemption from, or in a transaction not subject to, the prospectus requirements of applicable securities laws.

Securities legislation in certain provinces or territories of Canada may provide a purchaser with remedies for rescission or damages if this prospectus (including any amendment thereto) contains a misrepresentation, provided that the remedies for rescission or damages are exercised by the

purchaser within the time limit prescribed by the securities legislation of the purchaser's province or territory. The purchaser should refer to any applicable provisions of the securities legislation of the purchaser's province or territory for particulars of these rights or consult with a legal advisor.

Pursuant to section 3A.3 of National Instrument 33-105 Underwriting Conflicts (NI 33-105), the underwriters are not required to comply with the disclosure requirements of NI 33-105 regarding underwriter conflicts of interest in connection with this offering.

In relation to each Member State of the EEA which has implemented the Prospectus Directive (each, a Relevant Member State), with effect from and including the date on which the Prospectus Directive is implemented in that Relevant Member State no offer of shares which are the subject of the offering contemplated by this prospectus may be made to the public in that Relevant Member State other than:

provided that no such offer of shares shall result in a requirement for us or any underwriter to publish a prospectus pursuant to Article 3 of the Prospectus Directive or a supplemental prospectus pursuant to Article 16 of the Prospectus Directive.

Each person in a Relevant Member State who initially acquires any ADSs or to whom any offer is made will be deemed to have represented, acknowledged and agreed that it is a "qualified investor" within the meaning of the law in that Relevant Member State implementing Article 2(1)(e) of the Prospectus Directive. In the case of any ADSs being offered to a financial intermediary as that term is used in Article 3(2) of the Prospectus Directive, each such financial intermediary will be deemed to have represented, acknowledged and agreed that the ADSs acquired by it in the offer have not been acquired on a non-discretionary basis on behalf of, nor have they been acquired with a view to their offer or resale to, persons in circumstances that may give rise to an offer of any ADSs to the public other than their offer or resale in a Relevant Member State to qualified investors as so defined or in circumstances in which the prior consent of the representatives has been obtained to each such proposed offer or resale.

The Company, the representatives and their affiliates will rely upon the truth and accuracy of the foregoing representations, acknowledgements and agreements.

This prospectus has been prepared on the basis that any offer of ADSs in any Relevant Member State will be made pursuant to an exemption under the Prospectus Directive from the requirement to publish a prospectus for offers of ADSs. Accordingly any person making or intending to make an offer in that Relevant Member State of ADSs that are the subject of this offering contemplated in this prospectus may only do so in circumstances in which no obligation arises for the Company or any of the underwriters to publish a prospectus pursuant to Article 3 of the Prospectus Directive in relation to such offer. Neither the Company nor the underwriters have authorized, nor do they authorize, the making of any offer of ADSs in circumstances in which an obligation arises for the Company or the underwriters to publish a prospectus for such offer.

For the purpose of the above provisions, the expression "an offer to the public" in relation to any ADSs in any Relevant Member State means the communication in any form and by any means of sufficient information on the terms of the offer and the ADSs to be offered so as to enable an investor to decide to purchase or subscribe the ADSs, as the same may be varied in the Relevant Member State by any measure implementing the Prospectus Directive in the Relevant Member State and the expression "Prospectus Directive" means Directive 2003/71/EC (including the 2010 PD Amending Directive, to the extent implemented in the Relevant Member States) and includes any relevant implementing measure in the Relevant Member State and the expression "2010 PD Amending Directive" means Directive 2010/73/EU.

In addition, in the United Kingdom, this document is being distributed only to, and is directed only at, and any offer subsequently made may only be directed at persons who are "qualified investors" (as defined in the Prospectus Directive) (1) who have professional experience in matters relating to investments falling within Article 19 (5) of the Financial Services and Markets Act 2000 (Financial Promotion) Order 2005, as amended, or the Order, and/or (2) who are high net worth companies (or persons to whom it may otherwise be lawfully communicated) falling within Article 49(2)(a) to (d) of the Order (all such persons together being referred to as "relevant persons"). This document must not be acted on or relied on in the United Kingdom by persons who are not relevant persons. In the United Kingdom, any investment or investment activity to which this document relates is only available to, and will be engaged in with, relevant persons.

The ADSs may not be publicly offered in Switzerland and will not be listed on the SIX Swiss Exchange, or the SIX, or on any other stock exchange or regulated trading facility in Switzerland. This document has been prepared without regard to the disclosure standards for issuance prospectuses under art. 652a or art. 1156 of the Swiss Code of Obligations or the disclosure standards for listing prospectuses under art. 27 ff. of the SIX Listing Rules or the listing rules of any other stock exchange or regulated trading facility in Switzerland. Neither this document nor any other offering or marketing material relating to the ADSs or this offering may be publicly distributed or otherwise made publicly available in Switzerland.

Neither this document nor any other offering or marketing material relating to this offering, the Company, the ADSs have been or will be filed with or approved by any Swiss regulatory authority. In particular, this document will not be filed with, and the offer of ADSs will not be supervised by, the Swiss Financial Market Supervisory Authority FINMA, and the offer of ADSs has not been and will not be authorized under the Swiss Federal Act on Collective Investment Schemes, or CISA. The investor protection afforded to acquirers of interests in collective investment schemes under the CISA does not extend to acquirers of ADSs.

Notice to Prospective Investors in the Dubai International Financial Centre

This prospectus relates to an Exempt Offer in accordance with the Offered Securities Rules of the Dubai Financial Services Authority, or DFSA. This prospectus is intended for distribution only to persons of a type specified in the Offered Securities Rules of the DFSA. It must not be delivered to, or relied on by, any other person. The DFSA has no responsibility for reviewing or verifying any documents in connection with Exempt Offers. The DFSA has not approved this prospectus nor taken steps to verify the information set forth herein and has no responsibility for the prospectus. The ADSs to which this prospectus relates may be illiquid and/or subject to restrictions on their resale. Prospective purchasers of the ADSs offered should conduct their own due diligence on the ADSs. If

you do not understand the contents of this prospectus you should consult an authorized financial advisor.

No placement document, prospectus, product disclosure statement or other disclosure document has been lodged with the Australian Securities and Investments Commission, in relation to this offering. This prospectus does not constitute a prospectus, product disclosure statement or other disclosure document under the Corporations Act 2001, or the Corporations Act, and does not purport to include the information required for a prospectus, product disclosure statement or other disclosure document under the Corporations Act.

Any offer in Australia of the ADSs may only be made to persons, or the Exempt Investors, who are "sophisticated investors" (within the meaning of section 708(8) of the Corporations Act), "professional investors" (within the meaning of section 708(11) of the Corporations Act) or otherwise pursuant to one or more exemptions contained in section 708 of the Corporations Act so that it is lawful to offer the ADSs without disclosure to investors under Chapter 6D of the Corporations Act.

The ADSs applied for by Exempt Investors in Australia must not be offered for sale in Australia in the period of 12 months after the date of allotment under this offering, except in circumstances where disclosure to investors under Chapter 6D of the Corporations Act would not be required pursuant to an exemption under section 708 of the Corporations Act or otherwise or where the offer is pursuant to a disclosure document which complies with Chapter 6D of the Corporations Act. Any person acquiring ADSs must observe such Australian on-sale restrictions.

This prospectus contains general information only and does not take account of the investment objectives, financial situation or particular needs of any particular person. It does not contain any securities recommendations or financial product advice. Before making an investment decision, investors need to consider whether the information in this prospectus is appropriate to their needs, objectives and circumstances, and, if necessary, seek expert advice on those matters.

The ADSs have not been offered or sold and will not be offered or sold in Hong Kong, by means of any document, other than (a) to "professional investors" as defined in the Securities and Futures Ordinance (Cap. 571) of Hong Kong and any rules made under that Ordinance; or (b) in other circumstances that do not result in the document being a "prospectus" as defined in the Companies Ordinance (Cap. 32) of Hong Kong or that do not constitute an offer to the public within the meaning of that Ordinance. No advertisement, invitation or document relating to the ADSs has been or may be issued or has been or may be in the possession of any person for the purposes of issue, whether in Hong Kong or elsewhere, which is directed at, or the contents of which are likely to be accessed or read by, the public of Hong Kong (except if permitted to do so under the securities laws of Hong Kong) other than with respect to ADSs, which are or are intended to be disposed of only to persons outside Hong Kong or only to "professional investors" as defined in the Securities and Futures Ordinance and any rules made under that Ordinance.

The ADSs have not been and will not be registered under the Financial Instruments and Exchange Law of Japan (Law No. 25 of 1948, as amended) and, accordingly, will not be offered or sold, directly or indirectly, in Japan, or for the benefit of any Japanese Person or to others for re-offering or resale, directly or indirectly, in Japan or to any Japanese Person, except in compliance with all applicable laws, regulations and ministerial guidelines promulgated by relevant Japanese

governmental or regulatory authorities in effect at the relevant time. For the purposes of this paragraph, "Japanese Person" shall mean any person resident in Japan, including any corporation or other entity organized under the laws of Japan.

This prospectus has not been registered as a prospectus with the Monetary Authority of Singapore. Accordingly, this prospectus and any other document or material in connection with the offer or sale, or invitation for subscription or purchase, of ADSs may not be circulated or distributed, nor may the ADSs be offered or sold, or be made the subject of an invitation for subscription or purchase, whether directly or indirectly, to persons in Singapore other than (i) to an institutional investor under Section 274 of the Securities and Futures Act, Chapter 289 of Singapore, or the SFA, (ii) to a relevant person pursuant to Section 275(1), or any person pursuant to Section 275(1A), and in accordance with the conditions specified in Section 275, of the SFA, or (iii) otherwise pursuant to, and in accordance with the conditions of, any other applicable provision of the SFA.

Where the ADSs are subscribed or purchased under Section 275 of the SFA by a relevant person who is:

securities (as defined in Section 239(1) of the SFA) of that corporation or the beneficiaries' rights and interest (howsoever described) in that trust shall not be transferred within six months after that corporation or that trust has acquired the ADSs pursuant to an offer made under Section 275 of the SFA except:

The following table sets forth the costs and expenses, other than the underwriting commission, payable by us in connection with the sale of the ADSs being registered. All amounts are estimates except for the SEC registration fee, the FINRA filing fee and The NASDAQ Global Select Market listing fee.

The validity of the issuance of the shares underlying the ADSs offered in this prospectus and certain other matters of Danish law will be passed upon for us by Kromann Reumert, Copenhagen, Denmark. Certain matters of U.S. law will be passed upon for us by Cooley LLP, New York, New York. Mintz, Levin, Cohn, Ferris, Glovsky and Popeo, P.C., Boston, Massachusetts, and Plesner, Copenhagen, Denmark are acting as counsel for the underwriters in connection with this offering.

The consolidated financial statements as of December 31, 2014 and 2013, and for each of the two years ended December 31, 2014 and 2013 included in this Registration Statement, have been audited by Deloitte Statsautoriseret Revisionspartnerselskab, an independent registered public accounting firm, as stated in their report appearing herein. Such financial statements of the Company have been included in reliance upon the report of such firm given upon their authority as experts in accounting and auditing. The offices of Deloitte Statsautoriseret Revisionspartnerselskab are located at Weidekampsgade 6, 2300 Copenhagen, Denmark.

We are organized under the laws of Denmark, with domicile in the municipality of Helsingør, Denmark.

All of the members of the board of directors and the executive board named herein are residents of Denmark or other jurisdictions outside the United States. A substantial portion of ours and such persons' assets are located in Denmark or other jurisdictions outside the United States. As a result, it may not be possible for investors to effect service of process upon such persons or us with respect to litigation that may arise under U.S. law or to enforce against them or our company judgments obtained in U.S. courts, whether or not such judgments were made pursuant to civil liability provisions of the federal or state securities laws of the United States or any other laws of the United States.

We have been advised by our Danish legal advisors, Kromann Reumert, that there is not currently a treaty between the United States and Denmark providing for reciprocal recognition and enforceability of judgments rendered in connection with civil and commercial disputes and, accordingly, that a final judgment rendered by a U.S. court based on civil liability would not be enforceable in Denmark. It is uncertain whether Danish courts would allow actions to be predicated on the securities laws of the United States or other jurisdictions outside Denmark. Danish courts are likely to deny claims for punitive damages and may grant a reduced amount of damages compared to U.S. courts.

This prospectus, which constitutes a part of the registration statement, does not contain all of the information set forth in the registration statement or the exhibits and schedules filed therewith. For further information with respect to Bavarian Nordic A/S and the ADSs offered hereby, reference is made to the registration statement and the exhibits and schedules filed therewith. Statements contained in this prospectus regarding the contents of any contract or any other document that is filed as an exhibit to the registration statement are not necessarily complete, and each such statement is qualified in all respects by reference to the full text of such contract or other document filed as an exhibit to the registration statement. A copy of the registration statement and the exhibits and schedules filed therewith may be inspected without charge at the public reference room maintained by the SEC, located at 100 F Street N.E., Room 1580, Washington, D.C. 20549, and copies of all or any part of the registration statement may be obtained from such offices upon the payment of the fees prescribed by the SEC. Please call the SEC at 1-800-SEC-0330 for further information about the public reference room. The SEC also maintains a website that contains reports, proxy and information statements and other information regarding registrants that file electronically with the SEC. The address is www.sec.gov. We currently make available to the public our annual and interim reports, as well as certain information regarding our corporate governance and other matters, on the Investors Relations page of our website, www.bavarian-nordic.com.

After this offering, we will be subject to the reporting requirements of the Exchange Act applicable to foreign private issuers. Because we are a foreign private issuer, the SEC's rules do not require us to deliver proxy statements or to file quarterly reports on Form 10-Q, among other things. However, we plan to produce quarterly financial reports and furnish them to the SEC after the end of each of the first three quarters of our fiscal year and to file our annual report on Form 20-F within four months after the end of our fiscal year. In addition, our "insiders" are not subject to the SEC's rules that prohibit short-swing trading. Our annual consolidated financial statements will be prepared

in accordance with International Financial Reporting Standards, or IFRS, as issued by the International Accounting Standards Board, or IASB, and certified by an independent public accounting firm.

We will send the depositary a copy of all notices of shareholders meetings and other reports, communications and information that are made generally available to shareholders. The depositary has agreed to mail to all holders of ADSs a notice containing the information (or a summary of the information) contained in any notice of a meeting of our shareholders received by the depositary and will make available to all holders of ADSs such notices and all such other reports and communications received by the depositary.


		Page
Report of Independent Registered Public Accounting Firm		F-2
Consolidated Income Statements for the Years Ended December 31, 2014 and 2013		F-3
Consolidated Statements of Comprehensive Income for the Years Ended December 31, 2014 and 2013		F-4
Consolidated Statements of Cash Flow for the Years Ended December 31, 2014 and 2013		F-5
Consolidated Statements of Financial Position—Assets as of December 31, 2014 and 2013		F-6
Consolidated Statements of Financial Position—Equity and Liabilities as of December 31, 2014 and 2013		F-7
Consolidated Statements of Changes in Equity at December 31, 2014 and 2013		F-8
Notes to the Consolidated Financial Statements		F-10
Unaudited Condensed Consolidated Income Statements for the Periods Ended September 30, 2015 and 2014		F-51
Unaudited Condensed Consolidated Statements of Comprehensive Income for the Periods Ended September 30, 2015 and 2014		F-52
Unaudited Condensed Consolidated Statements of Financial Position—Assets as of September 30, 2015 and December 31, 2014		F-53
Unaudited Condensed Consolidated Statements of Financial Position—Equity and Liabilities as of September 30, 2015 and December 31, 2014		F-54
Unaudited Condensed Consolidated Statements of Cash Flow for the Periods Ended September 30, 2015 and 2014		F-55
Unaudited Condensed Consolidated Statements of Changes in Equity for the Periods Ended September 30, 2015 and 2014		F-56
Notes to the Unaudited Condensed Consolidated Interim Financial Statements		F-57

To the Board of Directors and Shareholders of Bavarian Nordic A/S, Kvistgaard, Denmark

We have audited the accompanying consolidated statement of financial position of Bavarian Nordic A/S and subsidiaries (the "Company") as of December 31, 2014 and 2013 and the consolidated statement of income, comprehensive income, changes in shareholders' equity, and cash flows for the years ended December 31, 2014 and 2013. These financial statements are the responsibility of the Company's management. Our responsibility is to express an opinion on the financial statements based on our audit.

We conducted our audit in accordance with the standards of the Public Company Accounting Oversight Board (United States). Those standards require that we plan and perform the audit to obtain reasonable assurance about whether the financial statements are free of material misstatement. The Company is not required to have, nor were we engaged to perform, an audit of its internal control over financial reporting. Our audit included consideration of internal control over financial reporting as a basis for designing audit procedures that are appropriate in the circumstances, but not for the purpose of expressing an opinion on the effectiveness of the Company's internal control over financial reporting. Accordingly, we express no such opinion. An audit also includes examining, on a test basis, evidence supporting the amounts and disclosures in the financial statements, assessing the accounting principles used and significant estimates made by management, as well as evaluating the overall financial statement presentation. We believe that our audit provides a reasonable basis for our opinion.

In our opinion, such consolidated financial statements present fairly, in all material respects, the financial position of Bavarian Nordic A/S and subsidiaries as of December 31, 2014 and 2013, and the results of their operations and cash flows for years ended December 31, 2014 and 2013, in conformity with International Financial Reporting Standards as issued by the International Accounting Standards Board.

Consolidated Income Statements for the Years Ended December 31, 2014 and 2013

Consolidated Statements of Comprehensive Income for the Years Ended
December 31, 2014 and 2013

Consolidated Statements of Cash Flow for the Years Ended December 31, 2014 and 2013

Consolidated Statements of Financial Position—Assets
as of December 31, 2014 and 2013

Consolidated Statements of Financial Position—Equity and Liabilities as of
December 31, 2014 and 2013

The share capital comprises a total of 27,671,247 shares of DKK 10 as of December 31, 2014 (26,094,361 shares). The shares are not divided into share classes, and each share carries one vote.

The share capital comprises a total of 26,094,361 shares of DKK 10 as of December 31, 2013 (26,094,361 shares). The shares are not divided into share classes, and each share carries one vote.

Consolidated Statements of Changes in Equity at December 31, 2014 and 2013 (Continued)

Changing the Articles of Association requires that the resolution passes by at least ²/3 of the votes as well as ²/3 of the voting capital represented.

Bavarian Nordic (the Company or the Group) is a fully integrated biotechnology company developing novel vaccines for the prevention of life-threatening infectious diseases and the treatment of cancer, commercializing developed technology through private and public partnerships, and manufacturing vaccines for its partnerships with governmental institutions and the pharmaceutical industry.

The Company focuses on diseases for which the unmet medical need is high and for which the Company can harness the power of the immune system to induce a response. The Company's live virus vaccine platform has generated one commercial product for smallpox, one Phase 3 immunotherapy candidate for prostate cancer, one Phase 3 candidate for Ebola and several other clinical programs in the areas of infectious disease and oncology.

The Company has a significant 10+ year relationship with the US government and has been awarded contracts in relation to development, manufacturing and sales of the Company's smallpox vaccine, IMVAMUNE. In addition, the Company has also established commercial relationships with Bristol-Myers Squibb, BMS, for the commercialization of PROSTVAC the Company's Phase 3 cancer immunotherapy candidate (since March 2015), and with the Janssen Pharmaceutical Companies of Johnson & Johnson, or Janssen, for the Company's Ebola vaccine candidate and additional infectious disease targets (since October 2014).

The Company owns and operates a fully integrated, highly scalable current Good Manufacturing Practices commercial scale vaccine production facility in Kvistgaard, Denmark, and has built an extensive patent portfolio.

The consolidated financial statements for Bavarian Nordic have been prepared in accordance with the International Financial Reporting Standards (IFRS) as issued by the International Accounting Standard Board (IASB).

The accounting policies are unchanged from last year except for changes due to implementation of new and revised standards that were effective January 1, 2014.

The consolidated financial statements are presented in Danish kroner (DKK), which is the functional currency of the parent company.

The consolidated financial statements are presented on a historical cost basis, apart from derivative financial instruments, securities and liability relating to phantom shares, which are measured at fair value.

The accounting policies have been consistently applied for the financial year and for the comparative figures.

The IASB has issued new standards and revisions to existing standards and new interpretations, which are mandatory for accounting periods commencing on or after January 1, 2014. The implementation of new or revised standards and interpretations that are in force have not changed the accounting policies and thus not affected net profit for the year or the financial position.

At the date of publication of the consolidated financial statements, a number of new and amended standards and interpretations have not yet entered into force.

The following standards are in general expected to change the current accounting regulation most significantly:

IASB has issued IFRS 9 "Financial Instruments" with effective date January 1, 2018 however it has not yet been implemented. IFRS 9 "Financial Instruments" is part of IASB's project to replace IAS 39 "Financial Instruments: Recognition and Measurement", and the new standard will change the classification, presentation and measurement of financial instruments and hedging requirements. Bavarian Nordic is assessing the impact of the standard, but it is not expected to have any material impact on future consolidated financial statements.

IFRS 15 "Revenue from Contracts with Customers" is effective for annual periods beginning on or after 1 January 2018, however it has not yet been implemented. Entities will apply a five-step model to determine when, how and at what amount revenue is to be recognized depending on whether certain criteria are met. Before implementation of the standard, Bavarian Nordic will assess whether IFRS 15 "Revenue from Contracts with Customers" has an impact on current and new significant agreements. The new standard is not expected to have any material impact on future consolidated financial statements.

The accounting policies for specific line items are described in the notes to the consolidated financial statements. Set out below is a description of the accounting policies for the basis of consolidation, foreign currency translation, segment reporting and the cash flow statement.

Income is recognized in the income statement when generated. Assets and liabilities are recognized in the statement of financial position when it is probable that any future economic benefit will flow to or from the Company and the value can be reliably measured. On initial recognition, assets and liabilities are measured at cost. Subsequently, assets and liabilities are measured as

described in the description of the accounting policies in the respective notes to the financial statements.

The consolidated financial statements include Bavarian Nordic A/S and the subsidiaries in which the Group holds more than 50% of the voting rights or otherwise has control.

The consolidated financial statements are prepared on the basis of the financial statements of the parent company and the individual subsidiaries, and these are prepared in accordance with the Group's accounting policies and for the same accounting period.

Intra-group income and expenses together with all intra-group profits, receivables and payables are eliminated on consolidation. In the preparation of the consolidated financial statements, the book value of shares in subsidiaries held by the parent company is set off against the equity of the subsidiaries.

On initial recognition, transactions denominated in currencies other than the Group's functional currency are translated at the exchange rate ruling at the transaction date.

Receivables, payables and other monetary items denominated in foreign currencies that have not been settled at the balance sheet date are translated at the exchange rates at the balance sheet date. Exchange differences between the exchange rate at the date of the transaction and the exchange rate at the date of payment or the balance sheet date, respectively, are recognized in the income statement under financials. Property, plant and equipment and intangible assets, inventories and other non-monetary assets acquired in foreign currency and measured based on historical cost are translated at the exchange rates at the transaction date.

On recognition in the consolidated financial statements of subsidiaries whose financial statements are presented in a functional currency other than Danish kroner (DKK), the income statements are translated at the average exchange rates of the respective months. Balance sheet items are translated at the exchange rates at the balance sheet date.

Exchange differences arising on the translation of foreign subsidiaries' opening balance sheet items to the exchange rates at the balance sheet date and on the translation of the income statements from exchange rates beginning of the month to exchange rates at the balance sheet date are recognized as other comprehensive income.

The Group is focused on growth strategies that through private and public partnerships will develop and commercialize novel vaccines and immunotherapies against infectious diseases and cancer.

The Group decided in March 2015 to abandon the divisional structure and merged the two divisions; "Cancer Immunotherapy" and "Infectious Diseases". Therefore, the Group does no longer prepare segment reporting internally, hence only has one operating segment to report externally.

The internal financial reporting no longer contains separate sections for the two divisions.

Geographic spilt of revenue and revenue from major customers are disclosed in the notes to the consolidated financial statements (note 3).

The cash flow statement is prepared in accordance with the indirect method on the basis of the Group's net profit for the year. The statement shows the Group's cash flows broken down into operating, investing and financing activities, cash and cash equivalents at year end and the impact of the calculated cash flows on the Group's cash and cash equivalents.

Cash flows in foreign currencies are translated into Danish kroner at the exchange rate on the transaction date. In the cash flows from operating activities, net profit for the year is adjusted for non-cash operating items and changes in working capital.

Cash flows from investing activities include cash flows from the purchase and sale of intangible assets, property, plant and equipment, investments and securities.

Cash flows from financing activities include cash flows from the raising and payment of loans and capital increases.

Additionally, cash flows from assets held under finance leases are recognized by way of lease payments made.

In the preparation of the consolidated financial statements, management makes a number of accounting estimates which form the basis for the presentation, recognition and measurement of the Group's assets and liabilities.

The recognition and measurement of assets and liabilities often depends on future events that are somewhat uncertain. In that connection, it is necessary to assume a course of events that reflects management's assessment of the most probable course of events.

In connection with the preparation of the consolidated financial statements, management has made a number of estimates and assumptions concerning carrying amounts. Management has made the following accounting judgments which significantly affect the amounts recognized in the consolidated financial statements:

2 Significant accounting estimates, assumptions and uncertainties (Continued)

Please refer to the specific notes for further description of the significant accounting estimates and assumptions used.

Revenue comprises the fair value of the consideration received or receivable for sales of goods and income derived from development services including sale of delivered development services under the IMVAMUNE/IMVANEX development project. Revenue is measured net of value added tax, duties, etc. collected on behalf of a third party and discounts. The revenue is recognized when it is probable that future economic benefits will flow to the Company and these benefits can be measured reliably and when any significant risks and rewards of ownership of the goods or right to the services are transferred and the Company no longer retains managerial responsibility for, or control of, the goods or services sold.

Agreements with commercial partners generally include non-refundable upfront license and collaboration fees, milestone payments, the receipt of which is dependent upon the achievement of certain clinical, regulatory or commercial milestones, as well as royalties on product sales of licensed products, if and when such product sales occur, and revenue from the supply of products. For these agreements that include multiple elements, total contract consideration is attributed to separately identifiable components on a reliable basis that reasonably reflects the selling prices that might be expected to be achieved in stand-alone transactions provided that each component has value to the partner on a stand-alone basis. The then allocated consideration is recognised as revenue in accordance with the principles described above.

Sales of goods and licences that transfer the rights associated with ownership of an intangible asset are recognized at a point in time when control is transferred. Revenue from development services and licences that do not transfer the right of ownership to an intangible asset are recognized over time in line with the execution and delivery of the work. If multiple components are not separable, they are combined into a single component and recognized over the period where the Company is actively involved in development and deliver significant services to the collaboration partner.

Whether a component of a multiple element contract has value to the partner on a stand-alone basis is based on an assessment of specific facts and circumstances and is associated with judgement. This applies also to the assessment of whether a license transfers rights associated with ownership of an intangible asset. Furthermore, allocation of the total consideration of a contract to separately identifiable components requires considerable estimates and judgement to be made by the Company. At inception and throughout the life of a contract the Company is performing an analysis of the agreement with its partners based on available facts and circumstances at each assessment date such as historical experience and knowledge from the market to the extent

obtainable. This includes also an understanding of the purpose of the deliverables under the contract and the negotiation taken place prior to concluding the contract.

In 2013 the Company received DKK 215 million in payment for development results under the IMVAMUNE/IMVANEX development contract. Of this amount, DKK 173 million related to development results delivered in previous financial years and DKK 42 million were included in IMVAMUNE/IMVANEX sales as the amended performance criteria were fulfilled in 2013.

Biomedical Advanced Research and Development Authority (BARDA), USA, DKK 1,190 million (2013: DKK 1,199 million).

Production costs consist of costs incurred in generating the revenue for the year. Costs for raw materials, consumables, production staff and a proportion of production overheads, including maintenance, depreciation and impairment of tangible assets used in production as well as operation, administration and management of the production facility are recognized as production costs. In addition, the costs related to excess capacity and write-down to net realisable value of goods on stock are recognized.

Production costs include external filling costs of DKK 112 million for 2014 (DKK 180 million).

Other production costs decreased from DKK 51 million in 2013 to DKK (8) million in 2014, which primarily was due to an extraordinary production performance with low level of write-downs during 2014 and reversal of DKK 12 million in write-downs from 2013. The total write-down for 2014 was DKK 0 million (DKK 54 million). The development in write-downs is shown in note 17.

Research and development costs include salaries and costs directly attributable to the Company's research and development projects, less government grants. Furthermore, salaries and costs supporting direct research and development, including costs of patents, rent, leasing and depreciation attributable to laboratories, and external scientific consultancy services, are recognized under research and development costs. No indirect or general overhead costs that are not directly attributable to research and development activities are included in the disclosure of research and development expenses recognized in the income statement.

Contract research costs incurred to achieve revenue are recognized under production costs. Research costs are expensed in the year they occur.

Development costs are generally expensed in the year they occur. In line with industry custom, capitalization of development costs does not begin until it is deemed realistic that the product can be completed and marketed and it is highly likely that a marketing authorization will be received. In addition, there must be sufficient certainty that the future earnings to the Company will cover not only production costs, direct distribution and administrative costs, but also the development costs.

However, the Company has met the criteria for capitalize the development costs attributable to the development of IMVAMUNE/IMVANEX, as the RFP-3 contract with the U.S. Government initially comprised the delivery of 20 million doses and an option to buy additional doses.

The Company has delivered 28 million doses to the U.S. Government for emergency use.

In July 2015, the Company obtained an order to deliver further IMVAMUNE/IMVANEX batches to the U.S. Government.

The product has received regulatory approved in both the EU and Canada. Regulatory approval in the United States is pending completion of the last Phase 3 study. The Company intends to and believes that it has adequate technical, financial and other resources to complete the Phase 3 study and file for FDA approval. Historical sale shows that there is a market for sale of smallpox vaccine and management believes that the Company's smallpox vaccine is likely to generate probable future economic benefits for us. Capitalization of the development costs attributable to this development project began at the date of regulatory approval of the applicable clinical trial.

Capitalized development costs regarding the registration of IMVAMUNE/IMVANEX under the RFP-3 contract with the U.S. Government are expensed (amortized) and recognized in the income statement under research and development costs when the related income on delivery of the development results have been earned and recognized as revenue. When the development has

been completed and IMVAMUNE/IMVANEX has been approved by the FDA, the remaining carrying amount will be amortized in concurrence with the delivery of doses over the expected economic life of the asset.

The costs capitalized at December 31, 2014 were limited to those costs incurred and considered recoverable. The primary reason for the probable recovery of the capitalized costs is the delivery agreement with BARDA, which included the historical delivery of 28 million doses prior to the final regulatory approval by the FDA and as such before the completion of the development project.

Grants that compensate the Group for research and development expenses incurred, which are recognized directly in the income statement, are set off against the costs of research and development at the time when a final and binding right to the grant has been obtained.

Research and development costs include expenses for external clinical research organizations, or CRO's, of DKK 259 million for 2014 (DKK 294 million).

The Group only has defined contribution plans and pays regular fixed contributions to independent pension funds and insurance companies.

In 2014 Group Management included CEO and President of the Company Paul Chaplin (Division President for Infectious Diseases until June 1, 2014), CFO Ole Larsen, Division President for Cancer Immunotherapy James B. Breitmeyer and CEO Anders Hedegaard until June 1, 2014.

As of June 1, 2014 Corporate Management consists of Paul Chaplin and Ole Larsen. Until June 1, 2014 Corporate Management only included Anders Hedegaard.

Provisions for incentive agreements with Paul Chaplin and James B. Breitmeyer are recognized in staff costs, while provisions relating to former Division President for Cancer Immunotherapy Reiner Laus, are recognized in other administrative costs. See note 23 for further details.

Members of the Group Management have contracts of employment containing standard terms for members of the Group Management of Danish listed companies, including the periods of notice that both parties are required to give and competition clauses. If a contract of employment of a member of the Group Management is terminated by the Company without misconduct on the part of such member, the member of the Group Management is entitled to compensation, which, depending on the circumstances, may amount to a maximum of 12-18 months' remuneration. In the event of a change of control the compensation can amount to 24 months' remuneration.

Severance pay in 2013 to former Division President for Cancer Immunotherapy Reiner Laus (DKK 3.5 million) includes share-based payment of DKK 0.8 million.

The losses recognized in 2013 are mainly related to sale of assets from the facility in Berlin.

Interest income is recognized in the income statement at the amounts relating to the financial year. Financial income also includes net positive value adjustments of financial instruments and securities as well as net currency gains.

Net foreign exchange gains are mainly related to the increasing USD rate during 2014.

Net foreign exchange gains include DKK 37.9 million of unrealized gains related to intercompany receivable with Bavarian Nordic, Inc.

Interest expenses are recognized in the income statement at the amounts relating to the financial year. Financial expenses also include net negative value adjustments of financial instruments and securities, net currency losses and adjustment of the net present value of provisions.

Net foreign exchange losses for 2013 include DKK 12.1 million of unrealized losses related to intercompany receivable with Bavarian Nordic, Inc.

Income tax for the year comprises current tax and deferred tax for the year. The part relating to the profit for the year is recognized in the income statement, and the part attributable to items in the comprehensive income is recognized in the comprehensive income statement.

The tax effect of costs that have been recognized directly in equity is recognized in equity under the relevant items.

Current tax payable but not yet paid is recognized in the balance sheet under current liabilities.

Deferred tax is measured using the balance sheet liability method on all temporary differences between accounting values and tax values. Deferred tax liabilities arising from temporary tax differences are recognized in the balance sheet as a liability.

Deferred tax assets arising from temporary deductible differences and tax losses carried forward are recognized when it is probable that they can be realized by offsetting them against taxable temporary differences or future taxable profits. At each balance sheet date, it is assessed whether it is probable that there will be sufficient future taxable income for the deferred tax asset to be utilized.

Deferred income tax is provided on temporary taxable differences arising on investments in subsidiaries, unless the parent company is able to control the timing when the deferred tax is to be realized and it is likely that the deferred tax will not be realized within the foreseeable future.

Deferred tax is calculated at the tax rates applicable on the balance sheet date for the income years in which the tax asset is expected to be utilized.

Management is required to make an estimate in the recognition of deferred tax assets. The assessment is based on latest budgets and forecasts approved by the board of directors that include revenue from existing and expected future contracts for the sale of IMVAMUNE/IMVANEX and development projects. In management's opinion, it is probable that sufficient taxable income will be available against which the unused tax losses can be utilized.

Recognized deferred tax assets relate to temporary differences between valuations for accounting and taxation purposes and tax losses carried forward:

Deferred tax assets arising from temporary deductible differences and tax losses carried forward are recognized to the extent they are expected to be offset against future taxable income.

Recognized tax losses carried forward relate to Bavarian Nordic A/S and the two Danish subsidiaries Aktieselskabet af 1. juni 2011 I and BN Infectious Diseases A/S.

The tax value of non-recognized tax losses carried forward in Bavarian Nordic A/S and the two Danish subsidiaries amounts to DKK 182 million (DKK 182 million).

The tax value of non-recognized tax losses and tax credits carried forward in subsidiary Bavarian Nordic, Inc. amounts to DKK 204.9 million (DKK 158.6 million) of which DKK 30.7 million

(DKK 22.8 million) relates to state tax and DKK 174.2 million (DKK 135.8 million) relates to federal tax.

Bavarian Nordic GmbH and Bavarian Nordic Washington DC, Inc. have no tax losses carried forward.

In the calculation of deferred tax as of December 31, 2014, the Company has taken into account the gradual reduction of the Danish corporation tax rate from 25% in 2013 to 22% in 2016.

Earnings per share is calculated as the profit or loss for the year compared to the weighted average of the issued shares in the financial year. The basis for the calculation of diluted earnings per share is the weighted-average number of ordinary shares in the financial year adjusted for the dilutive effects of warrants.

Outstanding warrants have been included in the calculation of diluted earnings per share for 2014. The outstanding warrants are excluded in the calculation for 2013, as the inclusion of potential shares would improve earnings per share for 2013 as net profit for the year is negative.

Intangible assets are measured at historic cost less accumulated amortization and impairment losses. Development projects that meet the requirements for recognition as assets are measured at direct cost relating to the development projects. Interest expenses on borrowings to finance the production of intangible assets are included in cost if they relate to the period of production. Other borrowing costs are expensed.

Capitalized development costs regarding the registration of IMVAMUNE under the RFP-3 contract with the U.S. Government are expensed (amortized) and recognized in the income statement under research and development costs when the related income on delivery of the development results have been earned and recognized as revenue, which may be before the completion of the development project and obtaining of approval. When the development has been completed and IMVAMUNE/IMVANEX has been approved by the FDA, the remaining carrying amount will be amortized in concurrence with the delivery of doses over the expected economic life of the asset.

Expensing (amortization) of capitalized development costs prior to the completion of the development project is shown as disposals under cost. Amortization made after obtaining approval is shown under accumulated amortization.

Purchased rights or rights acquired in connection with acquisitions which fulfil the requirements for recognition are measured at cost. Amortization is provided on a straight-line basis over the useful economic lives of the assets, max. 15 years.

The carrying amounts of intangible assets carried at cost or amortized cost are tested at least annually to determine whether there are indications of any impairment in excess of that expressed in normal amortization. If that is the case, the asset is written down to the recoverable amount, which is the higher of its fair value less costs to sell and its value in use. Impairment losses on intangible assets are recognized under the same line item as amortization of the assets.

For development projects in progress, the recoverable amount is assessed annually, regardless of whether any indications of impairment have been found.

Management has assessed that development costs relating to the registration of IMVAMUNE/IMVANEX under the RFP-3 contract with the U.S. Government continue to meet the conditions for capitalization.

In 2013, the Company started expensing (amortizing) capitalized development costs under the IMVAMUNE/IMVANEX project, as the Company is receiving payment for the delivered development results as from 2013 and recognizing payments as revenue when received. Management believes that the development results have been delivered at the time when the Company's right to payment has vested, and that the delivered development results represent a separate value to the U.S. Government. The right to payment vests simultaneously with the delivery of the doses. Accordingly, expensing (amortization) of the development costs is commenced before completion of the project and approval of IMVAMUNE/IMVANEX. We received funding of $25 million from the U.S. Government to cover additional costs of the expansion of the study and, therefore, 25% (1,000 subjects/4,000 subjects) of the Phase 3 costs have been recognized as contract costs under "Production costs" and $25 million has been recognized as revenue. The remaining 75% (3,000

subjects/4,000 subjects) of the Phase 3 costs have been capitalized under the IMVAMUNE/IMVANEX development project.

IMVAMUNE/IMVANEX development project includes development costs related to the registration of IMVAMUNE/IMVANEX under the RFP-3 contract. The disposals relates to delivery of development results, see the accounting policies described above.

Property, plant and equipment include land and buildings, production equipment, leasehold improvements, office and IT equipment and laboratory equipment and is measured at cost less accumulated depreciation and impairment losses.

Cost includes the costs directly attributable to the purchase of the asset, until the asset is ready for use. For assets constructed by the Company, cost includes materials, components, third-party suppliers and labour.

Interest expenses on loans to finance the construction of property, plant and equipment are included in cost if they relate to the construction period. Other borrowing costs are recognized in the income statement.

Depreciation is charged over the expected economic lives of the assets, and the depreciation methods, expected lives and residual values are reassessed individually for the assets at the end of each financial year. Assets are depreciated on a straightline basis over their estimated useful lives as follows:

The carrying amounts of property, plant and equipment carried at cost or amortized cost are tested annually to determine whether there are indications of any impairment in excess of that expressed in normal depreciation. If that is the case, the asset is written down to the recoverable amount, which is the higher of its fair value less costs to sell and its value in use. Impairment losses on property, plant and equipment are recognized under the same line item as depreciation of the assets.

Grants that compensate the Group for purchase of assets are recognized initially in the balance sheet as a liability and are then recognized in the income statement on a systematic basis over the useful life of the asset.

The management reviews the estimated useful lives of material property, plant and equipment at the end of each financial year. Management's review of useful lives in 2014 did not give rise to any changes as compared with 2013.

Property, plant and equipment under construction mainly includes investment in equipment and a small scale filling line at December 31, 2014.

Mortgage loans of DKK 35 million are secured by mortgages totaling DKK 50 million on the property Bøgeskovvej 9/Hejreskovvej 10A, Kvistgaard. In addition, as of December 31, 2014, mortgage deeds for a total of DKK 75 million have been issued. The carrying amount of assets mortgaged in security of mortgage loans is DKK 291 million.

Property, plant and equipment under construction mainly includes investment related to the expansion of the facility in Kvistgaard (DKK 31.1 million) at December 31, 2013.

The Company decided at the end of 2012 to discontinue its operations at the facility in Berlin where the production of clinical trial material to the MVA-BN-based vaccine candidates had taken place. The disposals of assets in 2013 primarily relates to the close down of the facility in Berlin.

Mortgage loans of DKK 37 million are secured by mortgages totaling DKK 50 million on the property Bøgeskovvej 9/Hejreskovvej 10A, Kvistgaard. In addition, as of December 31, 2013, mortgage deeds for a total of DKK 75 million have been issued in security of a construction loan of DKK 43 million.

The carrying amount of assets mortgaged in security of mortgage and construction loans is DKK 261 million.

Inventories except for raw materials are measured at the lower of cost using the weighted average cost formula method less write-downs for obsolescence and net realisable value. Raw materials are measured at cost based on the FIFO method.

For raw materials, cost is determined as direct acquisition costs incurred. The cost of finished goods produced in-house and work in progress includes raw materials, consumables, filling cost, QC testing and direct payroll costs plus indirect costs of production.

Indirect costs of production include indirect materials and labour as well as maintenance of and depreciation on the machinery used in production processes, factory buildings and equipment used and cost of production administration and management.

The net realisable value is the estimated sales price in the ordinary course of business less relevant sales costs determined on the basis of marketability, obsolescence and changes in the expected sales price.

Production overheads are measured on the basis of actual costs. The basis of the actual costs is reassessed regularly to ensure that they are adjusted for changes in the utilization of production capacity, production changes and other relevant factors.

Biological living material is used, and the measurements and assumptions for the estimates made may be incomplete or inaccurate, and unexpected events or circumstances may occur, which may cause the actual outcomes to later deviate from these estimates. It may be necessary to change previous estimates as a result of changes in the assumptions on which the estimates were based or due to new information or subsequent events, for which certainty could not be achieved in the earlier estimates.

Estimates that are material to the financial reporting are made in the determination of any impairment of inventories as a result of 'out-of-specification' products, expiry of products and sales risk.

Receivables are measured at initial recognition at fair value and subsequently at amortized value usually equal to the nominal value, net of depreciation, to counter the loss after an individual assessment of risk of loss.

There are no overdue receivables and there is no provision for bad debts as no losses are expected on trade receivables.

Receivables are measured at initial recognition at fair value and subsequently at amortized value usually equal to the nominal value.

Prepayments recognized under assets include costs paid in respect of subsequent financial years, including project costs incurred that relate to revenue of subsequent years. Prepayments are measured at cost.

Derivative financial instruments and liability relating to phantom shares are measured at fair value. For further details regarding measurement of fair value for phantom shares see note 27.

Other financial liabilities are measured at initial recognition at fair value less any transaction costs. Subsequent other financial liabilities are measured at amortized cost using the effective interest method, whereby the difference between proceeds and the nominal value is recognized in the income statement as a financial expense over the period. Amortized cost usually equal to the nominal value.

For a further description of financial instruments see note 22. The phantom share programs are described in note 27.

On initial recognition, derivative financial instruments are measured at the fair value on the settlement date.

Directly attributable costs related to the purchase or issuance of the individual financial instruments (transaction costs) are added to the fair value on initial recognition, unless the financial asset or the financial liability is measured at fair value with recognition of fair value adjustments in the income statement. Subsequently, they are measured at fair value at the balance sheet date based on the official exchange rates, market interest rates and other market data such as volatility adjusted for the special characteristics of each instrument.

Changes in the fair value of derivative financial instruments designated as and qualifying for recognition as fair value hedges of a recognized asset or a recognized liability are recognized in the income statement together with any changes in the value of the hedged asset or hedged liability. Changes in the fair value of derivative financial instruments designated as and qualifying for recognition as effective hedges of future transactions are recognized as comprehensive income. The ineffective portion is recognized immediately in the income statement. When the hedged transactions are realized, cumulative changes are recognized as part of the cost of the transactions in question.

For derivative financial instruments that do not qualify for hedge accounting, changes in fair value are recognized as financial income and financial expenses in the income statement as they occur.

Securities consist of listed bonds, which are measured at fair value as of the balance sheet date. Bonds with a maturity of less than three months on the date of acquisition are recognized in the line item "Cash and cash equivalents". Bavarian Nordic's portfolio of securities is treated as "financial items at fair value through profit or loss", as the portfolio is accounted for and valued on the basis of the fair value in compliance with Bavarian Nordic's investment policy.

Both realized and unrealized value adjustments are recognized in the income statement under financials.

Through its operations, investments and financing the Bavarian Nordic Group is exposed to fluctuations in exchange rates and interest rates. These risks are managed centrally in the Parent Company, which manages the Group's liquidity. The Group pursues a treasury policy approved by the board of directors. The policy operates with a low risk profile, so that exchange rate risks, interest rate risks and credit risks arise only in commercial relations. The Group therefore does not undertake any active speculation in financial risk.

The Group's capital structure is regularly assessed by the board of directors relative to the Group's cash flow position and cash flow budgets.

The Group is exposed to interest rate and foreign exchange risks as described below. Management believes that the Group is not sensitive to price risks as its raw material purchases make up a very modest part of its total production costs.

It is the Group's policy to hedge interest rate risks on loans whenever it is deemed that interest payments can be hedged at a satisfactory level relative to the related costs. Hedging will then consist of interest rate swaps that convert floating rate loans to fixed rate loans. The interest rate risk involved in placing cash funds and investing in securities is managed on the basis of duration.

The Group's exchange rate exposure is primarily to U.S. dollar and EUR. The exchange rate exposure to U.S. dollar is hedged to the greatest possible extent by matching incoming and outgoing payments denominated in U.S. dollar, looking at maximum one year ahead. Regular assessments are made of whether the remaining net position should be hedged by currency forward contracts or currency option contracts. The exposure to EUR is not hedged as management believes that fluctuations in EUR are limited due to the Danish fixed-rate policy which we expect to be maintained. Thus the fluctuations in EUR do not have a significant impact on financial performance.

Exchange rate risks in respect of recognized financial assets and liabilities

The table below shows the net effect it would have had on equity and profit for the year if the year-end exchange rates of U.S. dollar and EUR had been 15% or 1%, respectively, higher than the actual exchange rates.

Currency forward contracts and currency option contracts which are not designated in hedge accounting are classified as held for trading with fair value adjustments recognized in the income statement.

When the Company has temporary excess of U.S. dollar, the U.S. dollar are sold and repurchased at a lower $-rate, if possible, entering currency swaps.

The Group's bank deposits are placed in deposit accounts without restrictions. The Group's cash and cash equivalents totaled DKK 398.4 million as of December 31, 2014 (DKK 346.8 million).

The Group's fixed rate bond portfolio expires as shown below. Amounts are stated excluding interest.

Fluctuations in interest rate levels affect the Group's bond portfolio. An increase in the interest rate level by 1 percentage point relative to the interest rate level on the balance sheet date would have had a negative effect of DKK 4-5 million on the Group's profit and equity (DKK 5-6 million). A corresponding fall in the interest rate level would have had an equivalent positive effect on profit and equity.

The Group's finacial liabilites mature as shown below. Amounts are stated including interest.

With respect to the Group's mortgage debt, an increase in the applicable interest rate by 1 percentage point would have had a negative impact on the Group's profit and equity of DKK 0.4 million. A corresponding fall in the interest rate would have had an equivalent positive impact.

The Company has a credit facility of DKK 20 million (DKK 120 million). As of December 31, 2014 the credit facility is not used.

The primary credit risk relates to trade receivables. The Group's customers are predominantly public authorities, and the credit risk on the Company's receivables is therefore considered to be very low.

Cash and cash equivalents are not deemed to be subject to any special credit risk as they are deposited with Nordea. The bond portfolio is invested in either Danish government bonds, Danish mortgage bonds or bonds issued by Danish banks with high ratings.

Management regularly assesses whether the Group's capital structure best serves the interests of the Company and its shareholders. The overall goal is to ensure that the Group has a capital structure which supports its long-term growth target.

The portfolio of publicly traded government bonds and publicly traded mortgage bonds is valued at listed prices and price quotas.

Currency forward contracts, currency option contract and currency swap contracts are valued according to generally accepted valuation methods based on relevant observable swap curves and exchange rates.

Provisions are recognized when the Company has an obligation as a result of events in the current or in previous financial years with a probability that the obligation will result in an outflow of the Company's financial resources.

Provisions are measured as the best estimate of the costs needed at the balance sheet date to settle obligations. Provisions also include contingent payments at the conclusion of agreements, contracts, etc. Contingent payments are measured at fair value calculated as the probability that the results, which trigger future payments, are achieved and a fixed discount factor. Where payment is subject to continuing employment with the Group, the provision is built up over the vesting period. Changes to the assessed fair value of the contingent payments due to changes in risk factors are recognized in administrative costs. Adjustment of net present value is recognized as a financial expense.

A management estimate is required on recognition of contingent payments (incentive agreements with current and former members of the group management). Management considers in the light of expectations for the coming year's research and development achievements the likelihood that expected results will trigger contingent payments. Contingent payments were DKK 22 million as of December 31, 2014 (DKK 16 million as of December 31, 2013).

The estimates and assumptions applied are based on historical experience and other factors which management considers relevant under the circumstances, but which are inherently incomplete and inaccurate at the time of presentation of the financial statements, and unexpected events or circumstances may arise. The Company is subject to risks and uncertainties which may have the effect that the actual outcomes may deviate from the estimates made.

A long-term incentive agreement was entered into with Paul Chaplin in 2009. The incentive scheme offers one-off payments ranging from EUR 150,000 up to EUR 1.5 million. The one-off payments are subject to achievement of various potential future milestones and are furthermore conditional upon continuing employment (irrespective of the position held) with the Company at the time of the achievement of the respective milestone event. The long-term incentive scheme expires on December 31, 2015. Bavarian Nordic A/S has no obligation to continue other similar programs after that date.

The total outstanding consideration to Paul Chaplin amounts to a maximum of DKK 31 million but the Company only expects to pay-out a total amount of DKK 2 million before the incentive agreement expires end 2015.

In connection with the appointment of James B. Breitmeyer in 2013 a long-term incentive agreement was signed. The incentive scheme offers one-off payments ranging from $300.000 up to $1 million. The one-off payments are subject to achievement of various potential future milestones in relation to PROSTVAC and are furthermore conditional upon continuing employment with the Company at the time of the achievement of the respective milestone event.

The total outstanding consideration to James B. Breitmeyer amounts to a maximum of DKK 12 million. The risk-adjusted net present value amounts to DKK 5 million, of which DKK 2 million has been accrued as per December 31, 2014.

As part of an agreement entered into between the Company and the former Division President for Cancer Immunotherapy Reiner Laus regarding the Company's purchase of his shares in Bavarian Nordic, Inc. (formerly BN ImmunoTherapeutics, Inc.) in December 2009, Reiner Laus is entitled to receive a consideration triggered upon successful achievement of certain predefined milestones. In addition, a separate agreement regarding cancellation of certain contractual rights for Reiner Laus' sale of shares in Bavarian Nordic, Inc. entitles Reiner Laus to a consideration upon successful achievement of certain pre-defined milestones.

The total outstanding consideration to Reiner Laus amounts to a maximum of DKK 55 million. The risk-adjusted net present value amounts to DKK 18 million. The agreement remains unchanged after Reiner Laus' resignation.

The Company decided at the end of 2012 to discontinue its operations at the facility in Berlin. The Company still have a provision of DKK 1 million for repayment of some investment grants received from the German authorities, as Bavarian Nordic no longer meets all the criteria for receipt of the grants already disbursed.

Mortgage loans are measured at the time of borrowing at fair value less any transaction costs. Subsequently, mortgage debt is measured at amortized cost. This means that the difference between the proceeds of the loan and the amount to be repaid is recognized in the income statement over the term of the loan as a financial expense using the effective interest method.

The fair value of the debt amounts to DKK 38 million (DKK 83 million) based on the market value of the underlying bonds.

Advance payments are recognized under liabilities and will be recognized in the income statement as the delivery of paid products takes place.

In October 2014, Bavarian Nordic entered into a global license and supply agreement for the MVA-BN Filovirus (Ebola and Marburg) vaccine candidate with Crucell Holland B.V. Under this contract the Company has received a prepayment of DKK 356 million for Bulk Drog Substance (BDS) product to be delivered to Crucell during 2015. Revenue will be recognized along with the delivery of the BDS in 2015.

In April 2013, Bavarian Nordic received a new order from the U.S. Government for the delivery of up to 8 million doses of IMVAMUNE/IMVANEX. The Company received a total prepayment of DKK 158 million relating to the delivery of the first 4 million doses. The delivery of these doses was completed in the first half of 2014. In September 2014 the Company received the order for the last 4 million doses, following a prepayment of DKK 99 million. If Bavarian Nordic fails to fulfill the contract, the Company has a repayment obligation. It is the Company's assessment that the repayment obligation is reduced concurrently with delivery of vaccines, and a proportionate share of the prepayment is recognized as revenue in concurrence with the delivery of the doses. At year-end 2014, only 276 thousand doses remain to be delivered corresponding to a deferred revenue of DKK 7 million.

In 2012 the FDA requested to expand the Phase 3 study of IMVAMUNE/IMVANEX by an additional 1,000 subjects, bringing the total enrollment in the study to 4,000 patients. The Company has received funding of $25 million from U.S. Government to cover the additional costs of the expansion of the study. The funding was disbursed by way of four separate payments received in 2012 and 2013. The payments are recognized as revenue in concurrence with the recognition of the cost of the Phase 3 study. 25% of the Phase 3 costs are being expensed while the remaining 75% is being capitalized as IMVAMUNE/IMVANEX development project as described in note 15. The split between expensing (25%) and capitalizing (75%) is based on the original number of subjects in the Phase 3 study (3,000) and the increased number of subjects (4,000).

There is no repayment obligation. As of December 31, 2014, recognition of DKK 7 million in revenue is outstanding.

In 2012 the Company was contracted by the U.S. Government to complete a study covering the possible long-term storage of frozen Bulk Drug Substance (BDS), including collection of long-term stability data on frozen BDS. The contract runs until 2017 and has a total value of $5 million, which is being paid out in 6 separate payments. In 2014 the Company received a payment of DKK 4 million. The payments are recognized as revenue in concurrence with recognition of the cost of the study. As of December 31, 2014, recognition of DKK 5 million in revenue is outstanding. There is no repayment obligation.

The management and board of directors of Bavarian Nordic A/S are considered related parties.

Besides the remuneration of the board of directors, the CEO, the CFO and other group management, cf. note 8 and note 23, and the share-based payments, cf. note 27, there are no significant transactions with related parties.

Transactions with subsidiaries are eliminated in the consolidated financial statements, in accordance with the accounting policies.

Share-based incentive plans in which employees can only opt to buy shares in the parent company (warrants) are measured at the equity instruments' fair value at the grant date and recognized in the income statement over the vesting period. The balancing item is recognized directly in equity. The fair value on the date of grant is determined using the Black-Scholes model.

Cash-based incentive programs in which employees can have the difference between the agreed exercise price and the actual share price settled in cash (phantom shares) are measured at fair value at the date of grant and recognized in the income statement over the period when the final right of cash-settlement is obtained. Granted rights are subsequently re-measured on each balance sheet date and upon final settlement, and any changes in the fair value of the programs are recognized in the income statement. The balancing item is recognized under other liabilities.

The fair value of the cash-based incentive programs is determined using the Black-Scholes model.

In order to motivate and retain key employees and encourage the achievement of common goals for employees, management and shareholders, Bavarian Nordic A/S has established an incentive plan by way of warrant plans. Furthermore, the Company has established three-year phantom share programs for all employees of the Group.

The board of directors has been granting warrants to the Company´s management and selected employees of the Company and its subsidiaries. Up until 2013, the Company´s board of directors were also granted warrants, but in 2014 it was decided to change the remuneration structure for the board of directors.

The warrants are granted in accordance with the authorizations given to the board of directors by the shareholders. The board of directors has fixed the terms of and the size of the grants of warrants, taking into account authorizations from the shareholders, the Company's guidelines for incentive pay, an assessment of expectations of the recipient´s work efforts and contribution to the Company´s growth, as well as the need to motivate and retain the recipient. Grant takes place on the date of establishment of the program. Exercise of warrants is by default subject to continuing employment with the Group. The warrants granted are subject to the provisions of the Danish Public Companies Act regarding termination of employees prior to their exercise of warrants in the case of recipients who are subject to the act.

The exercise price and exercise periods for the individual grants are stated in the tables below.

In 2011, the Company established a three-year phantom share program under which all employees in the Group receive up to six phantom shares per month free of charge during the period from January 1, 2012 to December 31, 2014. Each employee who is a full-time employee during the entire term of the plan will be eligible to receive a maximum of 216 phantom shares. This program was exercised in January 2015.

In 2013, the Company established a three-year phantom share program covering all employees in the Group. The employees receive up to six phantom shares per month free of charge during the period from January 1, 2014 to December 31, 2016. Each employee who is a full-time employee during the entire term of the plan will be eligible to receive a maximum of 216 phantom shares.

In 2014, the Company established a three-year phantom share program covering all employees in the Group. The employees receive up to six phantom shares per month free of charge during the period from January 1, 2015 to December 31, 2017. Each employee who is a full-time employee during the entire term of the plan will be eligible to receive a maximum of 216 phantom shares.

Grants are made on a monthly basis during the life of the programs as long as the employee is employed with the Group.

On expiry of the programs, the employees may exercise the phantom shares granted to them and thus be entitled to a cash bonus calculated on the basis of the increase in the price of the Company´s shares. The exercise under the 2012-2014 program and the 2014-2016 program is conditional on the price of the Company´s shares being at least 10% higher than the exercise price at the time of exercise. The exercise under the 2015-2017 program is conditional on the price of the Company´s shares being at least DKK 5 higher than the exercise price at the time of exercise.

On expiry of the programs, former employees are entitled to settlement of the phantom shares granted during their term of employment.

The expense in respect of phantom shares granted in 2014 provided a cost of DKK 3.2 million.

The expense in respect of phantom shares granted in 2014 and revaluation of previously granted phantom shares provided a cost of DKK 11.2 million (2013: DKK 2.3 million).

The Company has license agreements with the National Cancer Institute (NCI) and Public Health Service (PHS) in the U.S. for PROSTVAC, CV 301 and brachyury, respectively. The

agreements include contingent liabilities for the Company to pay performance-based royalties, if and when certain milestone events are achieved. Payments considered remote are not included in the amounts above.

Further, the agreements include potential contingent liabilities for the Company to pay additional sublicensing royalties on the fair market value of consideration received, if and when the Company grants such sublicenses. See disclosures for PROSTVAC in note 30 below. These payments are not included in the amounts above.

Bavarian Nordic, Inc. has signed a contract with PPD Development, LP regarding implementation/management of the PROSPECT study. Bavarian Nordic, Inc. may terminate the contract with one month's notice. Upon termination of the contract before the study has been completed Bavarian Nordic, Inc. shall reimburse PPD Development, LP for all non-cancelable obligations to third parties as well as any obligations agreed on for the purpose of winding down the study.

The total outstanding consideration regarding incentive agreements with Paul Chaplin, James B. Breitmeyer and Reiner Laus amounts to a maximum of DKK 98 million. As per December 31, 2014 the provision amounts to DKK 22 million. For further description of the incentive agreement see note 23.

Bavarian Nordic A/S has by letter of indemnity (DKK 150 million) granted Nordea Bank Denmark a floating charge on unsecured claims arising from the sale of goods and services and stocks of raw materials, intermediate products and finished products. The floating charge secures the operating credit line of DKK 20 million. In addition, the floating charge secures the line for trading in financial instruments (DKK 50 million).

Based on management's assessment Bavarian Nordic is not involved in any lawsuits or arbitration cases which could have a material impact on the Group's financial position or results of operations.

In March 2015 Bavarian Nordic signed an agreement that provides Bristol-Myers Squibb an exclusive option to license and commercialize PROSTVAC. Bavarian Nordic can receive up to $975 million in upfront and milestone payments. The agreement includes the following payments:

At signing Bavarian Nordic received the upfront option grant payment of $60 million, which was recognized as a prepayment from customers in the statement of financial position as of September 30, 2015

In May 2015 The European Investment Bank granted Bavarian Nordic a EUR 50 million loan facility.

In June the U.S. National Institutes of Health exercised several contract options for the development of a vaccine against Marburg virus. The contract, originally awarded in 2012, will provide approximately $15 million in additional funds.

In July 2015 Bavarian Nordic received an IMVAMUNE/IMVANEX Smallpox Vaccine order from the U.S. Government valued at $133 million.

In August 2015 Bavarian Nordic announced the resignation of James B. Breitmeyer as Executive Vice President and Chief Development Officer.

In September 2015 Bavarian Nordic received a $9 million contract from Janssen as part of the Advanced Development of Prime-Boost Ebola Vaccine Regimen.

The consolidated financial statements were approved by the Board of Directors and Corporate Management and authorized for issue on October 19, 2015.

Unaudited Condensed Consolidated Income Statements for the Periods Ended
September 30, 2015 and 2014

Unaudited Condensed Consolidated Statements of Comprehensive Income for the Periods
Ended September 30, 2015 and 2014

Unaudited Condensed Consolidated Statements of Financial Position—Assets
as of September 30, 2015 and December 31, 2014

Unaudited Condensed Consolidated Statements of Financial Position—Equity and Liabilities
as of September 30, 2015 and December 31, 2014

Unaudited Condensed Consolidated Statements of Cash Flow for the Periods
Ended September 30, 2015 and 2014

Unaudited Condensed Consolidated Statements of Changes in Equity for the Periods Ended September 30, 2015 and 2014

The interim financial statements are prepared in accordance with IAS 34, Interim Financial Reporting, as issued by the International Accounting Standards Board (IASB).

The interim financial statements are presented in Danish kroner (DKK), which is considered the primary currency of the Group's activities and the functional currency of the parent company.

The accounting policies used in the interim financial statements are consistent with those used in the consolidated financial statements for 2014 and in accordance with the recognition and measurement policies in the International Financial Reporting Standards (IFRS) as issued by the IASB. However, the Company entered into a new significant agreement with Bristol-Myers Squibb (BMS) and the following represents the accounting policies with regard to this agreement:

In March 2015, Bavarian Nordic entered into an Option and License Agreement with BMS under which the Company can receive up to $975 million in upfront and milestone payments. The agreement includes the following payments:

Bavarian Nordic received the upfront option grant payment of $60 million, which was recognized as a prepayment from customers in the statement of financial position as of September 30, 2015 and will be recognized as revenue if and when BMS exercises the option (or if the option expires unexercised). Upon any such exercise of the option by BMS, the PROSTVAC license and any associated trial information to date will effectively transfer to BMS without any restrictions. Accordingly, we will recognize as revenue the option exercise and license payments. As BMS and we have agreed that we will complete the Phase 3 trial, a portion of the payment will be allocated to the completion of the Phase 3 trial of PROSTVAC if BMS exercises its option before the Phase 3 trial is completed. Upon completion of the Phase 3 trial, the Company will recognize as revenue the Phase 3 completion milestone payments. Regulatory and sales milestone payments will be recognized as revenue when relevant milestones are achieved.

As a result of the new agreement entered into with BMS regarding PROSTVAC, Management reassessed the accounting treatment of acquired NCI licenses. As part of the Company's business model and core operations, the Company acquires licenses for further development with subsequent disposal of the licenses either through a sale or by entering into a partnership agreement under

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

which the licenses are assumed to be effectively transferred to the partner. Prior to March 2015, previously acquired licenses from the National Cancer Institute (NCI) have been recognized as an intangible asset because it has been undetermined whether the licenses would be recovered through use by the Company itself or through sale. The NCI licenses will effectively transfer to BMS if the option related to the PROSTVAC agreement is exercised. In the first quarter of 2015, Management has therefore reclassified the acquired NCI licenses from intangible assets to development project for sale under current assets. Therefore, the carrying amount of the acquired licenses as of March 2015 (DKK 28 million) has been reclassified. As the reclassification is a result of the change in the Company's expectations of how it will realize the asset as a consequence of the agreement with BMS and thus, the comparative figures for 2014 have not been restated. Further, in accordance with the license agreement with NCI, Bavarian Nordic has an obligation to pay 10% of the received upfront option payment from BMS to NCI. This additional license payment of $6 million has been paid and is recognized as part of the development projects for sale (see below).

Development projects for sale consist of licenses that have been acquired with the intent to further develop the technology and subsequently disposal of the licenses either through a sale or by entering into a partnership agreement under which the licenses are assumed to be transferred to the partner.

Only the license payments to acquire the licenses are capitalized whereas all costs related to further development of the technology are expensed in the year they occur unless the criteria for recognition as an asset are met.

At initial recognition acquired licenses are measured at cost. Subsequently the acquired licenses are measured at the lower of cost and net realisable value.

The net realisable value is the estimated sales price in the ordinary course of business less relevant sales costs determined on the basis of marketability."

The Company refers to the consolidated financial statements for 2014 for further description of the accounting policies.

In the preparation of the interim financial statements according to IAS 34, Interim Financial Reporting, as issued by the IASB, Management is required to make certain estimates as many financial statement items cannot be reliably measured, but must be estimated. Such estimates comprise judgments made on the basis of the most recent information available at the reporting date. It may be necessary to change previous estimates as a result of changes to the assumptions on which the estimates were based or due to supplementary information, additional experience or subsequent events.

Similarly, the value of assets and liabilities often depends on future events that are somewhat uncertain. In that context, it is necessary to set out e.g. a course of events that reflects Management's assessment of the most probable course of events.

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

2. Significant accounting estimates, assumptions and uncertainties (Continued)

Further to the significant accounting estimates, assumptions and uncertainties, which are stated in the consolidated financial statements for 2014 (note 2), Management has not changed significant estimates and judgments regarding recognition and measurement.

In accordance with the Group's accounting policy, Management has assessed whether the upfront option payment of USD 60 million represents a transfer of goods or services that has value to Bristol-Myers Squibb on a stand-alone basis. As Management has concluded that no goods or services have been transferred yet, the upfront option payment of USD 60 million is recognized in the statement of financial position at September 30, 2015 as a prepayment from customers.

Research and development costs for the three and nine months ended September 30, 2015 of DKK 77,663 thousand and DKK 296,848 thousand, respectively, include severance costs of DKK 0 million and DKK 12 million as the research and development functions were centralized, the

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

divisional structure of "Cancer Immunotherapy" and "Infectious Diseases" was merged and the headcount was reduced by approximately 40 researchers in the second quarter of 2015.

Tax on income was an expense of DKK 3 million, corresponding to an effective tax rate of 5.6%. The low effective tax rate was primarily due to an intercompany transaction that results in a tax deductible expenditure for Bavarian Nordic A/S and is taxable income in Bavarian Nordic, Inc. But since the taxable income in Bavarian Nordic, Inc. can be offset with previously non-recognized tax losses carry forward, the net impact at the group level in the third quarter is a tax income, leading to a low effective tax rate for the nine month period ended September 30, 2015.

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

Prepayment from customers have increased by DKK 238 million compared to December 31, 2014. The second upfront payment from Janssen of DKK 222 million ($35.8 million) was received in January and the upfront option payment of DKK 399 million ($60 million) from Bristol-Myers Squibb was received in March. In the first nine months of 2015 DKK 379 million have been recognized as revenue along with the deliveries to Janssen. The upfront payments from Janssen covers 60-70% of the agreed sales price.

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

The Group has financial instruments measured at fair value at level 1 and level 2.

The portfolio of publicly traded government bonds and publicly traded mortgage bonds is valued at listed prices and price quotas.

Currency forward contracts, currency option contracts and currency swap contracts are valued according to generally accepted valuation methods based on relevant observable swap curves and exchange rates.

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

The total recognized cost of the warrant programs was DKK 7.9 million in the first nine months of 2015 (DKK 4.5 million for the first nine months of 2014).

15. Loan facility agreement of EUR 50 million entered with the European Investment Bank

In May 2015, Bavarian Nordic secured a loan facility of EUR 50 million from the European Investment Bank (EIB) in support of the Company's research and development of novel vaccines against Ebola and other infectious diseases as well as cancer immunotherapies. The loan facility, which is unsecured, may be utilized in one or more tranches. Under the terms of the agreement, Bavarian Nordic will have up to 18 months to draw on these monies. The loan is a three to five year

Notes to the Unaudited Condensed Consolidated Interim Financial Statements (Continued)

15. Loan facility agreement of EUR 50 million entered with the European Investment Bank (Continued)

bullet loan and could potentially carry a fixed or variable interest payment. The margin associated with the loan facility is 3.26%.

16. Significant changes in contingent liabilities and other contractual obligations

If and when Bristol-Myers Squibb (BMS) exercises the option under the Option and License Agreement for PROSTVAC from March 2015, Bavarian Nordic will receive $80 million, and the National Cancer Institute (NCI) has a right to 10% of this payment, i.e. $8 million.

In October 2015 Bavarian Nordic received an order valued at $6.4 million for 143,000 doses of IMVAMUNE/IMVANEX from the Public Health Agency of Canada.

In November 2015 Bavarian Nordic's share capital was increased by nominally DKK 1,852,970 as a consequence of employees' exercise of warrants. The total proceeds to Bavarian Nordic A/S from the capital increase amounted to DKK 10.8 million.

18. Approval of the unaudited condensed consolidated interim financial statements

The unaudited condensed consolidated interim financial statements were approved by the Board of Directors and Corporate Management and authorized for issue on November 27, 2015.

Through and including , 2016 (the 25th day after the date of this prospectus), all dealers effecting transactions in the ADSs, whether or not participating in this offering, may be required to deliver a prospectus. This delivery requirement is in addition to a dealer's obligation to deliver a prospectus when acting as an underwriter and with respect to an unsold allotment or subscription.

According to the Danish Companies Act, the general meeting is allowed to discharge our board members and members of our executive management from liability for any particular financial year based on a resolution relating to the financial statements. This discharge means that the general meeting will discharge such board members and members of our executive management from liability to our company. However, the general meeting cannot discharge any claims by individual shareholders or other third parties.

Additionally, we intend to enter into agreements with our board members and members of our executive management, pursuant to which, subject to limited exceptions, we will agree to indemnify such board members and members of our executive management from civil liability, including (i) any reasonably incurred damages or fines payable by them as a result of an act or failure to act in the exercise of their duties performed before or after the date of the indemnification agreement; (ii) any reasonable costs of conducting a defense against a claim; and (iii) any reasonable costs of appearing in other legal proceedings in which such individuals are involved as current or former board members or members of our executive management.

There is a risk that such agreements will be deemed void under Danish law, either because they are deemed contrary to the rules on discharge of liability in the Danish Companies Act, as set forth above, because the agreements are deemed contrary to sections 19 and 23 of the Danish Act on Damages, which contain mandatory provisions on recourse claims between an employee (including members of our executive management) and the company, or because the agreements are deemed contrary to the general provisions of the Danish Contracts Act.

The form of underwriting agreement filed as Exhibit 1.1 to this registration statement will also provide for indemnification of us and our directors and officers upon the terms and subject to the conditions specified therein.

The following list sets forth information as to all securities we have sold since January 1, 2013, which were not registered under the Securities Act.

In November 2015, we issued (i) 149,797 shares upon the exercise of outstanding warrants on November 16, 2015 at an exercise price of DKK 59.1 per share and (ii) 35,500 shares upon the exercise of outstanding warrants on November 16, 2015 at an exercise price of DKK 54.1 per share.

The transactions described above were made outside the United States pursuant to Regulation S or to U.S. persons pursuant to Rule 701 promulgated under the Securities Act, in that the securities were offered and sold either pursuant to written compensatory plans or pursuant to a

written contract relating to compensation, as provided by Rule 701 or to U.S. persons pursuant to Section 4(a)(2) of the Securities Act in that such sales and issuances did not involve a public offering.

(a) Exhibits. See the Exhibit Index attached to this registration statement, which is incorporated by reference herein.

(b) Financial Statement Schedules. Schedules not listed above have been omitted because the information required to be set forth therein is not applicable or is shown in the consolidated financial statements or notes thereto.

Insofar as indemnification for liabilities arising under the Securities Act may be permitted to directors, officers and controlling persons of the Registrant pursuant to the foregoing provisions, or otherwise, the Registrant has been advised that in the opinion of the SEC such indemnification is against public policy as expressed in the Securities Act, and is, therefore, unenforceable. In the event that a claim for indemnification against such liabilities (other than the payment by the Registrant of expenses incurred or paid by a director, officer, or controlling person of the Registrant in the successful defense of any action, suit or proceeding) is asserted by such director, officer or controlling person in connection with the securities being registered, the Registrant will, unless in the opinion of its counsel the matter has been settled by controlling precedent, submit to a court of appropriate jurisdiction the question of whether such indemnification by it is against public policy as expressed in the Securities Act and will be governed by the final adjudication of such issue.

The undersigned Registrant hereby undertakes to provide to the underwriters at the closing specified in the underwriting agreement certificates in such denominations and registered in such names as required by the underwriters to permit prompt delivery to each purchaser.

Pursuant to the requirements of the Securities Act of 1933, as amended, the Registrant has duly caused this Amendment No.1 to the Registration Statement on Form F-1 to be signed on its behalf by the undersigned, thereunto duly authorized, in Kvistgaard, Denmark, on January 11, 2016.

Pursuant to the requirements of the Securities Act, this Amendment No.1 to the Registration Statement has been signed by the following persons in the capacities and on the dates indicated.

AMENDED AND RESTATED DEPOSIT AGREEMENT

AMENDED AND RESTATED DEPOSIT AGREEMENT, dated as of January 5, 2016, by and among (i) Bavarian Nordic A/S, a company incorporated under the laws of the Kingdom of Denmark, and its successors (the “Company”), (ii) Deutsche Bank Trust Company Americas, an indirect wholly owned subsidiary of Deutsche Bank A.G., acting in its capacity as depositary, and any successor depositary hereunder (the “Depositary”), and (iii) all Holders and Beneficial Owners of American Depositary Shares evidenced by American Depositary Receipts issued hereunder (all such capitalized terms as hereinafter defined).

W I T N E S S E T H T H A T:

WHEREAS, the Company and Deutsche Bank Trust Company Americas entered into a Deposit Agreement dated as of May 29, 2013 (the “Old Deposit Agreement”) to provide for the deposit of Shares (as hereinafter defined) of the Company from time to time with the Custodian (as hereinafter defined) for the purposes set forth in such Old Deposit Agreement, for the creation of American Depositary Shares representing the Shares so deposited and for the execution and delivery of American Depositary Receipts (“Old Receipts”) evidencing the American Depositary Shares;

WHEREAS, the Company and Deutsche Bank Trust Company Americas, in its capacity as successor depositary under the Old Deposit Agreement, now wish to amend and restate the Old Deposit Agreement and the Old Receipts;

NOW, THEREFORE, in consideration of the foregoing premises and pursuant to Section 6.1 of the Old Deposit Agreement, the parties hereto hereby amend and restate the Old Deposit Agreement and the Old Receipts in their entirety as follows:

ARTICLE I

DEFINITIONS

All capitalized terms used, but not otherwise defined, herein shall have the meanings set forth below, unless otherwise clearly indicated:

SECTION 1.1 “Affiliate” shall have the meaning assigned to such term by the Commission under Regulation C promulgated under the Securities Act.

SECTION1.2 “Agent” shall mean such entity or entities as the Depositary may appoint under Section 7.10, including the Custodian or any successor or addition thereto.

SECTION1.3 “American Depositary Share(s)” and “ADS(s)” shall mean the securities represented by the rights and interests in the Deposited Securities granted to the Holders and Beneficial Owners pursuant to the terms and conditions of this Deposit Agreement

and evidenced by the American Depositary Receipts issued hereunder. Each American Depositary Share shall represent, prior to the close of business (NY time) on January 15, 2016, the right to receive one Share and as of the open of business (NY time) on January 19, 2016, the right to receive one-third of one Share, until there shall occur a distribution upon Deposited Securities referred to in Section 4.2 or a change in Deposited Securities referred to in Section 4.9 with respect to which additional American Depositary Receipts are not executed and delivered, and thereafter each American Depositary Share shall represent the Shares or Deposited Securities specified in such Sections.

SECTION 1.4 “ADS Record Date” shall have the meaning given to such term in Section 4.7.

SECTION1.5 “Beneficial Owner” shall mean as to any ADS, any person or entity having a beneficial interest in any ADSs. A Beneficial Owner need not be the Holder of the ADR evidencing such ADSs. A Beneficial Owner may exercise any rights or receive any benefits hereunder solely through the Holder of the ADR(s) evidencing the ADSs in which such Beneficial Owner has an interest.

SECTION1.6 “Business Day” shall mean each Monday, Tuesday, Wednesday, Thursday and Friday which is not (a) a day on which banking institutions in the Borough of Manhattan, The City of New York are authorized or obligated by law or executive order to close and (b) a day on which the market(s) in which Receipts are traded are closed.

SECTION 1.7 “Commission” shall mean the Securities and Exchange Commission of the United States or any successor governmental agency in the United States.

SECTION 1.8 “Company” shall mean Bavarian Nordic A/S, a company incorporated and existing under the laws of the Kingdom of Denmark, and its successors.

SECTION 1.9 “Custodian” shall mean, as of the date hereof, Danske Bank Aktieselskab, having its principal office at 2-12 Holmens Kanal, DK-1092 Copenhagen K, Denmark, as the custodian for the purposes of this Deposit Agreement, and any other firm or corporation which may hereinafter be appointed by the Depositary pursuant to the terms of Section 5.5 as a successor or an additional custodian or custodians hereunder, as the context shall require. The term “Custodian” shall mean all custodians, collectively.

SECTION 1.10 “Deliver” and “Delivery” shall mean, when used in respect of American Depositary Shares, Receipts, Deposited Securities and Shares, the physical delivery of the certificate representing such security, or the electronic delivery of such security by means of book-entry transfer, as appropriate, including, without limitation, through DRS/Profile (in the case of American Depositary Shares) and through VP Securities A/S (the “VP”) in the case of Shares. With respect to DRS/Profile ADRs, the terms “execute”, “issue”, “register”, “surrender”, “transfer” or “cancel” refer to applicable entries or movements to or within DRS/Profile.

SECTION 1.11 “Deposit Agreement” shall mean this Deposit Agreement and all

exhibits hereto, as the same may from time to time be amended and supplemented in accordance with the terms hereof.

SECTION 1.12 “Depositary” shall mean Deutsche Bank Trust Company Americas, an indirect wholly owned subsidiary of Deutsche Bank A.G., in its capacity as depositary under the terms of this Deposit Agreement, and any successor depositary hereunder.

SECTION 1.13 “Deposited Securities” as of any time shall mean Shares at such time deposited or deemed to be deposited under this Deposit Agreement and any and all other securities, property and cash received or deemed to be received by the Depositary or the Custodian in respect thereof and held hereunder, subject, in the case of cash, to the provisions of Section 4.6. The collateral delivered in connection with Pre-Release Transactions described in Section 2.10 hereof shall not constitute Deposited Securities.

SECTION 1.14 “Dollars” and “$” shall mean the lawful currency of the United States.

SECTION 1.15 “DRS/Profile” shall mean the system for the uncertificated registration of ownership of securities pursuant to which ownership of ADSs is maintained on the books of the Depositary without the issuance of a physical certificate and transfer instructions may be given to allow for the automated transfer of ownership between the books of DTC and the Depositary. Ownership of ADSs held in DRS/Profile is evidenced by periodic statements issued by the Depositary to the Holders entitled thereto.

SECTION 1.16 “DTC” shall mean The Depository Trust Company, the central book-entry clearinghouse and settlement system for securities traded in the United States, and any successor thereto. Participants within DTC are hereinafter referred to as “DTC Participants”.

SECTION 1.17 “Exchange Act” shall mean the United States Securities Exchange Act of 1934, as from time to time amended.

SECTION 1.18 “Foreign Currency” shall mean any currency other than Dollars.

SECTION 1.19 “Foreign Registrar” shall mean the entity, if any, that carries out the duties of registrar for the Shares or any successor as registrar for the Shares and any other appointed agent of the Company for the transfer and registration of Shares.

SECTION 1.20 “Holder” shall mean the person in whose name a Receipt is registered on the books of the Depositary (or the Registrar, if any) maintained for such purpose. A Holder may or may not be a Beneficial Owner. A Holder shall be deemed to have all requisite authority to act on behalf of those Beneficial Owners of the ADRs registered in such Holder’s name.

SECTION 1.21 “Indemnified Person” and “Indemnifying Person” shall have the meaning set forth in Section 5.8. hereof.

SECTION 1.22 “Pre-Release Transaction” shall have the meaning set forth in Section 2.10 hereof.

SECTION 1.23 “Principal Office” when used with respect to the Depositary, shall mean the principal office of the Depositary at which at any particular time its depositary receipts business shall be administered, which, at the date of this Deposit Agreement, is located at 60 Wall Street, New York, New York 10005, U.S.A.

SECTION 1.24 “Receipt(s)”; “American Depositary Receipt(s)” and “ADR(s)” shall mean the certificate(s) or DRS/Profile statements issued by the Depositary evidencing the American Depositary Shares issued under the terms of this Deposit Agreement, as such Receipts may be amended from time to time in accordance with the provisions of this Deposit Agreement. References to Receipts shall include physical certificated Receipts as well as ADSs issued through DRS/Profile, unless the context otherwise requires.

SECTION 1.25 “Registrar” shall mean the Depositary or any bank or trust company having an office in the Borough of Manhattan, The City of New York, which shall be appointed by the Depositary to register ownership of Receipts and transfer of Receipts as herein provided, shall include any co-registrar appointed by the Depositary for such purposes. Registrars (other than the Depositary) may be removed and substitutes appointed by the Depositary.

SECTION 1.26 “Restricted Securities” shall mean Shares, or American Depositary Shares representing such Shares, which (i) have been acquired directly or indirectly from the Company or any of its Affiliates in a transaction or chain of transactions not involving any public offering and subject to resale limitations under the Securities Act or the rules issued thereunder, or (ii) are held by an officer or director (or persons performing similar functions) or other Affiliate of the Company, or (iii) are subject to other restrictions on sale or deposit under the laws of the United States, the Kingdom of Denmark, or under a shareholders’ agreement or the Company’s constituent documents or under the regulations of an applicable securities exchange unless, in each case, such Shares are being sold to persons other than an Affiliate of the Company in a transaction (x) covered by an effective resale registration statement or (y) exempt from the registration requirements of the Securities Act (as hereinafter defined), and the Shares are not, when held by such person, Restricted Securities.

SECTION 1.27 “Securities Act” shall mean the United States Securities Act of 1933, as from time to time amended.

SECTION 1.28 “Shares” shall mean ordinary shares in registered form of the Company, heretofore validly issued and outstanding and fully paid or hereafter validly issued and outstanding and fully paid. References to Shares shall include evidence of rights to receive Shares, whether or not stated in the particular instance; provided, however, that in no event shall Shares include evidence of rights to receive Shares with respect to which the full purchase price has not been paid or Shares as to which pre-emptive rights have theretofore not been validly waived or exercised; provided further, however, that, if there shall occur any change in par value,

split-up, consolidation, exchange, reclassification, conversion or any other event described in Section 4.9, in respect of the Shares of the Company, the term “Shares” shall thereafter, to the extent permitted by law, represent the successor securities resulting from such change in par value, split-up, consolidation, exchange, conversion, reclassification or event.

SECTION 1.29 “United States” or “U.S.” shall mean the United States of America.

ARTICLE II

APPOINTMENT OF DEPOSITARY; FORM OF RECEIPT;
DEPOSIT OF SHARES; EXECUTION
AND DELIVERY, TRANSFER AND SURRENDER OF RECEIPTS

SECTION 2.1 Appointment of Depositary. The Company hereby appoints the Depositary as exclusive depositary for the Deposited Securities and hereby authorizes and directs the Depositary to act in accordance with the terms set forth in this Deposit Agreement. Each Holder and each Beneficial Owner, upon acceptance of any ADSs (or any interest therein) issued in accordance with the terms of this Deposit Agreement, shall be deemed for all purposes to (a) be a party to and bound by the terms of this Deposit Agreement and (b) appoint the Depositary its attorney-in-fact, with full power to delegate, to act on its behalf and to take any and all actions contemplated in this Deposit Agreement, to adopt any and all procedures necessary to comply with applicable law and to take such action as the Depositary in its sole discretion may deem necessary or appropriate to carry out the purposes of this Deposit Agreement (the taking of such actions to be the conclusive determinant of the necessity and appropriateness thereof).

SECTION 2.2 Form and Transferability of Receipts.

(a) Receipts in certificated form shall be substantially in the form set forth in Exhibit A annexed to this Deposit Agreement, with appropriate insertions, modifications and omissions, as hereinafter provided. Receipts may be issued in denominations of any number of American Depositary Shares. No Receipt in certificated form shall be entitled to any benefits under this Deposit Agreement or be valid or obligatory for any purpose, unless such Receipt shall have been executed by the Depositary by the manual or facsimile signature of a duly authorized signatory of the Depositary. The Depositary shall maintain books on which each Receipt so executed and Delivered, in the case of Receipts in certificated form, and each Receipt issued through any book-entry system, including, without limitation, DRS/Profile, in either case as hereinafter provided and the transfer of each such Receipt shall be registered. Receipts in certificated form bearing the manual or facsimile signature of a duly authorized signatory of the Depositary who was at any time a proper signatory of the Depositary shall bind the Depositary, notwithstanding that such signatory has ceased to hold such office prior to the execution and Delivery of such Receipts by the Registrar or did not hold such office on the date of issuance of such Receipts.

In addition to the foregoing, the Receipts may be endorsed with or have incorporated in the text thereof such legends or recitals or modifications not inconsistent with the provisions of this Deposit Agreement as may be reasonably required by the Depositary in order to comply with

any applicable law or regulations thereunder or with the rules and regulations of any securities exchange or market upon which American Depositary Shares may be listed, traded or quoted or conform with any usage with respect thereto, or to indicate any special limitations or restrictions to which any particular Receipts are subject by reason of the date of issuance of the underlying Deposited Securities or otherwise.

Notwithstanding anything in this Deposit Agreement or in the Receipt to the contrary, to the extent available by the Depositary, American Depositary Shares shall be evidenced by Receipts issued through DRS/Profile unless certificated Receipts are specifically requested by the Holder. Holders and Beneficial Owners shall be bound by the terms and conditions of this Deposit Agreement and of the form of Receipt set forth in Exhibit A annexed to this Deposit Agreement, regardless of whether their Receipts are certificated or issued through DRS/Profile.

(b) Subject to the limitations contained herein and in the form of Receipt, title to a Receipt (and to the American Depositary Shares evidenced thereby), when properly endorsed (in the case of certificated Receipts) or upon delivery to the Depositary of proper instruments of transfer, shall be transferable by delivery with the same effect as in the case of a negotiable instrument under the laws of the State of New York; provided, however, that the Depositary, notwithstanding any notice to the contrary, may treat the Holder thereof as the absolute owner thereof for the purpose of determining the person entitled to distribution of dividends or other distributions or to any notice provided for in this Deposit Agreement and for all other purposes and neither the Depositary nor the Company will have any obligation or be subject to any liability under the Deposit Agreement to any holder of a Receipt, unless such holder is the Holder thereof.

SECTION 2.3 Deposits. (a) Subject to the terms and conditions of this Deposit Agreement and applicable law, Shares or evidence of rights to receive Shares (other than Restricted Securities) may be deposited by any person (including the Depositary in its individual capacity but subject, however, in the case of the Company or any Affiliate of the Company, to Section 5.7 hereof) at any time, whether or not the transfer books of the Company or the Foreign Registrar, if any, are closed, by Delivery of the Shares to the Custodian. Every deposit of Shares shall be accompanied by the following: (A) (i) in the case of Shares Delivered in certificated form, appropriate instruments of transfer or endorsement, in a form satisfactory to the Custodian, and (ii) in the case of Shares Delivered by book-entry transfer, confirmation of such book-entry transfer to the Custodian or that irrevocable instructions have been given to cause such Shares to be so transferred, (B) such certifications and payments (including, without limitation, the Depositary’s fees and related charges) and evidence of such payments (including, without limitation, stamping or otherwise marking such Shares by way of receipt) as may be required by the Depositary or the Custodian in accordance with the provisions of this Deposit Agreement, (C) if the Depositary so requires, a written order directing the Depositary to execute and Deliver to, or upon the written order of, the person or persons stated in such order a Receipt or Receipts for the number of American Depositary Shares representing the Shares so deposited, (D) evidence satisfactory to the Depositary (which may include an opinion of counsel reasonably satisfactory to the Depositary provided at the cost of the person seeking to deposit Shares) that all conditions to such deposit have been met and all necessary approvals have been granted by, and there has been compliance with the rules and regulations of, any applicable governmental agency, and (E)

if the Depositary so requires, (i) an agreement, assignment or instrument satisfactory to the Depositary or the Custodian which provides for the prompt transfer by any person in whose name the Shares are or have been recorded to the Custodian of any distribution, or right to subscribe for additional Shares or to receive other property in respect of any such deposited Shares or, in lieu thereof, such indemnity or other agreement as shall be satisfactory to the Depositary or the Custodian and (ii) if the Shares are registered in the name of the person on whose behalf they are presented for deposit, a proxy or proxies entitling the Custodian to exercise voting rights in respect of the Shares for any and all purposes until the Shares so deposited are registered in the name of the Depositary, the Custodian or any nominee. No Share shall be accepted for deposit unless accompanied by confirmation or such additional evidence, if any is required by the Depositary, that is reasonably satisfactory to the Depositary or the Custodian that all conditions to such deposit have been satisfied by the person depositing such Shares under the laws and regulations of the Kingdom of Denmark and any necessary approval has been granted by any governmental body in the Kingdom of Denmark, if any, which is then performing the function of the regulator of currency exchange. The Depositary may issue Receipts against evidence of rights to receive Shares from the Company, any agent of the Company or any custodian, registrar, transfer agent, clearing agency or other entity involved in ownership or transaction records in respect of the Shares. Without limitation of the foregoing, the Depositary shall not knowingly accept for deposit under this Deposit Agreement any Shares required to be registered under the provisions of the Securities Act, unless a registration statement is in effect as to such Shares. The Depositary will use commercially reasonable efforts to comply with reasonable written instructions of the Company that the Depositary shall not accept for deposit hereunder any Shares specifically identified in such instructions at such times and under such circumstances as may reasonably be specified in such instructions in order to facilitate the Company’s compliance with the securities laws in the United States.

(b) As soon as practicable after receipt of any permitted deposit hereunder and compliance with the provisions of this Deposit Agreement, to the extent required, the Custodian shall present the Shares so deposited, together with the appropriate instrument or instruments of transfer or endorsement, duly stamped, to the Foreign Registrar for transfer and registration of the Shares (as soon as transfer and registration can be accomplished and at the expense of the person for whom the deposit is made) in the name of the Depositary, the Custodian or a nominee of either. Deposited Securities shall be held by the Depositary or by a Custodian for the account and to the order of the Depositary or a nominee, in each case for the account of the Holders and Beneficial Owners, at such place or places as the Depositary or the Custodian shall determine.

(c) In the event any Shares are deposited which entitle the holders thereof to receive a per-share distribution or other entitlement in an amount different from the Shares then on deposit, the Depositary is authorized to take any and all actions as may be necessary (including, without limitation, making the necessary notations on Receipts) to give effect to the issuance of such ADSs and to ensure that such ADSs are not fungible with other ADSs issued hereunder until such time as the entitlement of the Shares represented by such non-fungible ADSs equals that of the Shares represented by ADSs prior to such deposit. The Company agrees to give timely written notice to the Depositary if any Shares issued or to be issued contain rights different from those of any other Shares theretofore issued and shall assist the Depositary with the establishment

of procedures enabling the identification of such non-fungible Shares upon Delivery to the Custodian.

SECTION 2.4 Execution and Delivery of Receipts. After the deposit of any Shares pursuant to Section 2.3 hereof, the Custodian shall notify the Depositary of such deposit and the person or persons to whom or upon whose written order a Receipt or Receipts are Deliverable in respect thereof and the number of American Depositary Shares to be evidenced thereby. Such notification shall be made by letter, first class airmail postage prepaid, or, at the request, risk and expense of the person making the deposit, by cable, telex, SWIFT, facsimile or electronic transmission. After receiving such notice from the Custodian, the Depositary, subject to this Deposit Agreement (including, without limitation, the payment of the fees, expenses, taxes and/or other charges owing hereunder), shall issue the ADSs representing the Shares so deposited to or upon the order of the person or persons named in the notice Delivered to the Depositary and shall execute and Deliver a Receipt registered in the name or names requested by such person or persons evidencing in the aggregate the number of American Depositary Shares to which such person or persons are entitled. Nothing herein shall prohibit any Pre-Release Transaction upon the terms set forth in this Deposit Agreement.

SECTION 2.5 Transfer of Receipts; Combination and Split-up of Receipts.

(a) Transfer. The Depositary, or, if a Registrar (other than the Depositary) for the Receipts shall have been appointed, the Registrar, subject to the terms and conditions of this Deposit Agreement, shall register transfers of Receipts on its books, upon surrender at the Principal Office of the Depositary of a Receipt by the Holder thereof in person or by duly authorized attorney, properly endorsed in the case of a certificated Receipt or accompanied by, or in the case of DRS/Profile Receipts receipt by the Depositary of, proper instruments of transfer (including signature guarantees in accordance with standard industry practice) and duly stamped as may be required by the laws of the State of New York and of the United States and any other applicable jurisdiction. Subject to the terms and conditions of this Deposit Agreement, including payment of the applicable fees and charges of the Depositary set forth in Section 5.9 hereof and Article (9) of the Receipt, the Depositary shall execute a new Receipt or Receipts and Deliver the same to or upon the order of the person entitled thereto evidencing the same aggregate number of American Depositary Shares as those evidenced by the Receipts surrendered.

(b) Combination & Split Up. The Depositary, subject to the terms and conditions of this Deposit Agreement shall, upon surrender of a Receipt or Receipts for the purpose of effecting a split-up or combination of such Receipt or Receipts and upon payment to the Depositary of the applicable fees and charges set forth in Section 5.9 hereof and Article (9) of the Receipt, execute and Deliver a new Receipt or Receipts for any authorized number of American Depositary Shares requested, evidencing the same aggregate number of American Depositary Shares as the Receipt or Receipts surrendered.

(c) Co-Transfer Agents. The Depositary may appoint one or more co-transfer agents for the purpose of effecting transfers, combinations and split-ups of Receipts at designated transfer offices on behalf of the Depositary. In carrying out its functions, a co-transfer agent may

require evidence of authority and compliance with applicable laws and other requirements by Holders or persons entitled to such Receipts and will be entitled to protection and indemnity, in each case to the same extent as the Depositary. Such co-transfer agents may be removed and substitutes appointed by the Depositary. Each co-transfer agent appointed under this Section 2.5 (other than the Depositary) shall give notice in writing to the Depositary accepting such appointment and agreeing to be bound by the applicable terms of this Deposit Agreement.

(d) At the request of a Holder, the Depositary shall, for the purpose of substituting a certificated Receipt with a Receipt issued through DRS/Profile, or vice versa, execute and Deliver a certificated Receipt or DRS/Profile statement, as the case may be, for any authorized number of American Depositary Shares requested, evidencing the same aggregate number of American Depositary Shares as those evidenced by the certificated Receipt or DRS/Profile statement, as the case may be, substituted.

SECTION 2.6 Surrender of Receipts and Withdrawal of Deposited Securities. Upon surrender, at the Principal Office of the Depositary, of American Depositary Shares for the purpose of withdrawal of the Deposited Securities represented thereby, and upon payment of (i) the fees and charges of the Depositary for the making of withdrawals of Deposited Securities and cancellation of Receipts (as set forth in Section 5.9 hereof and Article (9) of the Receipt) and (ii) all applicable taxes and/or governmental charges payable in connection with such surrender and withdrawal, and subject to the terms and conditions of this Deposit Agreement, the Company’s constituent documents, Section 7.8 hereof and any other provisions of or governing the Deposited Securities and other applicable laws, the Holder shall be entitled to Delivery, to him or upon his order, of the Deposited Securities at the time represented by the American Depositary Shares so surrendered. American Depositary Shares may be surrendered for the purpose of withdrawing Deposited Securities by Delivery of a Receipt evidencing such American Depositary Shares (if held in certificated form) or by book-entry Delivery of such American Depositary Shares to the Depositary.

A Receipt surrendered for such purposes shall, if so required by the Depositary, be properly endorsed in blank or accompanied by proper instruments of transfer in blank, and if the Depositary so requires, the Holder thereof shall execute and deliver to the Depositary a written order directing the Depositary to cause the Deposited Securities being withdrawn to be Delivered to or upon the written order of a person or persons designated in such order. Thereupon, the Depositary shall direct the Custodian to Deliver (without unreasonable delay) at the designated office of the Custodian or through a book entry Delivery of the Shares (in either case, subject to Sections 2.7, 3.1, 3.2, 5.9, and to the other terms and conditions of this Deposit Agreement, to the Company’s constituent documents, to the provisions of or governing the Deposited Securities and to applicable laws, now or hereafter in effect) through the VP to or upon the written order of the person or persons designated in the order delivered to the Depositary as provided above, the Deposited Securities represented by such American Depositary Shares, together with any certificate or other proper documents of or relating to title of the Deposited Securities as may be legally required, as the case may be, to or for the account of such person.

The Depositary may, in its discretion, refuse to accept for surrender a number of American Depositary Shares representing a number other than a whole number of Shares. In the case of surrender of a Receipt evidencing a number of American Depositary Shares representing other than a whole number of Shares, the Depositary shall cause ownership of the appropriate whole number of Shares to be Delivered in accordance with the terms hereof, and shall, at the discretion of the Depositary, either (i) issue and Deliver to the person surrendering such Receipt a new Receipt evidencing American Depositary Shares representing any remaining fractional Share, or (ii) sell or cause to be sold the fractional Shares represented by the Receipt surrendered and remit the proceeds of such sale (net of (a) applicable fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) to the person surrendering the Receipt.

At the request, risk and expense of any Holder so surrendering a Receipt, and for the account of such Holder, the Depositary shall direct the Custodian to forward (to the extent permitted by law) any cash or other property (other than securities) held in respect of, and any certificate or certificates and other proper documents of or relating to title to, the Deposited Securities represented by such Receipt to the Depositary for Delivery at the Principal Office of the Depositary, and for further Delivery to such Holder. Such direction shall be given by letter or, at the request, risk and expense of such Holder, by cable, telex, electronic or facsimile transmission. Upon receipt by the Depositary, the Depositary may make delivery to such person or persons entitled thereto at the Principal Office of the Depositary of any dividends or cash distributions with respect to the Deposited Securities represented by such American Depositary Shares, or of any proceeds of sale of any dividends, distributions or rights, which may at the time be held by the Depositary.

SECTION 2.7 Limitations on Execution and Delivery, Transfer, etc. of Receipts; Suspension of Delivery, Transfer, etc.

(a) Additional Requirements. As a condition precedent to the execution and Delivery, registration, registration of transfer, split-up, subdivision combination or surrender of any Receipt, the delivery of any distribution thereon or withdrawal of any Deposited Securities, the Depositary or the Custodian may require (i) payment from the depositor of Shares or presenter of the Receipt of a sum sufficient to reimburse it for any tax or other governmental charge and any stock transfer or registration fee with respect thereto (including any such tax or charge and fee with respect to Shares being deposited or withdrawn) and payment of any applicable fees and charges of the Depositary as provided in Section 5.9 hereof and Article (9) of the Receipt, (ii) the production of proof satisfactory to it as to the identity and genuineness of any signature or any other matter contemplated by Section 3.1 hereof and (iii) compliance with (A) any laws or governmental regulations relating to the execution and Delivery of Receipts or American Depositary Shares or to the withdrawal or Delivery of Deposited Securities and (B) such reasonable regulations and procedures as the Depositary may establish consistent with the provisions of this Deposit Agreement and applicable law.

(b) Additional Limitations. The issuance of ADSs against deposits of Shares generally or against deposits of particular Shares may be suspended, or the issuance of ADSs

against the deposit of particular Shares may be withheld, or the registration of transfer of Receipts in particular instances may be refused, or the registration of transfers of Receipts generally may be suspended, during any period when the transfer books of the Depositary are closed or if any such action is deemed necessary or advisable by the Depositary or the Company, in good faith, at any time or from time to time because of any requirement of law, any government or governmental body or commission or any securities exchange on which the Receipts or Shares are listed, or under any provision of this Deposit Agreement or provisions of, or governing, the Deposited Securities, or any meeting of shareholders of the Company or for any other reason, subject, in all cases, to Section 7.8 hereof.

SECTION 2.8 Lost Receipts, etc. In case any Receipt shall be mutilated, destroyed, lost or stolen, unless the Depositary has notice that such ADR has been acquired by a bona fide purchaser, subject to Section 5.9 hereof, the Depositary shall execute and Deliver a new Receipt (which, in the discretion of the Depositary may be issued through DRS/Profile unless specifically requested otherwise) in exchange and substitution for such mutilated Receipt upon cancellation thereof, or in lieu of and in substitution for such destroyed, lost or stolen Receipt. Before the Depositary shall execute and Deliver a new Receipt in substitution for a destroyed, lost or stolen Receipt, the Holder thereof shall have (a) filed with the Depositary (i) a request for such execution and delivery before the Depositary has notice that the Receipt has been acquired by a bona fide purchaser and (ii) a sufficient indemnity bond in form and amount acceptable to the Depositary and (b) satisfied any other reasonable requirements imposed by the Depositary.

SECTION 2.9 Cancellation and Destruction of Surrendered Receipts. All Receipts surrendered to the Depositary shall be cancelled by the Depositary. The Depositary is authorized to destroy Receipts so cancelled in accordance with its customary practices. Cancelled Receipts shall not be entitled to any benefits under this Deposit Agreement or be valid or obligatory for any purpose.

SECTION 2.10 Pre-Release. Subject to the further terms and provisions of this Section 2.10, the Depositary, its Affiliates and their agents, on their own behalf, may own and deal in any class of securities of the Company and its Affiliates and in ADSs. In its capacity as Depositary, the Depositary may (i) issue ADSs prior to the receipt of Shares (each such transaction a “Pre-Release Transaction”) as provided below and (ii) Deliver Shares upon the receipt and cancellation of ADSs that were issued in a Pre-Release Transaction, but for which Shares may not yet have been received. The Depositary may receive ADSs in lieu of Shares under (i) above and receive Shares in lieu of ADSs under (ii) above. Each such Pre-Release Transaction will be (a) subject to a written agreement whereby the person or entity (the “Applicant”) to whom ADSs or Shares are to be Delivered (1) represents that at the time of the Pre-Release Transaction the Applicant or its customer beneficially owns the Shares or ADSs that are to be Delivered by the Applicant under such Pre-Release Transaction, (2) agrees to indicate the Depositary as owner of such Shares or ADSs in its records and to hold such Shares or ADSs in trust for the Depositary until such Shares or ADSs are Delivered to the Depositary or the Custodian, (3) unconditionally guarantees to deliver to the Depositary or the Custodian, as applicable, such Shares or ADSs, and (4) agrees to any additional restrictions or requirements

that the Depositary deems appropriate, (b) at all times fully collateralized with cash, United States government securities or such other collateral as the Depositary deems appropriate, (c) terminable by the Depositary on not more than five (5) Business Days’ notice and (d) subject to such further indemnities and credit regulations as the Depositary deems appropriate. The Depositary will normally limit the number of ADSs and Shares involved in such Pre-Release Transactions at any one time to thirty percent (30%) of the ADSs outstanding (without giving effect to ADSs outstanding under (i) above), provided, however, that the Depositary reserves the right to disregard such limit from time to time as it deems appropriate. The Depositary may also set limits with respect to the number of ADSs and Shares involved in Pre-Release Transactions with any one person on a case by case basis as it deems appropriate.

The Depositary may retain for its own account any compensation received by it in conjunction with the foregoing. Collateral provided pursuant to (b) above, but not the earnings thereon, shall be held for the benefit of the Holders (other than the Applicant).

ARTICLE III

CERTAIN OBLIGATIONS OF HOLDERS
AND BENEFICIAL OWNERS OF RECEIPTS

SECTION 3.1 Proofs, Certificates and Other Information. Any person presenting Shares for deposit, any Holder and any Beneficial Owner may be required, and every Holder and Beneficial Owner agrees, from time to time to provide to the Depositary or the Custodian such proof of citizenship or residence, taxpayer status, payment of all applicable taxes or other governmental charges, exchange control approval, legal or beneficial ownership of ADSs and Deposited Securities, compliance with applicable laws and the terms of this Deposit Agreement and the provisions of, or governing, the Deposited Securities or other information; to execute such certifications and to make such representations and warranties, and to provide such other information and documentation, in all cases as the Depositary may deem necessary or proper or as the Company may reasonably require by written request to the Depositary consistent with its obligations hereunder. The Depositary and the Registrar, as applicable, may withhold the execution or Delivery or registration of transfer of any Receipt or the distribution or sale of any dividend or distribution of rights or of the proceeds thereof, or to the extent not limited by the terms of Section 7.8 hereof, the Delivery of any Deposited Securities, until such proof or other information is filed or such certifications are executed, or such representations and warranties are made, or such other documentation or information provided, in each case to the Depositary’s and the Company’s satisfaction. The Depositary shall from time to time on the written request of the Company advise the Company of the availability of any such proofs, certificates or other information and shall, at the Company’s sole expense, provide or otherwise make available copies thereof to the Company upon written request therefor by the Company, unless such disclosure is prohibited by law. Each Holder and Beneficial Owner agrees to provide any information requested by the Company or the Depositary pursuant to this paragraph. Nothing herein shall obligate the Depositary to (i) obtain any information for the Company if not provided by the Holders or Beneficial Owners or (ii) verify or vouch for the accuracy of the information so provided by the Holders or Beneficial Owners.

SECTION 3.2 Liability for Taxes and Other Charges. If any present or future tax or other governmental charge shall become payable by the Depositary or the Custodian with respect to any Shares, Deposited Securities, Receipts or ADSs, such tax or other governmental charge shall be payable by the Holders and Beneficial Owners to the Depositary and such Holders and Beneficial Owners shall be deemed liable therefor. The Company, the Custodian and/or the Depositary may withhold or deduct from any distributions made in respect of Deposited Securities and may sell for the account of a Holder and/or Beneficial Owner any or all of the Deposited Securities and apply such distributions and sale proceeds in payment of such taxes (including applicable interest and penalties) or charges, with the Holder and the Beneficial Owner remaining fully liable for any deficiency. In addition to any other remedies available to it, the Depositary and the Custodian may refuse the deposit of Shares, and the Depositary may refuse to issue ADSs, to Deliver ADRs, register the transfer, split-up or combination of ADRs and (subject to Section 7.8) the withdrawal of Deposited Securities, until payment in full of such tax, charge, penalty or interest is received. Every Holder and Beneficial Owner agrees to, and shall, indemnify the Depositary, the Company, the Custodian and each and every of their respective officers, directors, employees, agents and Affiliates against, and hold each of them harmless from, any claims with respect to taxes, additions to tax (including applicable interest and penalties thereon) arising out of any refund of taxes, reduced rate of withholding at source or other tax benefit obtained for or by such Holder and/or Beneficial Owner. The obligations of Holders and Beneficial Owners of Receipts under this Section 3.2 shall survive any transfer of Receipts, any surrender of Receipts and withdrawal of Deposited Securities, or the termination of this Deposit Agreement.

SECTION 3.3 Representations and Warranties on Deposit of Shares. Each person depositing Shares under the Deposit Agreement shall be deemed thereby to represent and warrant that (i) such Shares and the certificates therefor are duly authorized, validly issued, fully paid, non-assessable and were legally obtained by such person, (ii) all preemptive (and similar) rights, if any, with respect to such Shares have been validly waived or exercised, (iii) the person making such deposit is duly authorized so to do, (iv) the Shares presented for deposit are free and clear of any lien, encumbrance, security interest, charge, mortgage or adverse claim, and are not, and the American Depositary Shares issuable upon such deposit will not be, Restricted Securities and (v) the Shares presented for deposit have not been stripped of any rights or entitlements. Such representations and warranties shall survive the deposit and withdrawal of Shares, the issuance and cancellation of American Depositary Shares in respect thereof and the transfer of such American Depositary Shares. If any such representations or warranties are false in any way, the Company and the Depositary shall be authorized, at the cost and expense of the person depositing Shares, to take any and all actions necessary to correct the consequences thereof. Each Holder and Beneficial Owner further agrees to indemnify the Depositary, any Custodian, the Company and each of their respective directors, officers, employees, agents and Affiliates against, and hold each of them harmless from, any Losses (as defined in Section 5.8 hereof) which any of them may incur or which may be made against any of them as a result of or in connection with the foregoing representations and warranties.

SECTION 3.4 Ownership Restrictions. Holders and Beneficial Owners shall comply with any limitations on ownership of Shares under the constituent documents of the

Company or applicable Danish law as if they held the number of Shares their ADSs represent. The Company shall inform the Holders, Beneficial Owners and the Depositary of any such ownership restrictions in place under the constituent documents of the Company from time to time. Holders and Beneficial Owners will be required to determine the requirements of Danish law with respect to any limitations on ownership of Shares.

SECTION 3.5 Compliance with Information Requests. Notwithstanding any other provision of this Deposit Agreement, the constituent documents of the Company and applicable law, each Holder and Beneficial Owner agrees to (a) provide such information as the Company or the Depositary may request pursuant to law (including, without limitation, relevant Danish law, any applicable law of the United States, the constituent documents of the Company, any resolutions of the Company’s Board of Directors adopted pursuant to such constituent documents, the requirements of any markets or exchanges upon which the Shares, ADSs or Receipts are listed or traded, or to any requirements of any electronic book-entry system by which the ADSs or Receipts may be transferred), regarding the capacity in which they own or owned Receipts, the identity of any other persons then or previously interested in such Receipts and the nature of such interest, and any other applicable matters, and (b) be bound by and subject to applicable provisions of the laws of the Kingdom of Denmark, the constituent documents of the Company and the requirements of any markets or exchanges upon which the ADSs, Receipts or Shares are listed or traded, or pursuant to any requirements of any electronic book-entry system by which the ADSs, Receipts or Shares may be transferred, to the same extent as if such Holder and Beneficial Owner held Shares directly, in each case irrespective of whether or not they are Holders or Beneficial Owners at the time such request is made and (c) without limiting the generality of the foregoing, comply with all applicable provisions of Danish law, the rules and requirements of any stock exchange on which the Shares are, or will be registered, traded or listed and the Company’s constituent documents regarding any such Holder’s or Beneficial Owner’s interest in Shares (including the aggregate of ADSs and Shares held by each such Holder or Beneficial Owner) and/or the disclosure of interests therein, whether or not the same may be enforceable against such Holder or Beneficial Owner. Each Holder and Beneficial Owner of ADSs further agrees to furnish the Company and the Depositary with any such notification made in accordance with this Section 3.5 and to comply with requests for information from the Company or the Depositary pursuant to the laws of the Kingdom of Denmark, the rules and requirements of any stock exchange on which the Shares are, or will be registered, traded or listed, and the Company’s constituent documents, whether or not they are Holders and/or Beneficial Owners at the time of such request. The Depositary agrees to use its reasonable efforts to forward upon the request of the Company, and at the Company’s expense, any such request from the Company to the Holders and to forward to the Company any such responses to such requests received by the Depositary.

The Company reserves the right to instruct Holders to deliver their ADSs for cancellation and withdrawal of the Deposited Securities so as to permit the Company to deal directly with the Holder thereof as a holder of Shares and Holders agree to comply with such instructions. The Depositary agrees to cooperate with the Company in its efforts to inform Holders of the Company’s exercise of its rights under this paragraph and agrees to consult with, and provide reasonable assistance without risk, liability or expense on the part of the Depositary, to the

Company on the manner or manners in which it may enforce such rights with respect to any Holder.

ARTICLE IV

THE DEPOSITED SECURITIES

SECTION 4.1 Cash Distributions. Whenever the Depositary receives confirmation from the Custodian of receipt of any cash dividend or other cash distribution on any Deposited Securities, or receives proceeds from the sale of any Shares, rights, securities or other entitlements under the terms hereof, the Depositary will, if at the time of receipt thereof any amounts received in a Foreign Currency can in the judgment of the Depositary (pursuant to Section 4.6 hereof) be converted on a practicable basis into Dollars transferable to the United States, promptly convert or cause to be converted such cash dividend, distribution or proceeds into Dollars (on the terms described in Section 4.6) and will distribute promptly the amount thus received (net of (a) the applicable fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) to the Holders of record as of the ADS Record Date in proportion to the number of American Depositary Shares held by such Holders respectively as of the ADS Record Date. The Depositary shall distribute only such amount, however, as can be distributed without attributing to any Holder a fraction of one cent. Any such fractional amounts shall be rounded down to the nearest whole cent and so distributed to Holders entitled thereto. Holders and Beneficial Owners understand that in converting Foreign Currency, amounts received on conversion are calculated at a rate which exceeds three or four decimal places (the number of decimal places used by the Depositary to report distribution rates). The excess amount may be retained by the Depositary as an additional cost of conversion, irrespective of any other fees and expenses payable or owing hereunder and shall not be subject to escheatment. If the Company, the Custodian or the Depositary is required to withhold and does withhold from any cash dividend or other cash distribution in respect of any Deposited Securities an amount on account of taxes, duties or other governmental charges, the amount distributed to Holders of the American Depositary Shares representing such Deposited Securities shall be reduced accordingly. Such withheld amounts shall be forwarded by the Company, the Custodian or the Depositary to the relevant governmental authority. Evidence of payment thereof by the Company shall be forwarded by the Company to the Depositary upon request. The Depositary will forward to the Company or its agent such information from its records as the Company may reasonably request to enable the Company or its agent to file necessary reports with governmental agencies, and such reports necessary to obtain benefits under the applicable tax treaties for the Holders and Beneficial Owners of Receipts.

SECTION 4.2 Distribution in Shares. If any distribution upon any Deposited Securities consists of a dividend in, or free distribution of, Shares, the Company shall cause such Shares to be deposited with the Custodian and registered, as the case may be, in the name of the Depositary, the Custodian or any of their nominees. Upon receipt of confirmation of such deposit from the Custodian, the Depositary shall establish the ADS Record Date upon the terms described in Section 4.7 and shall, subject to Section 5.9 hereof, either (i) distribute to the Holders as of the ADS Record Date in proportion to the number of American Depositary Shares held as of the ADS Record Date, additional American Depositary Shares, which represent in the

aggregate the number of Shares received as such dividend, or free distribution, subject to the other terms of this Deposit Agreement (including, without limitation, (a) the applicable fees and charges of, and expenses incurred by, the Depositary and (b) taxes and/or governmental charges), or (ii) if additional American Depositary Shares are not so distributed, each American Depositary Share issued and outstanding after the ADS Record Date shall, to the extent permissible by law, thenceforth also represent rights and interests in the additional Shares distributed upon the Deposited Securities represented thereby (net of (a) the applicable fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges). In lieu of Delivering fractional American Depositary Shares, the Depositary shall sell the number of Shares represented by the aggregate of such fractions and distribute the proceeds upon the terms described in Section 4.1. The Depositary may withhold any such distribution of Receipts if it has not received satisfactory assurances from the Company (including an opinion of counsel to the Company furnished at the expense of the Company) that such distribution does not require registration under the Securities Act or is exempt from registration under the provisions of the Securities Act. To the extent such distribution may be withheld, the Depositary may, subject to applicable law, dispose of all or a portion of such distribution in such amounts and in such manner, including by public or private sale, as the Depositary deems necessary and practicable, and the Depositary shall distribute the net proceeds of any such sale (after deduction of applicable (a) taxes and/or governmental charges and (b) fees and charges of, and expenses incurred by, the Depositary) to Holders entitled thereto upon the terms described in Section 4.1.

SECTION 4.3 Elective Distributions in Cash or Shares. Whenever the Company intends to distribute a dividend payable at the election of the holders of Shares in cash or in additional Shares, the Depositary shall, to the extent permitted by law and practicable, distribute to the Holders, on the basis of the same determination as is made in the local market in respect of the Shares for which no election is made, either (x) cash upon the terms described in Section 4.1 or (y) additional ADSs representing such additional Shares upon the terms described in Section 4.2.

SECTION 4.4 Distribution of Rights to Purchase Shares.

Whenever the Company intends to distribute to the holders of the Deposited Securities rights to subscribe for additional Shares, the Depositary shall determine whether it is lawful and reasonably practicable to sell such rights, and if it so determines that it is lawful and reasonably practicable, endeavor to sell such rights in a riskless principal capacity or otherwise, at such place and upon such terms (including public or private sale) as it may deem proper. The Company shall assist the Depositary to the extent necessary to determine such legality and practicability. The Depositary shall, upon such sale, convert and distribute proceeds of such sale (net of applicable (a) fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) upon the terms set forth in Section 4.1. If the Depositary is unable to arrange for the sale of the rights upon the terms described above, the Depositary shall allow such rights to lapse.

The Depositary shall not be responsible for, and the Company shall not be liable to Holders or Beneficial Owners for, (i) any failure to determine that it may be lawful or reasonably

practicable to sell such rights or (ii) any foreign exchange exposure or loss incurred in connection with such sale, or exercise. The Depositary shall not be responsible for the content of any materials forwarded to the Holders on behalf of the Company in connection with the rights distribution.

In the event that the Company, the Depositary or the Custodian shall be required to withhold and does withhold from any distribution of property (including rights) an amount on account of taxes or other governmental charges, the amount distributed to the Holders shall be reduced accordingly. In the event that the Depositary determines that any distribution is subject to any tax or other governmental charges which the Depositary is obligated to withhold, the Depositary may dispose of all or a portion of such property (including Shares and rights to subscribe therefor) in such amounts and in such manner, including by public or private sale, as the Depositary deems necessary and practicable to pay any such taxes and charges.

SECTION 4.5 Distributions Other Than Cash, Shares or Rights to Purchase Shares. Whenever the Company intends to distribute to the holders of Deposited Securities property other than cash, Shares or rights to purchase additional Shares, the Depositary shall endeavor to sell or cause such property to be sold in a public or private sale, at such place or places and upon such terms as it may deem proper and shall distribute the net proceeds, if any, of such sale received by the Depositary (net of applicable (a) fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) to the Holders as of the ADS Record Date upon the terms of Section 4.1. If the Depositary is unable to sell such property, the Depositary may dispose of such property in any way it deems reasonably practicable under the circumstances for nominal or no consideration and Holders and Beneficial Owners shall have no rights thereto or arising therefrom.

SECTION 4.6 Conversion of Foreign Currency. Whenever the Depositary or the Custodian shall receive Foreign Currency, by way of dividends or other distributions or the net proceeds from the sale of securities, property or rights, and in the judgment of the Depositary such Foreign Currency can at such time be converted on a practicable basis (by sale or in any other manner that it may determine in accordance with applicable law) into Dollars transferable to the United States and distributable to the Holders entitled thereto, the Depositary shall convert or cause to be converted, by sale or in any other manner that it may determine, such Foreign Currency into Dollars, and shall distribute such Dollars (net of any fees, expenses, taxes and/or other governmental charges incurred in the process of such conversion) in accordance with the terms of the applicable sections of this Deposit Agreement. If the Depositary shall have distributed warrants or other instruments that entitle the holders thereof to such Dollars, the Depositary shall distribute such Dollars to the holders of such warrants and/or instruments upon surrender thereof for cancellation, in either case without liability for interest thereon. Such distribution may be made upon an averaged or other practicable basis without regard to any distinctions among Holders on account of exchange restrictions, the date of delivery of any Receipt or otherwise.

Holders understand that in converting Foreign Currency, amounts received on conversion are calculated at a rate which may exceed the number of decimal places used by the Depositary to

report distribution rates (which in any case will not be less than two decimal places). Any excess amount may be retained by the Depositary as an additional cost of conversion, irrespective of any other fees and expenses payable or owing hereunder and shall not be subject to escheatment.

If such conversion or distribution can be effected only with the approval or license of any government or agency thereof, the Depositary may file such application for approval or license, if any, as it may deem necessary, practicable and at nominal cost and expense. Nothing herein shall obligate the Depositary to file or cause to be filed, or to seek effectiveness of any such application or license.

If at any time the Depositary shall determine that in its judgment the conversion of any Foreign Currency and the transfer and distribution of proceeds of such conversion received by the Depositary is not practical or lawful, or if any approval or license of any governmental authority or agency thereof that is required for such conversion, transfer and distribution is denied, or not obtainable at a reasonable cost, within a reasonable period or otherwise sought, the Depositary shall, in its sole discretion but subject to applicable laws and regulations, either (i) distribute the Foreign Currency (or an appropriate document evidencing the right to receive such Foreign Currency) received by the Depositary to the Holders entitled to receive such Foreign Currency, or (ii) hold such Foreign Currency uninvested and without liability for interest thereon for the respective accounts of the Holders entitled to receive the same.

The Depositary shall not incur any liability for, and the Company shall not incur any liability to Holders or Beneficial Owners for, any consequences of Foreign Currency conversion that may be incurred by Holders and/or Beneficial Owners on account of their ownership of American Depositary Shares or otherwise.

SECTION 4.7 Fixing of Record Date. Whenever necessary in connection with any distribution (whether in cash, Shares, rights, or other distribution), or whenever for any reason the Depositary causes a change in the number of Shares that are represented by each American Depositary Share, or whenever the Depositary shall receive notice of any meeting of or solicitation of holders of Shares or other Deposited Securities, or whenever the Depositary shall find it necessary or convenient, the Depositary shall fix a record date (the “ADS Record Date”), as close as practicable to the record date fixed by the Company with respect to the Shares (if applicable), for the determination of the Holders who shall be entitled to receive such distribution, to give instructions for the exercise of voting rights at any such meeting, or to give or withhold such consent, or to receive such notice or solicitation or to otherwise take action, or to exercise the rights of Holders with respect to such changed number of Shares represented by each American Depositary Share, or for any other reason. Subject to applicable law and the provisions of Section 4.1 through 4.6 and to the other terms and conditions of this Deposit Agreement, only the Holders of record at the close of business in New York on such ADS Record Date shall be so obligated or otherwise entitled to receive such distribution, to give such voting instructions, to receive such notice or solicitation, or otherwise take action.

SECTION 4.8 Voting of Deposited Securities. Subject to the next sentence, as soon as practicable after receipt of notice of any meeting at which the holders of Shares are

entitled to vote, or of solicitation of consents or proxies from holders of Shares or other Deposited Securities, the Depositary shall fix the ADS Record Date in respect of such meeting or solicitation of consent or proxy. The Depositary shall, if requested by the Company in writing in a timely manner (the Depositary having no obligation to take any further action if the request shall not have been received by the Depositary at least 30 days prior to the date of such vote or meeting) and at the Company’s expense and provided no U.S. legal prohibitions exist, mail by regular, ordinary mail delivery (or by electronic mail or as otherwise may be agreed between the Company and the Depositary in writing from time to time) or otherwise distribute to Holders as of the ADS Record Date: (a) such notice of meeting or solicitation of consent or proxy; (b) subject to the next paragraph, a statement that the Holders at the close of business on the ADS Record Date will be entitled, subject to any applicable law, the Company’s constituent documents and the provisions of or governing the Deposited Securities (which provisions, if any, shall be summarized in pertinent part by the Company), to instruct the Depositary as to the exercise of the voting rights, if any, pertaining to the Shares or other Deposited Securities represented by such Holder’s American Depositary Shares; and (c) a brief statement as to the manner in which such instructions may be given. Upon the timely receipt of written instructions of a Holder on the ADS Record Date of voting instructions in the manner specified by the Depositary, the Depositary shall endeavor, insofar as practicable and permitted under applicable law, the provisions of this Deposit Agreement, the Company’s constituent documents and the provisions of or governing the Deposited Securities, to vote or cause the Custodian to vote the Shares and/or other Deposited Securities (in person or by proxy) represented by American Depositary Shares evidenced by such Receipt in accordance with such voting instructions. Voting instructions may be given only in respect of a number of American Depositary Shares representing an integral number of Shares or other Deposited Securities.

Until such time as the Company’s Articles of Association permit pass-through voting of the ADSs, a precondition for exercising any such voting rights is that such Holder is registered in the register of shareholders of the Company not less than ten calendar days prior to the date of the meeting and gives the Company notice of its intention to attend the meeting, in person or by proxy, not later than a date (being not earlier than five calendar days before the meeting) specified in the notice convening the meeting. Pursuant to these requirements, Holders of record will be entitled to deposit their ADSs in a blocked account with the Depositary and to instruct the Depositary to request a Custodian to cause the equivalent underlying Shares or other Deposited Securities to be registered in a Holder’s name and to give notice to the Company of a Holder’s intention to vote the Shares or other Deposited Securities at such a meeting in person. Such notice shall also contain a statement that a Holder who deposits ADSs in a blocked account with the Depositary and who instructs a Custodian to register in the Holder’s name the equivalent underlying Shares or other Deposited Securities for the purpose of voting such Shares or other Deposited Securities at any meeting of holders of Shares or other Deposited Securities may instruct the Depositary, immediately following any such meeting, to request such Custodian to reregister the Shares or other Deposited Securities in the name in which such Shares or other Deposited Securities were previously registered and to release to the Holder from the blocked account the ADRs evidencing ADSs representing such Shares or other Deposited Securities.

Neither the Depositary nor the Custodian shall, under any circumstances exercise any discretion as to voting, and neither the Depositary nor the Custodian shall vote, attempt to exercise the right to vote, or in any way make use of for purposes of establishing a quorum or otherwise, the Shares or other Deposited Securities represented by American Depositary Shares except pursuant to and in accordance with such written instructions from Holders. Shares or other Deposited Securities represented by ADSs for which no specific voting instructions are received by the Depositary from the Holder shall not be voted.

Notwithstanding the above, save for applicable provisions of Danish law, and in accordance with the terms of Section 5.3, the Depositary shall not be liable for any failure to carry out any instructions to vote any of the Deposited Securities or the manner in which such vote is cast or the effect of any such vote.

There can be no assurance that Holders or Beneficial Owners generally or any Holder or Beneficial Owner in particular will receive the notice described above with sufficient time to enable the Holder to return voting instructions to the Depositary in a timely manner.

SECTION 4.9 Changes Affecting Deposited Securities. Upon any change in par value, split-up, subdivision cancellation, consolidation or any other reclassification of Deposited Securities, or upon any recapitalization, reorganization, merger, amalgamation or consolidation or sale of assets affecting the Company or to which it is otherwise a party, any securities which shall be received by the Depositary or the Custodian in exchange for, or in conversion of or replacement or otherwise in respect of, such Deposited Securities shall, to the extent permitted by law, be treated as new Deposited Securities under this Deposit Agreement, and the Receipts shall, subject to the provisions of this Deposit Agreement and applicable law, evidence American Depositary Shares representing the right to receive such additional securities. Alternatively, the Depositary may, with the Company’s prior approval (which approval shall not be unreasonably withheld), and shall, if the Company shall so request, subject to the terms of the Deposit Agreement and receipt of an opinion of counsel to the Company, furnished at the expense of the Company, satisfactory to the Depositary that such distributions are not in violation of any applicable laws or regulations, execute and Deliver additional Receipts as in the case of a stock dividend on the Shares, or call for the surrender of outstanding Receipts to be exchanged for new Receipts, in either case, as well as in the event of newly deposited Shares, with necessary modifications to the form of Receipt contained in Exhibit A hereto, specifically describing such new Deposited Securities and/or corporate change. Subject to the foregoing, The Company agrees to, jointly with the Depositary, amend the Registration Statement on Form F-6 as filed with the Commission to permit the issuance of such new form of Receipt. Notwithstanding the foregoing, in the event that any security so received may not be lawfully distributed to some or all Holders, the Depositary may, with the Company’s prior approval (which approval shall not be unreasonably withheld), and shall, if the Company requests, subject to receipt of an opinion of counsel to the Company, furnished at the expense of the Company, satisfactory to the Depositary that such action is not in violation of any applicable laws or regulations, sell such securities at public or private sale, at such place or places and upon such terms as it may deem proper and may allocate the net proceeds of such sales (net of (a) fees and charges of, and expenses incurred by, the Depositary and (b) taxes and/or governmental charges) for the account of the Holders

otherwise entitled to such securities upon an averaged or other practicable basis without regard to any distinctions among such Holders and distribute the net proceeds so allocated to the extent practicable as in the case of a distribution received in cash pursuant to Section 4.1. The Depositary shall not be responsible for, and the Company shall not be liable to Holders or Beneficial Owners for, (i) any failure to determine that it may be lawful or feasible to make such securities available to Holders in general or to any Holder in particular, (ii) any foreign exchange exposure or loss incurred in connection with such sale, or (iii) any liability to the purchaser of such securities.

SECTION 4.10 Available Information. As of the date of the Deposit Agreement, the Company publishes information in English required to maintain the exemption from registration under Rule 12g3-2(b) under the Exchange Act on its Internet Web site (http://www.bavarian-nordic.com) or through an electronic information delivery system generally available to the public in its primary trading market. Should the Company become subject to the periodic reporting or other informational requirements under the Exchange Act, it will be required in accordance therewith to file reports and other information with the Commission. The Depositary does not assume any duty to determine if the Company is complying with the current requirements of Rule 12g3-2(b) under the Exchange Act or to take any action if the Company is not complying with those requirements.

The Company represents that as of the date of this Deposit Agreement, the statements in this Section 4.10 and in Article (12) of the Receipts with respect to the exemption from registration under Rule 12g3-2(b) under the Exchange Act are true and correct. The Company agrees to promptly notify the Depositary and all Holders in the event of any change in the truth of any such statements.

As of the date of the effectiveness of the Company’s Registration Statement on Form 8-A, the Company will be subject to the periodic reporting requirements of the Exchange Act and accordingly file certain information with the Commission, which reports and documents may be inspected and copied through the Commission’s EDGAR system or at public reference facilities maintained by the Commission located at the date of this Deposit Agreement at 100 F Street, N.E., Washington, D.C. 20549.

SECTION 4.11 Reports. The Depositary shall make available during normal business hours on any Business Day for inspection by Holders at its Principal Office any reports and communications, including any proxy soliciting materials, received from the Company which are both (a) received by the Depositary, the Custodian, or the nominee of either of them as the holder of the Deposited Securities and (b) made generally available to the holders of such Deposited Securities by the Company. The Company agrees to provide to the Depositary, at the Company’s expense, all documents that it provides to the Custodian. The Depositary shall, at the expense of the Company and in accordance with Section 5.6, also mail by regular, ordinary mail delivery or by electronic transmission (if agreed by the Company and the Depositary) and unless otherwise agreed in writing by the Company and the Depositary, to Holders copies of such reports when furnished by the Company pursuant to Section 5.6.

SECTION 4.12 List of Holders. Promptly upon written request by the Company, the Depositary shall, at the expense of the Company, furnish to it a list, as of a recent date, of the names, addresses and holdings of American Depositary Shares by all persons in whose names Receipts are registered on the books of the Depositary.

SECTION 4.13 Taxation; Withholding. The Depositary will, and will instruct the Custodian to, forward to the Company or its agents such information from its records as the Company may reasonably request to enable the Company or its agents to file necessary tax reports with governmental authorities or agencies. The Depositary, the Custodian or the Company and its agents may, but shall not be obligated to, file such reports as are necessary to reduce or eliminate applicable taxes on dividends and on other distributions in respect of Deposited Securities under applicable tax treaties or laws for the Holders and Beneficial Owners. Holders and Beneficial Owners of American Depositary Shares may be required from time to time, and in a timely manner, to file such proof of taxpayer status, residence and beneficial ownership (as applicable), to execute such certificates and to make such representations and warranties, or to provide any other information or documents, as the Depositary or the Custodian may deem necessary or proper to fulfill the Depositary’s or the Custodian’s obligations under applicable law.

The Company shall remit to the appropriate governmental authority or agency any amounts required to be withheld by the Company and owing to such governmental authority or agency. Upon any such withholding, the Company shall remit to the Depositary information about such taxes and/or governmental charges withheld or paid, and, if so requested, the tax receipt (or other proof of payment to the applicable governmental authority) therefor, in each case, in a form satisfactory to the Depositary. The Depositary shall, to the extent required by U.S. law, report to Holders: (i) any taxes withheld by it; (ii) any taxes withheld by the Custodian, subject to information being provided to the Depositary by the Custodian; and (iii) any taxes withheld by the Company, subject to information being provided to the Depositary by the Company. The Depositary and the Custodian shall not be required to provide the Holders with any evidence of the remittance by the Company (or its agents) of any taxes withheld, or of the payment of taxes by the Company, except to the extent the evidence is provided by the Company to the Depositary. Neither the Depositary nor the Custodian shall be liable for the failure by any Holder or Beneficial Owner to obtain the benefits of credits on the basis of non-U.S. tax paid against such Holder’s or Beneficial Owner’s income tax liability. The Company shall not be liable to Holders or Beneficial Owners for the failure by any Holder or Beneficial Owner to obtain the benefits of credits on the basis of non-U.S. tax paid against such Holder’s or Beneficial Owner’s income tax liability.

In the event that the Depositary determines that any distribution in property (including Shares and rights to subscribe therefor) is subject to any tax or other governmental charge which the Depositary is obligated to withhold, the Depositary shall withhold the amount required to be withheld and may by public or private sale dispose of all or a portion of such property (including Shares and rights to subscribe therefor) in such amounts and in such manner as the Depositary deems necessary and practicable to pay such taxes and charges and the Depositary shall distribute

the net proceeds of any such sale after deduction of such taxes and charges to the Holders entitled thereto in proportion to the number of American Depositary Shares held by them respectively.

The Depositary is under no obligation to provide the Holders and Beneficial Owners with any information about the tax status of the Company. The Depositary shall not incur any liability for any tax consequences that may be incurred by Holders and Beneficial Owners on account of their ownership of the American Depositary Shares, including without limitation, tax consequences resulting from the Company (or any of its subsidiaries) being treated as a “Passive Foreign Investment Company” (as defined in the U.S. Internal Revenue Code and the regulations issued thereunder) or otherwise.

ARTICLE V

THE DEPOSITARY, THE CUSTODIAN AND THE COMPANY

SECTION 5.1 Maintenance of Office and Transfer Books by the Registrar. Until termination of this Deposit Agreement in accordance with its terms, the Depositary or if a Registrar for the Receipts shall have been appointed, the Registrar shall maintain in the Borough of Manhattan, the City of New York, an office and facilities for the execution and delivery, registration, registration of transfers, combination and split-up of Receipts, the surrender of Receipts and the delivery and withdrawal of Deposited Securities in accordance with the provisions of this Deposit Agreement.

The Depositary or the Registrar as applicable, shall keep books for the registration of Receipts and transfers of Receipts which at all reasonable times shall be open for inspection by the Company and by the Holders of such Receipts, provided that such inspection shall not be, to the Depositary’s or the Registrar’s knowledge, for the purpose of communicating with Holders of such Receipts in the interest of a business or object other than the business of the Company or other than a matter related to this Deposit Agreement or the Receipts.

The Depositary or the Registrar, as applicable, may close the transfer books with respect to the Receipts, at any time or from time to time, when deemed necessary or advisable by it in connection with the performance of its duties hereunder.

If any Receipts or the American Depositary Shares evidenced thereby are listed on one or more stock exchanges or automated quotation systems in the United States, the Depositary shall act as Registrar or appoint a Registrar or one or more co-registrars for registration of Receipts and transfers, combinations and split-ups, and to countersign such Receipts in accordance with any requirements of such exchanges or systems. Such Registrar or co-registrars may be removed and a substitute or substitutes appointed by the Depositary.

If any Receipts or the American Depositary Shares evidenced thereby are listed on one or more securities exchanges, markets or automated quotation systems, (i) the Depositary shall be entitled to, and shall, take or refrain from taking such action(s) as it may deem necessary or appropriate to comply with the requirements of such securities exchange(s), market(s) or

automated quotation system(s) applicable to it, notwithstanding any other provision of this Deposit Agreement; and (ii) upon the reasonable request of the Depositary, the Company shall provide the Depositary such information and assistance as may be reasonably necessary for the Depositary to comply with such requirements, to the extent that the Company may lawfully do so.

SECTION 5.2 Exoneration. Neither the Depositary, the Custodian or the Company shall be obligated to do or perform any act which is inconsistent with the provisions of this Deposit Agreement or shall incur any liability to Holders, Beneficial Owners or any third parties (i) if the Depositary, the Custodian or the Company or their respective controlling persons or agents (including, without limitation, Agents, in the case of the Depositary) shall be prevented or forbidden from, or subjected to any civil or criminal penalty or restraint on account of, or delayed in, doing or performing any act or thing required by the terms of the Deposit Agreement and any Receipt, by reason of any provision of any present or future law, rule, regulation, fiat, order or decree of the United States or any state thereof, the Kingdom of Denmark or any other country or jurisdiction, or of any other governmental authority or regulatory authority or stock exchange, or on account of the possible criminal or civil penalties or restraint, or by reason of any provision, present or future, of the Company’s constituent documents or any provision of or governing any Deposited Securities, or by reason of any act of God, war, terrorism, nationalization, expropriation, currency restrictions, work stoppage, strike, civil unrest, revolutions, rebellions, explosions, computer failure or circumstance beyond its control, (ii) by reason of any exercise of, or failure to exercise, any discretion provided for in this Deposit Agreement or in the Company’s constituent documents or provisions of or governing Deposited Securities, (iii) for any action or inaction of the Depositary, the Custodian or the Company or their respective controlling persons or agents (including, without limitation, Agents) in reliance upon the advice of or information from legal counsel, accountants, any person presenting Shares for deposit, any Holder, any Beneficial Owner or authorized representative thereof, or any other person believed by it in good faith to be competent to give such advice or information, including, without limitation, in determining if a proposed distribution, action or transaction under Article IV of the Deposit Agreement is lawful, (iv) for the inability by a Holder or Beneficial Owner to benefit from any distribution, offering, right or other benefit which is made available to holders of Deposited Securities but is not, under the terms of this Deposit Agreement, made available to Holders of American Depositary Shares or (v) for any special, consequential, indirect or punitive damages (collectively, “Special Damages”) for any breach of the terms of this Deposit Agreement or otherwise.

The Depositary, its controlling persons, its agents (including, without limitation, Agents), the Custodian and the Company, its controlling persons and its agents may rely and shall be protected in acting upon any written notice, request, opinion or other document believed by it to be genuine and to have been signed or presented by the proper party or parties.

No disclaimer of liability under the Securities Act is intended by any provision of this Deposit Agreement.

SECTION 5.3 Standard of Care. The Company and the Depositary and their respective directors, officers, Affiliates, employees and agents (including, without limitation, Agents) assume no obligation and shall not be subject to any liability under this Deposit Agreement or any Receipts to any Holder(s) or Beneficial Owner(s) or other persons (except for the Company’s and the Depositary’s obligations specifically set forth in Section 5.8), provided, that the Company and the Depositary and their respective directors, officers, Affiliates, employees and agents (including, without limitation, Agents) agree to perform their respective obligations specifically set forth in this Deposit Agreement or the applicable ADRs without gross negligence or willful misconduct.

Without limitation of the foregoing, neither the Depositary, nor the Company, nor any of their respective controlling persons, directors, officers, Affiliates, employees or agents (including, without limitation, Agents), shall be under any obligation to appear in, prosecute or defend any action, suit or other proceeding in respect of any Deposited Securities or in respect of the Receipts, which in its opinion may involve it in expense or liability, unless indemnity satisfactory to it against all expenses (including fees and disbursements of counsel) and liabilities be furnished as often as may be required (and no Custodian shall be under any obligation whatsoever with respect to such proceedings, the responsibility of the Custodian being solely to the Depositary).

In no event shall the Depositary or any of its directors, officers, employees, agents (including, without limitation, its Agents) and/or Affiliates, or any of them, be liable for any indirect, special, punitive or consequential damages to the Company, Holders, Beneficial Owners or any other person.

The Depositary and its agents (including, without limitation, Agents) shall not be liable for any failure to carry out any instructions to vote any of the Deposited Securities, or for the manner in which any vote is cast (provided that any such action or omission is in good faith) or the effects of any vote. The Depositary shall not incur any liability for any failure to determine that any distribution or action may be lawful or reasonably practicable, for the content of any information submitted to it by the Company for distribution to the Holders or for any inaccuracy of any translation thereof, for any investment risk associated with acquiring an interest in the Deposited Securities, for the validity or worth of the Deposited Securities or for any tax consequences that may result from the ownership of ADSs, Shares or Deposited Securities, for the credit-worthiness of any third party, for allowing any rights to lapse upon the terms of this Deposit Agreement or for the failure or timeliness of any notice from the Company, or for any action or non action by it in reliance upon the opinion, advice of or information from legal counsel, accountants, any person presenting Shares for deposit, any Holder or any other person believed by it in good faith to be competent to give such advice or information. The Depositary and its agents (including, without limitation, Agents) shall not be liable for any acts or omissions made by a successor depositary.

SECTION 5.4 Resignation and Removal of the Depositary; Appointment of Successor Depositary. The Depositary may at any time resign as Depositary hereunder by written notice of resignation delivered to the Company, such resignation to be effective on the earlier of

(i) the 90th day after delivery thereof to the Company (whereupon the Depositary shall, in the event no successor depositary has been appointed by the Company, be entitled to take the actions contemplated in Section 6.2 hereof), or (ii) upon the appointment by the Company of a successor depositary and its acceptance of such appointment as hereinafter provided, save that, any amounts, fees, costs or expenses owed to the Depositary hereunder or in accordance with any other agreements otherwise agreed in writing between the Company and the Depositary from time to time shall be paid to the Depositary prior to such resignation.

The Depositary may at any time be removed by the Company by written notice of such removal, which removal shall be effective on the later of (i) the 90th day after delivery thereof to the Depositary (whereupon the Depositary shall be entitled to take the actions contemplated in Section 6.2 hereof), or (ii) upon the appointment by the Company of a successor depositary and its acceptance of such appointment as hereinafter provided, save that, any amounts, fees, costs or expenses owed to the Depositary hereunder or in accordance with any other agreements otherwise agreed in writing between the Company and the Depositary from time to time shall be paid to the Depositary prior to such removal.

In case at any time the Depositary acting hereunder shall resign or be removed, the Company shall use its best efforts to appoint a successor depositary, which shall be a bank or trust company having an office in the Borough of Manhattan, the City of New York. The Company shall give notice to the Depositary of the appointment of a successor depositary not more than 90 days after delivery by the Depositary of written notice of resignation or by the Company of removal, each as provided in this section. In the event that a successor depositary is not appointed or notice of the appointment of a successor depositary is not provided by the Company in accordance with the preceding sentence, the Depositary shall be entitled to take the actions contemplated in Section 6.2 hereof. Every successor depositary shall be required by the Company to execute and deliver to its predecessor and to the Company an instrument in writing accepting its appointment hereunder, and thereupon such successor depositary, without any further act or deed (except as required by applicable law), shall become fully vested with all the rights, powers, duties and obligations of its predecessor. The predecessor depositary, upon payment of all sums due to it and on the written request of the Company, shall (i) execute and deliver an instrument transferring to such successor all rights and powers of such predecessor hereunder (other than as contemplated in Sections 5.8 and 5.9), (ii) duly assign, transfer and deliver all right, title and interest to the Deposited Securities to such successor, and (iii) deliver to such successor a list of the Holders of all outstanding Receipts and such other information relating to Receipts and Holders thereof as the successor may reasonably request. Any such successor depositary shall promptly mail notice of its appointment to such Holders.

Any corporation into or with which the Depositary may be merged or consolidated shall be the successor of the Depositary without the execution or filing of any document or any further act.

SECTION 5.5 The Custodian. The Custodian or its successors in acting hereunder shall be subject at all times and in all respects to the direction of the Depositary for the Deposited Securities for which the Custodian acts as custodian and shall be responsible solely to

it. If any Custodian resigns or is discharged from its duties hereunder with respect to any Deposited Securities and no other Custodian has previously been appointed hereunder, the Depositary shall promptly appoint a substitute custodian. The Depositary shall require such resigning or discharged Custodian to deliver the Deposited Securities held by it, together with all such records maintained by it as Custodian with respect to such Deposited Securities as the Depositary may request, to the Custodian designated by the Depositary. Whenever the Depositary determines, in its discretion, that it is appropriate to do so, it may appoint an additional entity to act as Custodian with respect to any Deposited Securities, or discharge the Custodian with respect to any Deposited Securities and appoint a substitute custodian, which shall thereafter be Custodian hereunder with respect to the Deposited Securities. After any such change, the Depositary shall give notice thereof in writing to all Holders.

Upon the appointment of any successor depositary, any Custodian then acting hereunder shall, unless otherwise instructed by the Depositary, continue to be the Custodian of the Deposited Securities without any further act or writing and shall be subject to the direction of the successor depositary. The successor depositary so appointed shall, nevertheless, on the written request of any Custodian, execute and deliver to such Custodian all such instruments as may be proper to give to such Custodian full and complete power and authority to act on the direction of such successor depositary.

SECTION 5.6 Notices and Reports. On or before the first date on which the Company gives notice, by publication or otherwise, of any meeting of holders of Shares or other Deposited Securities, or of any adjourned meeting of such holders, or of the taking of any action by such holders other than at a meeting, or of the taking of any action in respect of any cash or other distributions or the offering of any rights in respect of Deposited Securities, the Company shall transmit to the Depositary and the Custodian a copy of the notice thereof in English but otherwise in the form given or to be given to holders of Shares or other Deposited Securities. The Company shall also furnish to the Custodian and the Depositary a summary, in English, of any applicable provisions or proposed provisions of the Company’s constituent documents that may be relevant or pertain to such notice of meeting or be the subject of a vote thereat.

The Company will also transmit to the Depositary (a) English language versions of the other notices, reports and communications which are made generally available by the Company to holders of its Shares or other Deposited Securities and (b) English language versions of the Company’s annual and other reports prepared in accordance with the applicable requirements of the Commission. The Depositary shall arrange, at the request of the Company and at the Company’s expense, for the mailing of copies thereof to all Holders, or by any other means as agreed between the Company and the Depositary (at the Company’s expense) or make such notices, reports and other communications available for inspection by all Holders, provided, that, the Depositary shall have received evidence sufficiently satisfactory to it, including in the form of an opinion of local and/or U.S. counsel or counsel of other applicable jurisdiction, furnished at the expense of the Company, as the Depositary in its discretion so requests, that the distribution of such notices, reports and any such other communications to Holders from time to time is valid and does not or will not infringe any local, U.S. or other applicable jurisdiction regulatory restrictions or requirements if so distributed and made available to Holders. The Company will

timely provide the Depositary with the quantity of such notices, reports, and communications, as requested by the Depositary from time to time, in order for the Depositary to effect such mailings. The Company has delivered to the Depositary and the Custodian a copy of the Company’s constituent documents along with the provisions of or governing the Shares and any other Deposited Securities issued by the Company or any Affiliate of the Company, in connection with the Shares, in each case along with a certified English translation thereof, and promptly upon any amendment thereto or change therein, the Company shall deliver to the Depositary and the Custodian a copy of such amendment thereto or change therein (along with a certified English translation thereof). The Depositary may rely upon such copy for all purposes of this Deposit Agreement.

The Depositary will, at the expense of the Company, make available a copy of any such notices, reports or communications issued by the Company and delivered to the Depositary for inspection by the Holders of the Receipts evidencing the American Depositary Shares representing such Shares governed by such provisions at the Depositary’s Principal Office, at the office of the Custodian and at any other designated transfer office.

SECTION 5.7 Issuance of Additional Shares, ADSs etc. The Company agrees that in the event it or any of its Affiliates proposes (i) an issuance, sale or distribution of additional Shares, (ii) an offering of rights to subscribe for Shares or other Deposited Securities, (iii) an issuance of securities convertible into or exchangeable for Shares, (iv) an issuance of rights to subscribe for securities convertible into or exchangeable for Shares, (v) an elective dividend of cash or Shares, (vi) a redemption of Deposited Securities, (vii) a meeting of holders of Deposited Securities, or solicitation of consents or proxies, relating to any reclassification of securities, merger, subdivision, amalgamation or consolidation or transfer of assets or (viii) any reclassification, recapitalization, reorganization, merger, amalgamation, consolidation or sale of assets which affects the Deposited Securities, it will obtain U.S. legal advice and take all steps necessary to ensure that the application of the proposed transaction to Holders and Beneficial Owners does not violate the registration provisions of the Securities Act, or any other applicable laws (including, without limitation, the Investment Company Act of 1940, as amended, the Exchange Act or the securities laws of the states of the United States). In support of the foregoing or at the reasonable request of the Depositary where it deems necessary, the Company will furnish to the Depositary, at its own expense (a) a written opinion of U.S. counsel (reasonably satisfactory to the Depositary) stating whether or not application of such transaction to Holders and Beneficial Owners (1) requires a registration statement under the Securities Act to be in effect or is exempt from the registration requirements of the Securities Act and/or (2) dealing with such other reasonable issues requested by the Depositary, (b) an opinion of Danish counsel (reasonably satisfactory to the Depositary) stating that (1) making the transaction available to Holders and Beneficial Owners does not violate the laws or regulations of the Kingdom of Denmark and (2) all requisite regulatory consents and approvals have been obtained in the Kingdom of Denmark and (c) as the Depositary may reasonably request, a written opinion of counsel in any other jurisdiction in which Holders or Beneficial owners reside to the effect that making the transaction available to such Holders or Beneficial Owners does not violate the laws of such jurisdiction. If the filing of a registration statement is required, the Depositary shall not have any obligation to proceed with the transaction unless it shall have received evidence

reasonably satisfactory to it that such registration statement has been declared effective and that such distribution is in accordance with all applicable laws or regulations. If, being advised by counsel, the Company determines that a transaction is required to be registered under the Securities Act, the Company will either (i) register such transaction to the extent necessary, (ii) alter the terms of the transaction to avoid the registration requirements of the Securities Act or (iii) direct the Depositary to take specific measures, in each case as contemplated in this Deposit Agreement, to prevent such transaction from violating the registration requirements of the Securities Act.

The Company agrees with the Depositary that neither the Company nor any of its Affiliates will at any time (i) deposit any Shares or other Deposited Securities, either upon original issuance or upon a sale of Shares or other Deposited Securities previously issued and reacquired by the Company or by any such Affiliate, or (ii) issue additional Shares, rights to subscribe for such Shares, securities convertible into or exchangeable for Shares or rights to subscribe for such securities, unless such transaction and the securities issuable in such transaction are exempt from registration under the Securities Act or have been registered under the Securities Act (and such registration statement has been declared effective).

Notwithstanding anything else contained in this Deposit Agreement, nothing in this Deposit Agreement shall be deemed to obligate the Company to file any registration statement in respect of any proposed transaction.

SECTION 5.8 Indemnification. The Company agrees to indemnify the Depositary, any Custodian and each of their respective directors, officers, employees, agents (including, without limitation, Agents) and Affiliates against, and hold each of them harmless from, any losses, liabilities, taxes, costs, claims, judgments, proceedings, actions, demands and any charges or expenses of any kind whatsoever (including, but not limited to, reasonable fees and expenses of counsel and, in each case, any value added taxes and any similar taxes charged or otherwise imposed in respect thereof) (collectively referred to as “Losses”) which the Depositary or any agent (including, without limitation, any Agent) thereof may incur or which may be made against it as a result of or in connection with its appointment or the exercise of its powers and duties under this Deposit Agreement or that may arise (a) out of or in connection with any offer, issuance, sale, resale, transfer, deposit or withdrawal of Receipts, American Depositary Shares, the Shares, or other Deposited Securities, as the case may be, (b) out of or in connection with any offering documents in respect thereof or (c) out of or in connection with acts performed or omitted, including, but not limited to, any delivery by the Depositary on behalf of the Company of information regarding the Company in connection with this Deposit Agreement, the Receipts, the American Depositary Shares, the Shares, or any Deposited Securities, in any such case (i) by the Depositary, the Custodian or any of their respective directors, officers, employees, agents (including, without limitation, Agents) and Affiliates, except to the extent any such Losses directly arise out of the gross negligence or willful misconduct of any of them, or (ii) by the Company or any of its directors, officers, employees, agents and Affiliates.

Except as provided in the next succeeding paragraph, the Depositary shall indemnify, defend and hold harmless the Company against any Losses incurred by the Company in respect

of this Deposit Agreement to the extent such loss, liability or expense is due to the gross negligence or willful misconduct of the Depositary or its agents acting in such capacity hereunder.

Notwithstanding any other provision of this Deposit Agreement or any Receipts to the contrary, neither the Company nor the Depositary, nor any of their agents, shall be liable to the other for any Special Damages.

Any person seeking indemnification hereunder (an “Indemnified Person”) shall notify the person from whom it is seeking indemnification (the “Indemnifying Person”) of the commencement of any indemnifiable action or claim promptly after such Indemnified Person becomes aware of such commencement (provided that the failure to make such notification shall not affect such Indemnified Person’s rights to indemnification except to the extent the Indemnifying Person is materially prejudiced by such failure) and shall consult in good faith with the Indemnifying Person as to the conduct of the defense of such action or claim that may give rise to an indemnity hereunder, which defense shall be reasonable under the circumstances. No Indemnified Person shall compromise or settle any action or claim that may give rise to an indemnity hereunder without the consent of the Indemnifying Person, which consent shall not be unreasonably withheld.

The obligations set forth in this Section shall survive the termination of this Deposit Agreement and the succession or substitution of any party hereto.

SECTION 5.9 Fees and Charges of Depositary. The Company, the Holders, the Beneficial Owners, and persons depositing Shares or surrendering ADSs for cancellation and withdrawal of Deposited Securities shall be required to pay to the Depositary the Depositary’s fees and related charges identified as payable by them respectively as provided for under Article (9) of the Receipt. All fees and charges so payable may, at any time and from time to time, be changed by agreement between the Depositary and the Company, but, in the case of fees and charges payable by Holders and Beneficial Owners, only in the manner contemplated in Section 6.1. The Depositary shall provide, without charge, a copy of its latest fee schedule to anyone upon request.

The Depositary and the Company may reach separate agreement in relation to the payment of any additional remuneration to the Depositary in respect of any exceptional duties which the Depositary finds necessary or desirable and agreed by both parties in the performance of its obligations hereunder and in respect of the actual costs and expenses of the Depositary in respect of any notices required to be given to the Holders in accordance with Section 6.1 hereof.

In connection with any payment by the Company to the Depositary:

(i) all fees, taxes, duties, charges, costs and expenses which are payable by the Company shall be paid or be procured to be paid by the Company (and any such amounts which are paid by the Depositary shall be reimbursed to the Depositary by the Company upon demand therefor); and

(ii) such payment shall be subject to all necessary exchange control and other consents and approvals having been obtained. The Company undertakes to use its reasonable endeavours to obtain all necessary approvals that are required to be obtained by it in this connection.

The Company agrees to promptly pay to the Depositary such other expenses, fees and charges and to reimburse the Depositary for such out-of-pocket expenses as the Depositary and the Company may agree to from time to time or as are incurred in accordance herewith. Responsibility for payment of such charges may at any time and from time to time be changed by agreement between the Company and the Depositary. In the discretion of the Depositary, the Depositary shall present its statement for such expenses and fees or charges to the Company upon receipt or payment of any relevant invoice by the Depositary, once every three months, semiannually or annually.

All payments by the Company to the Depositary under this Section 5.9 shall be paid without set-off or counterclaim, and free and clear of and without deduction or withholding for or on account of, any present or future taxes, levies, imports, duties, fees, assessments or other charges of whatever nature, imposed by law, rule, regulation, court, tribunal or by any department, agency or other political subdivision or taxing authority thereof or therein, and all interest, penalties or similar liabilities with respect thereto.

The right of the Depositary to receive payment of fees, charges and expenses as provided above shall survive the termination of this Deposit Agreement. As to any Depositary, upon the resignation or removal of such Depositary as described in Section 5.4 hereof, such right shall extend for those fees, charges and expenses incurred prior to the effectiveness of such resignation or removal.

SECTION 5.10 Restricted Securities Owners. The Company agrees to advise in writing each of the persons or entities who, to the knowledge of the Company, holds Restricted Securities that such Restricted Securities are ineligible for deposit hereunder and, to the extent practicable, shall require each of such persons to represent in writing that such person will not deposit Restricted Securities hereunder. The Company shall inform Holders and Beneficial Owners and the Depositary of any other limitations on ownership of Shares that the Holders and Beneficial Owners may be subject to by reason of the number of American Depositary Shares held under the constituent documents of the Company or applicable Danish law, as such restrictions may be in force from time to time.

ARTICLE VI

AMENDMENT AND TERMINATION

SECTION 6.1 Amendment/Supplement. Subject to the terms and conditions of this Section 6.1 and applicable law, the Receipts outstanding at any time, the provisions of this Deposit Agreement and the form of Receipt attached hereto and to be issued under the terms

hereof may at any time and from time to time be amended or supplemented by written agreement between the Company and the Depositary in any respect which they may deem necessary or desirable without the consent of the Holders or Beneficial Owners. Any amendment or supplement which shall impose or increase any fees or charges (other than charges in connection with foreign exchange control regulations, and taxes and/or other governmental charges, delivery and other such expenses), or which shall otherwise materially prejudice any substantial existing right of Holders or Beneficial Owners, shall not, however, become effective as to outstanding Receipts until 30 days after notice of such amendment or supplement shall have been given to the Holders of outstanding Receipts. Notice of any amendment to the Deposit Agreement or form of Receipts shall not need to describe in detail the specific amendments effectuated thereby, and failure to describe the specific amendments in any such notice shall not render such notice invalid, provided, however, that, in each such case, the notice given to the Holders identifies a means for Holders and Beneficial Owners to retrieve or receive the text of such amendment (i.e., upon retrieval from the Commission’s, the Depositary’s or the Company’s website or upon request from the Depositary). The parties hereto agree that any amendments or supplements which (i) are reasonably necessary (as agreed by the Company and the Depositary) in order for (a) the American Depositary Shares to be registered on Form F-6 under the Securities Act or (b) the American Depositary Shares or the Shares to be traded solely in electronic book-entry form and (ii) do not in either such case impose or increase any fees or charges to be borne by Holders, shall be deemed not to materially prejudice any substantial rights of Holders or Beneficial Owners. Every Holder and Beneficial Owner at the time any amendment or supplement so becomes effective shall be deemed, by continuing to hold such American Depositary Share or Shares, to consent and agree to such amendment or supplement and to be bound by the Deposit Agreement as amended and supplemented thereby. In no event shall any amendment or supplement impair the right of the Holder to surrender such Receipt and receive therefor the Deposited Securities represented thereby, except in order to comply with mandatory provisions of applicable law. Notwithstanding the foregoing, if any governmental body should adopt new laws, rules or regulations which would require amendment or supplement of the Deposit Agreement to ensure compliance therewith, the Company and the Depositary may amend or supplement the Deposit Agreement and the Receipt at any time in accordance with such changed laws, rules or regulations. Such amendment or supplement to the Deposit Agreement in such circumstances may become effective before a notice of such amendment or supplement is given to Holders or within any other period of time as required for compliance with such laws, rules or regulations.

SECTION 6.2 Termination. The Depositary shall, at any time at the written direction of the Company, terminate this Deposit Agreement by mailing notice of such termination to the Holders of all Receipts then outstanding at least 90 days prior to the date fixed in such notice for such termination, provided that, the Depositary shall be reimbursed for any amounts, fees, costs or expenses owed to it in accordance with the terms of this Deposit Agreement and in accordance with any other agreements as otherwise agreed in writing between the Company and the Depositary from time to time, before such termination shall take effect. If 90 days shall have expired after (i) the Depositary shall have delivered to the Company a written notice of its election to resign, or (ii) the Company shall have delivered to the Depositary a written notice of the removal of the Depositary, and in either case a successor depositary shall not have been appointed and accepted its appointment as provided in Section 5.4, the Depositary may

terminate this Deposit Agreement by mailing notice of such termination to the Holders of all Receipts then outstanding at least 30 days prior to the date fixed for such termination. On and after the date of termination of this Deposit Agreement, the Holder will, upon surrender of such Receipt at the Principal Office of the Depositary, upon the payment of the charges of the Depositary for the surrender of Receipts referred to in Section 2.6 and subject to the conditions and restrictions therein set forth, and upon payment of any applicable taxes and/or governmental charges, be entitled to Delivery, to him or upon his order, of the amount of Deposited Securities represented by such Receipt. If any Receipts shall remain outstanding after the date of termination of this Deposit Agreement, the Registrar thereafter shall discontinue the registration of transfers of Receipts, and the Depositary shall suspend the distribution of dividends to the Holders thereof, and shall not give any further notices or perform any further acts under this Deposit Agreement, except that the Depositary shall continue to collect dividends and other distributions pertaining to Deposited Securities, shall sell rights or other property as provided in this Deposit Agreement, and shall continue to Deliver Deposited Securities, subject to the conditions and restrictions set forth in Section 2.6, together with any dividends or other distributions received with respect thereto and the net proceeds of the sale of any rights or other property, in exchange for Receipts surrendered to the Depositary (after deducting, or charging, as the case may be, in each case, the charges of the Depositary for the surrender of a Receipt, any expenses for the account of the Holder in accordance with the terms and conditions of this Deposit Agreement and any applicable taxes and/or governmental charges or assessments). At any time after the expiration of six months from the date of termination of this Deposit Agreement, the Depositary may, subject to applicable law, sell the Deposited Securities then held hereunder and may thereafter hold uninvested the net proceeds of any such sale, together with any other cash then held by it hereunder, in an unsegregated account, without liability for interest for the pro rata benefit of the Holders of Receipts whose Receipts have not theretofore been surrendered. After making such sale, the Depositary shall be discharged from all obligations under this Deposit Agreement with respect to the Receipts and the Shares, Deposited Securities and American Depositary Shares, except to account for such net proceeds and other cash (after deducting, or charging, as the case may be, in each case, the charges of the Depositary for the surrender of a Receipt, any expenses for the account of the Holder in accordance with the terms and conditions of this Deposit Agreement and any applicable taxes and/or governmental charges or assessments). Upon the termination of this Deposit Agreement, the Company shall be discharged from all obligations under this Deposit Agreement except for its obligations to the Depositary hereunder. The obligations under the terms of the Deposit Agreement and Receipts of Holders and Beneficial Owners of ADSs outstanding as of the effective date of any termination shall survive such effective date of termination and shall be discharged only when the applicable ADSs are presented by their Holders to the Depositary for cancellation under the terms of the Deposit Agreement and the Holders have each satisfied any and all of their obligations hereunder (including, but not limited to, any payment and/or reimbursement obligations which relate to prior to the effective date of termination but which payment and/or reimbursement is claimed after such effective date of termination).

ARTICLE VII

MISCELLANEOUS

SECTION 7.1 Counterparts. This Deposit Agreement may be executed in any number of counterparts, each of which shall be deemed an original, and all of such counterparts together shall constitute one and the same agreement. Copies of this Deposit Agreement shall be maintained with the Depositary and shall be open to inspection by any Holder during business hours.

SECTION 7.2 No Third-Party Beneficiaries. This Deposit Agreement is for the exclusive benefit of the parties hereto (and their successors) and shall not be deemed to give any legal or equitable right, remedy or claim whatsoever to any other person, except to the extent specifically set forth in this Deposit Agreement. Nothing in this Deposit Agreement shall be deemed to give rise to a partnership or joint venture among the parties hereto nor establish a fiduciary or similar relationship among the parties. The parties hereto acknowledge and agree that (i) the Depositary and its Affiliates may at any time have multiple banking relationships with the Company and its Affiliates, (ii) the Depositary and its Affiliates may be engaged at any time in transactions in which parties adverse to the Company or the Holders or Beneficial Owners may have interests and (iii) nothing contained in this Deposit Agreement shall (a) preclude the Depositary or any of its Affiliates from engaging in such transactions or establishing or maintaining such relationships, or (b) obligate the Depositary or any of its Affiliates to disclose such transactions or relationships or to account for any profit made or payment received in such transactions or relationships.

SECTION 7.3 Severability. In case any one or more of the provisions contained in this Deposit Agreement or in the Receipts should be or become invalid, illegal or unenforceable in any respect, the validity, legality and enforceability of the remaining provisions contained herein or therein shall in no way be affected, prejudiced or disturbed thereby.

SECTION 7.4 Holders and Beneficial Owners as Parties; Binding Effect. The Holders and Beneficial Owners from time to time of American Depositary Shares shall be parties to the Deposit Agreement and shall be bound by all of the terms and conditions hereof and of any Receipt by acceptance hereof or any beneficial interest therein.

SECTION 7.5 Notices. Any and all notices to be given to the Company shall be deemed to have been duly given if personally delivered or sent by mail, air courier or cable, telex, facsimile transmission or electronic transmission, confirmed by letter, addressed to Bavarian Nordic A/S, Hejreskovvej 10A, DK-3490 Kvistgaard, Denmark, Attention: President and CEO, or to any other address which the Company may specify in writing to the Depositary.

Any and all notices to be given to the Depositary shall be deemed to have been duly given if personally delivered or sent by mail, air courier or cable, telex, facsimile transmission or by electronic transmission (if agreed by the Company and the Depositary), at the Company’s expense, unless otherwise agreed in writing between the Company and the Depositary, confirmed by letter, addressed to Deutsche Bank Trust Company Americas, 60 Wall Street, New York, New York 10005, USA Attention: ADR Department, telephone: (001) 212 250-9100, facsimile: (001) 732 544 6346 or to any other address which the Depositary may specify in writing to the Company.

Any and all notices to be given to any Holder shall be deemed to have been duly given if personally delivered or sent by mail or cable, telex, facsimile transmission or by electronic transmission (if agreed by the Company and the Depositary), at the Company’s expense, unless otherwise agreed in writing between the Company and the Depositary, addressed to such Holder at the address of such Holder as it appears on the transfer books for Receipts of the Depositary, or, if such Holder shall have filed with the Depositary a written request that notices intended for such Holder be mailed to some other address, at the address specified in such request. Notice to Holders shall be deemed to be notice to Beneficial Owners for all purposes of this Deposit Agreement.

Delivery of a notice sent by mail, air courier or cable, telex, facsimile or electronic transmission shall be deemed to be effective at the time when a duly addressed letter containing the same (or a confirmation thereof in the case of a cable, telex, facsimile or electronic transmission) is deposited, postage prepaid, in a post-office letter box or delivered to an air courier service. The Depositary or the Company may, however, act upon any cable, telex, facsimile or electronic transmission received by it from the other or from any Holder, notwithstanding that such cable, telex, facsimile or electronic transmission shall not subsequently be confirmed by letter as aforesaid, as the case may be.

SECTION 7.6 Governing Law and Jurisdiction. This Deposit Agreement and the Receipts shall be interpreted in accordance with, and all rights hereunder and thereunder and provisions hereof and thereof shall be governed by, the laws of the State of New York without reference to the principles of choice of law thereof. Subject to the Depositary’s rights under the third paragraph of this Section 7.6, the Company and the Depositary agree that the federal or state courts in the City of New York shall have exclusive jurisdiction to hear and determine any suit, action or proceeding and to settle any dispute between them that may arise out of or in connection with this Deposit Agreement and, for such purposes, each irrevocably submits to the exclusive jurisdiction of such courts. Notwithstanding the above, the parties hereto agree that any judgment and/or order from any such New York court may be enforced in any court having jurisdiction thereover. The Company hereby irrevocably designates, appoints and empowers Bavarian Nordic Inc. (the “Process Agent”) now at 595 Penobscot Drive, Redwood City, CA 94063, USA, as its authorized agent to receive and accept for and on its behalf, and on behalf of its properties, assets and revenues, service by mail of any and all legal process, summons, notices and documents that may be served in any suit, action or proceeding brought against the Company in any federal or state court as described in the preceding sentence or in the next paragraph of this Section 7.6. If for any reason the Process Agent shall cease to be available to act as such, the Company agrees to designate a new agent in the City of New York on the terms and for the purposes of this Section 7.6 reasonably satisfactory to the Depositary. The Company further hereby irrevocably consents and agrees to the service of any and all legal process, summons, notices and documents in any suit, action or proceeding against the Company, by service by mail of a copy thereof upon the Process Agent (whether or not the appointment of such Process Agent shall for any reason prove to be ineffective or such Process Agent shall fail to accept or acknowledge such service), with a copy mailed to the Company by registered or certified air mail, postage prepaid, to its address provided in Section 7.5 hereof. The Company agrees that the

failure of the Process Agent to give any notice of such service to it shall not impair or affect in any way the validity of such service or any judgment rendered in any action or proceeding based thereon.

The Company irrevocably and unconditionally waives, to the fullest extent permitted by law, any objection that it may now or hereafter have to the laying of venue of any actions, suits or proceedings brought in any court as provided in this Section 7.6, and hereby further irrevocably and unconditionally waives and agrees not to plead or claim in any such court that any such action, suit or proceeding brought in any such court has been brought in an inconvenient forum.

The Company, the Depositary and by holding an American Depositary Share (or interest therein) Holders and Beneficial Owners each agree that, notwithstanding the foregoing and following, with regard to any claim or dispute or difference of whatever nature between or involving the parties hereto arising directly or indirectly from the relationship created by this Deposit Agreement, the Depositary, in its sole discretion, shall be entitled to refer such dispute or difference for final settlement by arbitration (“Arbitration”) in accordance with the Commercial Arbitration Rules of the American Arbitration Association (the “Rules”) then in force The arbitration shall be conducted by three arbitrators, one nominated by the Depositary, one nominated by the Company, and one nominated by the two party-appointed arbitrators within thirty (30) calendar days of the confirmation of the nomination of the second arbitrator. If any arbitrator has not been nominated within the time limits specified herein and in the Rules, then such arbitrator shall be appointed by the American Arbitration Association in accordance with the Rules. Judgment upon the award rendered by the arbitrators may be enforced in any court having jurisdiction thereof. The seat and place of any reference to arbitration shall be New York City, New York, and the procedural law of such arbitration shall be New York law. The language to be used in the arbitration shall be English. The fees of the arbitrator and other costs incurred by the parties in connection with such Arbitration shall be paid by the party or parties that is (are) unsuccessful in such Arbitration.

Holders and Beneficial Owners understand, and holding an American Depositary Share or an interest therein, such Holders and Beneficial Owners each irrevocably agree that any legal suit, action or proceeding against or involving the Company or the Depositary, arising out of or based upon the Deposit Agreement, American Depositary Shares, Receipts or the transactions contemplated hereby or thereby or by virtue of ownership thereof, may only be instituted in a state or federal court in New York, New York, and by holding an American Depositary Share or an interest therein each irrevocably waives any objection which it may now or hereafter have to the laying of venue of any such proceeding, and irrevocably submits to the exclusive jurisdiction of such courts in any such suit, action or proceeding. Holders and Beneficial Owners agree that the provisions of this paragraph shall survive such Holders’ and Beneficial Owners’ ownership of American Depositary Shares or interests therein.

EACH PARTY TO THE DEPOSIT AGREEMENT (INCLUDING, FOR AVOIDANCE OF DOUBT, EACH HOLDER AND BENEFICIAL OWNER AND/OR HOLDER OF INTERESTS IN ADRS) HEREBY IRREVOCABLY WAIVES, TO THE FULLEST EXTENT PERMITTED BY APPLICABLE LAW, ANY RIGHT IT MAY HAVE TO A TRIAL BY JURY

IN ANY SUIT, ACTION OR PROCEEDING AGAINST THE DEPOSITARY AND/OR THE COMPANY DIRECTLY OR INDIRECTLY ARISING OUT OF OR RELATING TO THE SHARES OR OTHER DEPOSITED SECURITIES, THE ADSs OR THE ADRs, THE DEPOSIT AGREEMENT OR ANY TRANSACTION CONTEMPLATED HEREIN OR THEREIN, OR THE BREACH HEREOF OR THEREOF (WHETHER BASED ON CONTRACT, TORT, COMMON LAW OR ANY OTHER THEORY).

The provisions of this Section 7.6 shall survive any termination of this Deposit Agreement, in whole or in part.

SECTION 7.7 Assignment. Subject to the provisions of Section 5.4 hereof, this Deposit Agreement may not be assigned by either the Company or the Depositary.

SECTION 7.8 Compliance with U.S. Securities Laws. Notwithstanding anything in this Deposit Agreement to the contrary, the withdrawal or Delivery of Deposited Securities will not be suspended by the Company or the Depositary except as would be permitted by Instruction I.A.(1) of the General Instructions to Form F-6 Registration Statement, as amended from time to time, under the Securities Act.

SECTION 7.9 Titles; References. All references in this Deposit Agreement to exhibits, articles, sections, subsections, and other subdivisions refer to the exhibits, articles, sections, subsections and other subdivisions of this Deposit Agreement unless expressly provided otherwise. The words “this Deposit Agreement”, “herein”, “hereof”, “hereby”, “hereunder”, and words of similar import refer to the Deposit Agreement as a whole as in effect between the Company, the Depositary and the Holders and Beneficial Owners of ADSs and not to any particular subdivision unless expressly so limited. Pronouns in masculine, feminine and neuter gender shall be construed to include any other gender, and words in the singular form shall be construed to include the plural and vice versa unless the context otherwise requires. Titles to sections of this Deposit Agreement are included for convenience only and shall be disregarded in construing the language contained in this Deposit Agreement. References herein to the laws of the Kingdom of Denmark shall include references to the laws, rules and regulations of the Kingdom of Denmark and any and all communities, provinces and states thereof.

SECTION 7.10 Agents. The Depositary shall be entitled, in its sole but reasonable discretion, to appoint one or more agents (the “Agents”) for the purpose, inter alia, of making distributions to the Holders or otherwise carrying out its obligations under this Deposit Agreement. In connection with the sale of securities, including, without limitation, Deposited Securities, the Depositary shall not have any liability for the price received in connection with any such sale, the timing thereof or any delay in action or omission to act nor shall it be responsible for any error or delay in action, omission to act, default or negligence on the part of the party so retained in connection with any such sale or proposed sale.

SECTION 7.11 Exclusivity. The Company agrees not to appoint any other depositary for the issuance or administration of depositary receipts evidencing any class of stock

IN WITNESS WHEREOF, BAVARIAN NORDIC A/S and DEUTSCHE BANK TRUST COMPANY AMERICAS have duly executed this Deposit Agreement as of the day and year first above set forth and all Holders and Beneficial Owners shall become parties hereto upon acceptance by them of American Depositary Shares evidenced by Receipts issued in accordance with the terms hereof.

	BAVARIAN NORDIC A/S


	By:	/s/ Paul Chaplin
	Name:	Paul Chaplin
	Title:	President & Chief Executive Officer


	By:	/s/ Gerard van Odijk
	Name:	Gerard van Odijk
	Title:	Chairman of the Board of Directors

	DEUTSCHE BANK TRUST COMPANY AMERICAS


	By:	/s/ Michael Fitzpatrick
	Name:	Michael Fitzpatrick
	Title:	Vice President


	By:	/s/ Michael Curran
	Name:	Michael Curran
	Title:	Vice President

Number

CUSIP

		American Depositary Shares (Each
		American Depositary Share
		representing [one-third of] one Fully
		Paid
		Ordinary Share)

EXHIBIT A

[FORM OF FACE OF RECEIPT]

AMERICAN DEPOSITARY RECEIPT

FOR

AMERICAN DEPOSITARY SHARES

representing

DEPOSITED ORDINARY SHARES

BAVARIAN NORDIC A/S

(Incorporated under the laws of the Kingdom of Denmark)

DEUTSCHE BANK TRUST COMPANY AMERICAS, as depositary (herein called the “Depositary”), hereby certifies that is the owner of American Depositary Shares (hereinafter “ADSs” or “American Depositary Shares”), representing deposited ordinary shares, including evidence of rights to receive such ordinary shares, (the “Shares”) of Bavarian Nordic A/S (the “Company”), a company incorporated under the laws of the Kingdom of Denmark. As of the date of the Deposit Agreement (hereinafter referred to), each ADS represents [one-third of] one Share deposited under the Deposit Agreement with the Custodian which at the date of execution of the Deposit Agreement is Danske Bank A/S (the “Custodian”). The ratio of ADSs to Shares is subject to subsequent amendment as provided in Articles IV and VI of the Deposit Agreement. The Depositary’s Principal Office is located at 60 Wall Street, New York, New York 10005, U.S.A.

(1) The Deposit Agreement. This American Depositary Receipt is one of an issue of American Depositary Receipts (“Receipts”), all issued and to be issued upon the terms and conditions set forth in the Amended and Restated Deposit Agreement, dated as of January 5, 2016 (as amended from time to time, the “Deposit Agreement”), by and among the Company, the Depositary, and all Holders and Beneficial Owners from time to time of Receipts issued

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thereunder, each of whom by accepting a Receipt agrees to become a party thereto and becomes bound by all the terms and conditions thereof. The Deposit Agreement sets forth the rights and obligations of Holders and Beneficial Owners of Receipts and the rights and duties of the Depositary in respect of the Shares deposited thereunder and any and all other securities, property and cash from time to time, received in respect of such Shares and held thereunder (such Shares, other securities, property and cash are herein called “Deposited Securities”). Copies of the Deposit Agreement are on file at the Principal Office of the Depositary and the Custodian.

Each owner and each Beneficial Owner, upon acceptance of any ADSs (or any interest therein) issued in accordance with the terms and conditions of the Deposit Agreement, shall be deemed for all purposes to (a) be a party to and bound by the terms of the Deposit Agreement and applicable ADR(s), and (b) appoint the Depositary its attorney-in-fact, with full power to delegate, to act on its behalf and to take any and all actions contemplated in the Deposit Agreement and applicable ADR(s), to adopt any and all procedures necessary to comply with applicable law and to take such action as the Depositary in its sole discretion may deem necessary or appropriate to carry out the purposes of the Deposit Agreement and the applicable ADR(s), the taking of such actions to be the conclusive determinant of the necessity and appropriateness thereof.

The statements made on the face and reverse of this Receipt are summaries of certain provisions of the Deposit Agreement and the Company’s constituent documents (as in effect on the date of the Deposit Agreement) and are qualified by and subject to the detailed provisions of the Deposit Agreement, to which reference is hereby made. All capitalized terms used herein which are not otherwise defined herein shall have the meanings ascribed thereto in the Deposit Agreement. To the extent there is any inconsistency between the terms of this Receipt and the terms of the Deposit Agreement, the terms of the Deposit Agreement shall prevail. Prospective and actual Holders and Beneficial Owners are encouraged to read the terms of the Deposit Agreement. The Depositary makes no representation or warranty as to the validity or worth of the Deposited Securities. The Depositary has made arrangements for the acceptance of the ADSs into DTC. Each Beneficial Owner of ADSs held through DTC must rely on the procedures of DTC and the DTC Participants to exercise and be entitled to any rights attributable to such ADSs. The Receipt evidencing the ADSs held through DTC will be registered in the name of a nominee of DTC. So long as the ADSs are held through DTC or unless otherwise required by law, ownership of beneficial interests in the Receipt registered in the name of DTC (or its nominee) will be shown on, and transfers of such ownership will be effected only through, records maintained by (i) DTC (or its nominee), or (ii) DTC Participants (or their nominees).

(2) Surrender of Receipts and Withdrawal of Deposited Securities. Upon surrender, at the Principal Office of the Depositary, of ADSs evidenced by this Receipt for the purpose of withdrawal of the Deposited Securities represented thereby, and upon payment of (i) the fees and charges of the Depositary for the making of withdrawals and cancellation of Receipts (as set forth in Article (9) hereof or in Section 5.9 of the Deposit Agreement) and (ii) all applicable taxes and/or governmental charges payable in connection with such surrender and withdrawal, and, subject to the terms and conditions of the Deposit Agreement, the Company’s constituent documents, Section 7.8 of the Deposit Agreement, Article (22) of this Receipt and the provisions

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of or governing the Deposited Securities and other applicable laws, the Holder hereof is entitled to Delivery, to him or upon his order, of the Deposited Securities represented by the ADS so surrendered. ADSs may be surrendered for the purpose of withdrawing Deposited Securities by Delivery of a Receipt evidencing such ADSs (if held in certificated form) or by book-entry delivery of such ADSs to the Depositary.

A Receipt surrendered for such purposes shall, if so required by the Depositary, be properly endorsed in blank or accompanied by proper instruments of transfer in blank, and if the Depositary so requires, the Holder thereof shall execute and deliver to the Depositary a written order directing the Depositary to cause the Deposited Securities being withdrawn to be Delivered to or upon the written order of a person or persons designated in such order. Thereupon, the Depositary shall direct the Custodian to Deliver (without unreasonable delay) at the designated office of the Custodian or through book entry delivery of the Shares (in either case subject to the terms and conditions of the Deposit Agreement, to the Company’s constituent documents, and to the provisions of or governing the Deposited Securities and applicable laws, now or hereafter in effect) or through a book entry Delivery of the Shares, to or upon the written order of the person or persons designated in the order delivered to the Depositary as provided above, the Deposited Securities represented by such ADSs, together with any certificate or other proper documents of or relating to title for the Deposited Securities as may be legally required, as the case may be, to or for the account of such person.

The Depositary may, in its discretion, refuse to accept for surrender a number of ADSs representing a number of Shares other than a whole number of Shares. In the case of surrender of a Receipt evidencing a number of ADSs representing other than a whole number of Shares, the Depositary shall cause ownership of the appropriate whole number of Shares to be Delivered in accordance with the terms hereof, and shall, at the discretion of the Depositary, either (i) issue and Deliver to the person surrendering such Receipt a new Receipt evidencing ADSs representing any remaining fractional Share, or (ii) sell or cause to be sold the fractional Shares represented by the Receipt so surrendered and remit the proceeds thereof (net of (a) applicable fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) to the person surrendering the Receipt. At the request, risk and expense of any Holder so surrendering a Receipt, and for the account of such Holder, the Depositary shall direct the Custodian to forward (to the extent permitted by law) any cash or other property (other than securities) held in respect of, and any certificate or certificates and other proper documents of or relating to title to, the Deposited Securities represented by such Receipt to the Depositary for Delivery at the Principal Office of the Depositary, and for further Delivery to such Holder. Such direction shall be given by letter or, at the request, risk and expense of such Holder, by cable, telex, electronic or facsimile transmission. Upon receipt by the Depositary, the Depositary may make delivery to such person or persons at the Principal Office of the Depositary of any dividends or distributions with respect to the Deposited Securities represented by such Receipt, or of any proceeds of sale of any dividends, distributions or rights, which may at the time be held by the Depositary.

(3) Transfers, Split-Ups and Combinations of Receipts. Subject to the terms and conditions of the Deposit Agreement, the Depositary or, if a Registrar (other than the Depositary)

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for the Receipts shall have been appointed, the Registrar shall register transfers of Receipts on its books, upon surrender at the Principal Office of the Depositary of a Receipt by the Holder thereof in person or by duly authorized attorney, properly endorsed (in the case of a certificated Receipt) or accompanied by, or in the case of DRS/Profile Receipts receipt by the Depositary of, proper instruments of transfer (including signature guarantees in accordance with standard industry practice) and duly stamped as may be required by the laws of the State of New York and of the United States of America and of any other applicable jurisdiction. Subject to the terms and conditions of the Deposit Agreement, including payment of the applicable fees and charges of the Depositary, the Depositary shall execute a new Receipt or Receipts (and, if necessary, cause the Registrar to countersign such Receipt(s)) and deliver the same to or upon the order of the person entitled to such Receipts evidencing the same aggregate number of ADSs as those evidenced by the Receipts surrendered. Upon surrender of a Receipt or Receipts for the purpose of effecting a split-up or combination of such Receipt or Receipts upon payment of the applicable fees and charges of the Depositary, and subject to the terms and conditions of the Deposit Agreement, the Depositary shall execute and deliver a new Receipt or Receipts for any authorized number of ADSs requested, evidencing the same aggregate number of ADSs as the Receipt or Receipts surrendered.

(4) Pre-Conditions to Registration, Transfer, Etc. As a condition precedent to the execution and delivery, registration, registration of transfer, split-up, subdivision combination or surrender of any Receipt, the delivery of any distribution thereon or withdrawal of any Deposited Securities, the Depositary or the Custodian may require (i) payment from the depositor of Shares or presenter of the Receipt of a sum sufficient to reimburse it for any tax or other governmental charge and any stock transfer or registration fee with respect thereto (including any such tax or charge and fee with respect to Shares being deposited or withdrawn) and payment of any applicable fees and charges of the Depositary as provided in the Deposit Agreement and in this Receipt, (ii) the production of proof satisfactory to it as to the identity and genuineness of any signature or any other matters contemplated in the Deposit Agreement and (iii) compliance with (A) any laws or governmental regulations relating to the execution and delivery of Receipts and ADSs or to the withdrawal or delivery of Deposited Securities and (B) such reasonable regulations as the Depositary may establish consistent with the Deposit Agreement and applicable law.

The issuance of ADSs against deposits of Shares generally or against deposits of particular Shares may be suspended, or the issuance of ADSs against the deposit of particular Shares may be withheld, or the registration of transfer of Receipts in particular instances may be refused, or the registration of transfer of Receipts generally may be suspended, during any period when the transfer books of the Depositary are closed or if any such action is deemed necessary or advisable by the Depositary or the Company, in good faith, at any time or from time to time because of any requirement of law, any government or governmental body or commission or any securities exchange upon which the Receipts or Shares are listed, or under any provision of the Deposit Agreement or provisions of, or governing, the Deposited Securities or any meeting of shareholders of the Company or for any other reason, subject in all cases to Article (22) hereof.

A-4

(5) Compliance With Information Requests. Notwithstanding any other provision of the Deposit Agreement, this Receipt, the constituent documents of the Company and applicable law, each Holder and Beneficial Owner agrees to (a) provide such information as the Company or the Depositary may request pursuant to law (including, without limitation, relevant Danish law, any applicable law of the United States, the constituent documents of the Company, any resolutions of the Company’s Board of Directors adopted pursuant to such constituent documents, the requirements of any markets or exchanges upon which the Shares, ADSs or Receipts are listed or traded, or to any requirements of any electronic book-entry system by which the ADSs or Receipts may be transferred) regarding the capacity in which they own or owned Receipts, the identity of any other persons then or previously interested in such Receipts and the nature of such interest, and any other applicable matters, and (b) be bound by and subject to applicable provisions of the laws of the Kingdom of Denmark, the constituent documents of the Company and the requirements of any markets or exchanges upon which the ADSs, Receipts or Shares are listed or traded, or pursuant to any requirements of any electronic book-entry system by which the ADSs, Receipts or Shares may be transferred, to the same extent as if such Holder and Beneficial Owner held Shares directly, in each case irrespective of whether or not they are Holders or Beneficial Owners at the time such request is made and (c) without limiting the generality of the foregoing, comply with all applicable provisions of Danish law, the rules and requirements of any stock exchange on which the Shares are, or will be registered, traded or listed and the Company’s constituent documents regarding any such Holder or Beneficial Owner’s interest in Shares (including the aggregate of ADSs and Shares held by each such Holder or Beneficial Owner) and/or the disclosure of interests therein, whether or not the same may be enforceable against such Holder or Beneficial Owner. Each Holder and Beneficial Owner of ADSs further agrees to furnish the Company and the Depositary with any such notification made in accordance with this Article (5) and the Deposit Agreement and to comply with requests for information from the Company or the Depositary pursuant to the laws of the Kingdom of Denmark, the rules and requirements of any stock exchange on which the Shares are, or will be registered, traded or listed, and the Company’s constituent documents, whether or not they are Holders and/or Beneficial Owners at the time of such request. The Depositary agrees to use its reasonable efforts to forward upon the request of the Company, and at the Company’s expense, any such request from the Company to the Holders and to forward to the Company any such responses to such requests received by the Depositary. The Company reserves the right to instruct Holders to deliver their ADSs for cancellation and withdrawal of the Deposited Securities so as to permit the Company to deal directly with the Holder thereof as a holder of Shares and Holders agree to comply with such instructions. The Depositary agrees to cooperate with the Company in its efforts to inform Holders of the Company’s exercise of its rights under this paragraph and agrees to consult with, and provide reasonable assistance without risk, liability or expense on the part of the Depositary, to the Company on the manner or manners in which it may enforce such rights with respect to any Holder.

(6) Liability of Holder for Taxes, Duties and Other Charges. If any present or future tax or other governmental charge shall become payable by the Depositary or the Custodian with respect to any Shares, Deposited Securities, Receipts or ADSs, such tax, or other governmental charge shall be payable by the Holders and Beneficial Owners to the Depositary and such Holders and Beneficial Owners shall be deemed liable therefor. The Company, the Custodian

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and/or the Depositary may withhold or deduct from any distributions made in respect of Deposited Securities and may sell for the account of the Holder and/or Beneficial Owner any or all of the Deposited Securities and apply such distributions and sale proceeds in payment of such taxes (including applicable interest and penalties) or charges, with the Holder and the Beneficial Owner hereof remaining fully liable for any deficiency. In addition to any other remedies available to it, the Depositary and the Custodian may refuse the deposit of Shares, and the Depositary may refuse to issue ADSs, to deliver ADSs, register the transfer, split-up or combination of ADRs and (subject to Article (22) hereof) the withdrawal of Deposited Securities, until payment in full of such tax, charge, penalty or interest is received. Holders and Beneficial Owners of American Depositary Shares may be required from time to time, and in a timely manner, to file such proof of taxpayer status, residence and beneficial ownership (as applicable), to execute such certificates and to make such representations and warranties, or to provide any other information or documents, as the Depositary or the Custodian may deem necessary or proper to fulfill the Depositary’s or the Custodian’s obligations under applicable law.

Holders understand that in converting Foreign Currency, amounts received on conversion are calculated at a rate which may exceed the number of decimal places used by the Depositary to report distribution rates (which in any case will not be less than two decimal places). Any excess amount may be retained by the Depositary as an additional cost of conversion, irrespective of any other fees and expenses payable or owing hereunder and shall not be subject to escheatment.

(7) Representations and Warranties of Depositors. Each person depositing Shares under the Deposit Agreement shall be deemed thereby to represent and warrant that (i) such Shares (and the certificates therefor) are duly authorized, validly issued, fully paid, non-assessable and were legally obtained by such person, (ii) all preemptive (and similar) rights, if any, with respect to such Shares, have been validly waived or exercised, (iii) the person making such deposit is duly authorized so to do, (iv) the Shares presented for deposit are free and clear of any lien, encumbrance, security interest, charge, mortgage or adverse claim and are not, and the ADSs issuable upon such deposit will not be, Restricted Securities and (v) the Shares presented for deposit have not been stripped of any rights or entitlements. Such representations and warranties shall survive the deposit and withdrawal of Shares and the issuance, cancellation and transfer of ADSs. If any such representations or warranties are false in any way, the Company and Depositary shall be authorized, at the cost and expense of the person depositing Shares, to take any and all actions necessary to correct the consequences thereof.

(8) Filing Proofs, Certificates and Other Information. Any person presenting Shares for deposit, any Holder and any Beneficial Owner may be required, and every Holder and Beneficial Owner agrees, from time to time to provide to the Depositary or the Custodian such proof of citizenship or residence, taxpayer status, payment of all applicable taxes or other governmental charges, exchange control approval, legal or beneficial ownership of ADSs and Deposited Securities, compliance with applicable laws and the terms of the Deposit Agreement and the provisions of, or governing, the Deposited Securities or other information, to execute such certifications and to make such representations and warranties, and to provide such other information and documentation, in all cases as the Depositary deems necessary or proper or as the Company may reasonably require by written request to the Depositary consistent with its

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obligations under the Deposit Agreement. The Depositary and the Registrar, as applicable, may withhold the execution or delivery or registration of transfer of any Receipt or the distribution or sale of any dividend or other distribution of rights or of the proceeds thereof or, to the extent not limited by Article (22) hereof or the terms of the Deposit Agreement, the delivery of any Deposited Securities until such proof or other information is filed, or such certifications are executed, or such representations and warranties made, or such other documentation or information is provided, in each case to the Depositary’s and the Company’s satisfaction. The Depositary shall from time to time on the written request advise the Company of the availability of any such proofs, certificates or other information and shall, at the Company’s sole expense, provide or otherwise make available copies thereof to the Company upon written request thereof by the Company, unless such disclosure is prohibited by law. Each Holder and Beneficial Owner agrees to provide any information requested by the Company or the Depositary pursuant to this paragraph. Nothing herein shall obligate the Depositary to (i) obtain any information for the Company if not provided by the Holders or Beneficial Owners or (ii) verify or vouch for the accuracy of the information so provided by the Holders or Beneficial Owners.

(9) Charges of Depositary. The Depositary shall charge the following fees for the services performed under the terms of the Deposit Agreement; provided, however, that no fees shall be payable upon distribution of cash dividends so long as the charging of such fee is prohibited by the exchange, if any, upon which the ADSs are listed:

(i) to any person to whom ADSs are issued or to any person to whom a distribution is made in respect of ADS distributions pursuant to stock dividends or other free distributions of stock, bonus distributions, stock splits or other distributions (except where converted to cash), a fee not in excess of U.S. $ 5.00 per 100 ADSs (or fraction thereof) so issued under the terms of the Deposit Agreement to be determined by the Depositary;

(ii) to any person surrendering ADSs for withdrawal of Deposited Securities or whose ADSs are cancelled or reduced for any other reason including, inter alia, cash distributions made pursuant to a cancellation or withdrawal, a fee of up to U.S. $5.00 per 100 ADSs (or portion thereof) reduced, cancelled or surrendered (as the case may be);

(iii) to any holder of ADSs (including, without limitation, Holders), a fee not in excess of U.S. $ 5.00 per 100 ADSs (or portion thereof) held for the distribution of cash dividends;

(iv) to any holder of ADSs (including, without limitation, Holders), a fee not in excess of U.S. $ 5.00 per 100 ADSs (or portion thereof) held for the distribution of cash entitlements (other than cash dividends) and/or cash proceeds, including proceeds from the sale of rights, securities and other entitlements;

(v) to any holder of ADSs (including, without limitation, Holders), a fee not in excess of U.S. $ 5.00 per 100 ADSs (or portion thereof) issued upon the exercise of rights; and

(vi) for the operation and maintenance costs in administering the ADSs an annual fee not in excess of U.S. $ 5.00 per 100 ADSs (or portion thereof), such fee to be

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assessed against Holders of record as of the date or dates set by the Depositary as it sees fit and collected at the sole discretion of the Depositary by billing such Holders for such fee or by deducting such fee from one or more cash dividends or other cash distributions.

In addition, Holders, Beneficial Owners, persons depositing Shares for deposit and persons surrendering ADSs for cancellation and withdrawal of Deposited Securities will be required to pay the following charges:

(i) taxes (including applicable interest and penalties) and other governmental charges;

(ii) such registration fees as may from time to time be in effect for the registration of Shares or other Deposited Securities with the Foreign Registrar and applicable to transfers of Shares or other Deposited Securities to or from the name of the Custodian, the Depositary or any nominees upon the making of deposits and withdrawals, respectively;

(iii) such cable, telex , facsimile and electronic transmission and delivery expenses as are expressly provided in the Deposit Agreement to be at the expense of the person depositing or withdrawing Shares or Holders and Beneficial Owners of ADSs;

(iv) the expenses, fees and other charges incurred by the Depositary in the conversion of Foreign Currency, including, without limitation, the expenses, fees and other charges imposed by any Affiliate (which may, in its sole discretion, act in a principal capacity in such transaction) that may be utilized in connection therewith;

(v) such fees and expenses as are incurred by the Depositary in connection with compliance with exchange control regulations and other regulatory requirements applicable to Shares, Deposited Securities, ADSs and ADRs;

(vi) the fees and expenses incurred by the Depositary in connection with the delivery of Deposited Securities, including any fees of a central depository for securities in the local market, where applicable; and

(vii) any fees, charges, costs or expenses that may be incurred from time to time by the Depositary and/or any of the Depositary’s agents (including, without limitation, Agents), including the Custodian, and/or agents of the Depositary’s agents (including, without limitation, Agents) in connection with the servicing of Shares, Deposited Securities and/or American Depositary Shares, the sale of securities (including, without limitation, Deposited Securities), the delivery of Deposited Securities or otherwise in connection with the Depositary’s or its Custodian’s compliance with applicable law, rule or regulation (such fees, charges, costs or expenses to be assessed against Holders of record as at the date or dates set by the Depositary as it sees fit and collected at the sole discretion of the Depositary by billing such Holders for such fee or by deducting such fee from one or more cash dividends or other cash distributions).

Any other charges and expenses of the Depositary under the Deposit Agreement will be paid by the Company upon agreement between the Depositary and the Company. The Depositary reserves the right to utilize and retain a division or Affiliate(s) of the Depositary to direct, manage and/or execute any public and/or private sale of securities under the Deposit Agreement

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and to engage in the conversion of Foreign Currency thereunder. It is anticipated that such division and/or Affiliate(s) will charge the Depositary a fee and/or commission in connection with each such transaction, and seek reimbursement of its costs and expenses related thereto. Such fees/commissions, costs and expenses, shall be deducted from amounts distributed and shall not be deemed to be fees of the Depositary under Article (9) of this Receipt or otherwise. All fees and charges may, at any time and from time to time, be changed by agreement between the Depositary and Company but, in the case of fees and charges payable by Holders or Beneficial Owners, only in the manner contemplated by Article (20) of this Receipt.

The Depositary may make payments to the Company and/or may share revenue with the Company derived from fees collected from Holders and Beneficial Owners, upon such terms and conditions as the Company and the Depositary may agree from time to time.

(10) Title to Receipts. It is a condition of this Receipt and every successive Holder and Beneficial Owner of this Receipt by accepting or holding the same consents and agrees, that title to this Receipt (and to each ADS evidenced hereby) is transferable by delivery of the Receipt, provided it has been properly endorsed or accompanied by proper instruments of transfer, such Receipt being a certificated security under the laws of the State of New York. Notwithstanding any notice to the contrary, the Depositary may deem and treat the Holder of this Receipt (that is, the person in whose name this Receipt is registered on the books of the Depositary) as the absolute owner hereof for the purpose of determining the person entitled to distributions of dividends or other distributions or to any notice provided for in the Deposit Agreement and for all other purposes. Neither the Depositary nor the Company shall have any obligation or be subject to any liability under the Deposit Agreement or this Receipt to any holder of this Receipt unless such holder is the Holder of this Receipt registered on the books of the Depositary.

(11) Validity of Receipt. This Receipt shall not be entitled to any benefits under the Deposit Agreement or be valid or obligatory for any purpose, unless this Receipt has been (i) dated, (ii) signed by the manual or facsimile signature of a duly authorized signatory of the Depositary. Receipts bearing the manual or facsimile signature of a duly-authorized signatory of the Depositary who was at any time a proper signatory of the Depositary shall bind the Depositary, notwithstanding the fact that such signatory has ceased to hold such office prior to the execution and delivery of such Receipt by the Depositary or did not hold such office on the date of issuance of such Receipts.

(12) Available Information; Reports; Inspection of Transfer Books. As of the date of the Deposit Agreement, the Company publishes information in English required to maintain the exemption from registration under Rule 12g3-2(b) under the Exchange Act on its Internet Web site (http://www.bavarian-nordic.com) or through an electronic information delivery system generally available to the public in its primary trading market. Should the Company become subject to the periodic reporting or other informational requirements under the Exchange Act, it will be required in accordance therewith to file reports and other information with the U.S. Securities and Exchange Commission. The Depositary does not assume any duty to determine if the Company is complying with the current requirements of Rule 12g3-2(b) under the Exchange Act or to take any action if the Company is not complying with those requirements.

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[FORM OF REVERSE OF RECEIPT]

SUMMARY OF CERTAIN ADDITIONAL PROVISIONS

OF THE DEPOSIT AGREEMENT

(13) Dividends and Distributions in Cash, Shares, etc. Whenever the Depositary receives confirmation from the Custodian of receipt of any cash dividend or other cash distribution on any Deposited Securities, or receives proceeds from the sale of any Shares, rights securities or other entitlements under the Deposit Agreement, the Depositary will, if at the time of receipt thereof any amounts received in a Foreign Currency can, in the judgment of the Depositary (upon the terms of the Deposit Agreement), be converted on a practicable basis, into Dollars transferable to the United States, promptly convert or cause to be converted such dividend, distribution or proceeds into Dollars and will distribute promptly the amount thus received (net of applicable fees and charges of, and expenses incurred by, the Depositary and taxes and governmental charges) to the Holders of record as of the ADS Record Date in proportion to the number of ADSs held by such Holders respectively as of the ADS Record Date. The Depositary shall distribute only such amount, however, as can be distributed without attributing to any Holder a fraction of one cent. Any such fractional amounts shall be rounded down to the nearest whole cent and so distributed to Holders entitled thereto. If the Company, the Custodian or the Depositary is required to withhold and does withhold from any cash dividend or other cash distribution in respect of any Deposited Securities an amount on account of taxes, duties or other governmental charges, the amount distributed to Holders on the ADSs representing such Deposited Securities shall be reduced accordingly. Such withheld amounts shall be forwarded by the Company, the Custodian or the Depositary to the relevant governmental authority. Evidence of payment thereof by the Company shall be forwarded by the Company to the Depositary upon request. The Depositary will forward to the Company or its agent such information from its records as the Company may reasonably request to enable the Company or its agent to file necessary reports with governmental agencies, such reports necessary to obtain benefits under the applicable tax treaties for the Holders and Beneficial Owners of Receipts. Any Foreign Currency received by the Depositary shall be converted upon the terms and conditions set forth in the Deposit Agreement.

If any distribution upon any Deposited Securities consists of a dividend in, or free distribution of, Shares, the Company shall cause such Shares to be deposited with the Custodian and registered, as the case may be, in the name of the Depositary, the Custodian or their nominees. Upon receipt of confirmation of such deposit from the Custodian, the Depositary shall, subject to and in accordance with the Deposit Agreement, establish the ADS Record Date and either (i) distribute to the Holders as of the ADS Record Date in proportion to the number of ADSs held as of the ADS Record Date, additional ADSs, which represent in aggregate the number of Shares received as such dividend, or free distribution, subject to the terms of the Deposit Agreement (including, without limitation, the applicable fees and charges of, and expenses incurred by, the Depositary, and taxes and/or governmental charges), or (ii) if additional ADSs are not so distributed, each ADS issued and outstanding after the ADS Record Date shall, to the extent permissible by law, thenceforth also represent rights and interests in the additional Shares distributed upon the Deposited Securities represented thereby (net of the applicable fees and charges of, and the expenses incurred by, the Depositary, and taxes and

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governmental charges). In lieu of delivering fractional ADSs, the Depositary shall sell the number of Shares represented by the aggregate of such fractions and distribute the proceeds upon the terms set forth in the Deposit Agreement.

The Depositary may withhold any such distribution of Receipts if it has not received satisfactory assurances from the Company (including an opinion of counsel to the Company furnished at the expense of the Company) that such distribution does not require registration under the Securities Act or is exempt from registration under the provisions of the Securities Act. To the extent such distribution may be withheld, the Depositary may dispose of all or a portion of such distribution in such amounts and in such manner, including by public or private sale, as the Depositary deems necessary and practicable, and the Depositary shall distribute the net proceeds of any such sale (after deduction of taxes and/or governmental charges and fees and charges of, and expenses incurred by, the Depositary) to Holders entitled thereto upon the terms of the Deposit Agreement.

Whenever the Company intends to distribute a dividend payable at the election of the holders of Shares in cash or in additional Shares, the Depositary shall, to the extent permitted by law, distribute to the Holders, on the basis of the same determination as is made in the local market in respect of the Shares for which no election is made, either cash or additional ADSs representing such additional Shares, in each case upon the terms described in the Deposit Agreement.

The Depositary shall not be responsible for, and the Company shall not be liable to Holders or Beneficial Owners for, (i) any failure to determine that it may be lawful or reasonably practicable to sell such rights or (ii) any foreign exchange exposure or loss incurred in connection with such sale, or exercise. The Depositary shall not be responsible for the content of any materials forwarded to the Holders on behalf of the Company in connection with the rights distribution.

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to any tax or other governmental charges which the Depositary is obligated to withhold, the Depositary may dispose of all or a portion of such property (including Shares and rights to subscribe therefor) in such amounts and in such manner, including by public or private sale, as the Depositary deems necessary and practicable to pay any such taxes and charges.

Whenever the Company intends to distribute to the holders of Deposited Securities property other than cash, Shares or rights to purchase additional Shares, the Depositary shall endeavor to sell or cause such property to be sold in a public or private sale, at such place or places and upon such terms as it may deem proper and shall distribute the net proceeds, if any, of such sale received by the Depositary (net of applicable (a) fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) to the Holders as of the ADS Record Date upon the terms of Section 4.1 of the Deposit Agreement. If the Depositary is unable to sell such property, the Depositary may dispose of such property in any way it deems reasonably practicable under the circumstances for nominal or no consideration and Holders and Beneficial Owners shall have no rights thereto or arising therefrom.

If (i) the Company does not request the Depositary to make such distribution to Holders or requests not to make such distribution to Holders, (ii) the Depositary does not receive satisfactory documentation within the terms of Section 5.7 of the Deposit Agreement, or (iii) the Depositary determines that all or a portion of such distribution is not reasonably practicable or feasible, the Depositary shall, subject to applicable law, endeavor to sell or cause such property to be sold in a public or private sale, at such place or places and upon such terms as it may deem proper and shall distribute the proceeds of such sale received by the Depositary (net of (a) applicable fees and charges of, and expenses incurred by, the Depositary and (b) taxes and governmental charges) to the Holders upon the terms hereof and of the Deposit Agreement. If the Depositary is unable to sell such property, the Depositary may dispose of such property in any way it deems reasonably practicable under the circumstances for nominal or no consideration and Holders and Beneficial Owners shall have no rights thereto or arising therefrom.

(14) Fixing of Record Date. Whenever necessary in connection with any distribution (whether in cash, Shares, rights or other distribution), or whenever for any reason the Depositary causes a change in the number of Shares that are represented by each ADS, or whenever the Depositary shall receive notice of any meeting of or solicitation of holders of Shares or other Deposited Securities, or whenever the Depositary shall find it necessary or convenient, the Depositary shall fix a record date (“ADS Record Date”) as close as practicable to the record date fixed by the Company with respect to the Shares (if applicable) for the determination of the Holders who shall be entitled to receive such distribution, to give instructions for the exercise of voting rights at any such meeting, or to give or withhold such consent, or to receive such notice or solicitation or to otherwise take action, or to exercise the rights of Holders with respect to such changed number of Shares represented by each ADS or for any other reason. Subject to applicable law and the terms and conditions of this Receipt and the Deposit Agreement, only the Holders of record at the close of business in New York on such ADS Record Date shall be so obligated or otherwise entitled to receive such distributions, to give such voting instructions, to receive such notice or solicitation, or otherwise take action.

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(15) Voting of Deposited Securities. Subject to the next sentence, as soon as practicable after receipt of notice of any meeting at which the holders of Shares are entitled to vote, or of solicitation of consents or proxies from holders of Shares or other Deposited Securities, the Depositary shall fix the ADS Record Date in respect of such meeting or solicitation of such consent or proxy. The Depositary shall, if requested by the Company in writing in a timely manner (the Depositary having no obligation to take any further action if the request shall not have been received by the Depositary at least 30 days prior to the date of such vote or meeting), at the Company’s expense and provided no U.S. legal prohibitions exist, mail by ordinary, regular mail delivery (or by electronic mail or as otherwise agreed by the Company and the Depositary in writing from time to time), or otherwise distribute to Holders as of the ADS Record Date: (a) such notice of meeting or solicitation of consent or proxy; (b) subject to the next paragraph, a statement that the Holders at the close of business on the ADS Record Date will be entitled, subject to any applicable law, the Company’s constituent documents and the provisions of or governing the Deposited Securities (which provisions, if any, shall be summarized in pertinent part by the Company), to instruct the Depositary as to the exercise of the voting rights, if any, pertaining to the Shares or other Deposited Securities represented by such Holder’s American Depositary Shares; and (c) a brief statement as to the manner in which such instructions may be given. Upon the timely receipt of written instructions of a Holder on the ADS Record Date of voting instructions in the manner specified by the Depositary, the Depositary shall endeavor, insofar as practicable and permitted under applicable law, the provisions of this Deposit Agreement, the Company’s constituent documents and the provisions of or governing the Deposited Securities, to vote or cause the Custodian to vote the Shares and/or other Deposited Securities (in person or by proxy) represented by American Depositary Shares evidenced by such Receipt in accordance with such voting instructions. Voting instructions may be given only in respect of a number of American Depositary Shares representing an integral number of Shares or other Deposited Securities.

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Neither the Depositary nor the Custodian shall, under any circumstances exercise any discretion as to voting, and neither the Depositary nor the Custodian shall vote, attempt to exercise the right to vote, or in any way make use of for purposes of establishing a quorum or otherwise the Shares or other Deposited Securities represented by ADSs except pursuant to and in accordance with such written instructions from Holders. Shares or other Deposited Securities represented by ADSs for which no specific voting instructions are received by the Depositary from the Holder shall not be voted.

Notwithstanding the above, and in accordance with Section 5.3 of the Deposit Agreement, the Depositary shall not be liable for any failure to carry out any instructions to vote any of the Deposited Securities, or for the manner in which such vote is cast or the effect of any such vote.

(16) Changes Affecting Deposited Securities. Upon any change in par value, split-up, subdivision cancellation, consolidation or any other reclassification of Deposited Securities, or upon any recapitalization, reorganization, merger, amalgamation or consolidation or sale of assets affecting the Company or to which it otherwise is a party, any securities which shall be received by the Depositary or a Custodian in exchange for, or in conversion of or replacement or otherwise in respect of, such Deposited Securities shall, to the extent permitted by law, be treated as new Deposited Securities under the Deposit Agreement, and the Receipts shall, subject to the provisions of the Deposit Agreement and applicable law, evidence ADSs representing the right to receive such additional securities. Alternatively, the Depositary may, with the Company’s prior approval (which approval shall not be unreasonably withheld), and shall, if the Company shall so request, subject to the terms of the Deposit Agreement and receipt of an opinion of counsel to the Company, furnished at the expense of the Company, satisfactory to the Depositary that such distributions are not in violation of any applicable laws or regulations, execute and deliver additional Receipts as in the case of a stock dividend on the Shares, or call for the surrender of outstanding Receipts to be exchanged for new Receipts, in either case, as well as in the event of newly deposited Shares, with necessary modifications to this form of Receipt specifically describing such new Deposited Securities and/or corporate change. Notwithstanding the foregoing, in the event that any security so received may not be lawfully distributed to some or all Holders, the Depositary may, with the Company’s prior approval (which approval shall not be unreasonably withheld), and shall if the Company requests, subject to receipt of an opinion of counsel to the Company, furnished at the expense of the Company, satisfactory to the Depositary that such distributions are not in violation of any applicable laws or regulations, sell such securities at public or private sale, at such place or places and upon such terms as it may deem proper and may allocate the net proceeds of such sales (net of fees and charges of, and expenses incurred by, the Depositary and taxes and governmental charges) for the account of the Holders otherwise entitled to such securities upon an averaged or other practicable basis without regard to any distinctions among such Holders and distribute the net proceeds so allocated to the extent

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practicable as in the case of a distribution received in cash pursuant to the Deposit Agreement. The Depositary shall not be responsible for, and the Company shall not be liable to Holders or Beneficial Owners for, (i) any failure to determine that it may be lawful or feasible to make such securities available to Holders in general or to any Holder in particular, (ii) any foreign exchange exposure or loss incurred in connection with such sale, or (iii) any liability to the purchaser of such securities.

(17) Exoneration. Neither the Depositary, the Custodian or the Company shall be obligated to do or perform any act which is inconsistent with the provisions of the Deposit Agreement or shall incur any liability to Holders, Beneficial Owners or any third parties (i) if the Depositary, the Custodian or the Company or their respective controlling persons or agents (including, without limitation, Agents, in the case of the Depositary) shall be prevented or forbidden from, or subjected to any civil or criminal penalty or restraint on account of, or delayed in, doing or performing any act or thing required by the terms of the Deposit Agreement and any Receipt, by reason of any provision of any present or future law, rule, regulation, fiat, order or decree of the United States or any state thereof, the Kingdom of Denmark or any other country or jurisdiction, or of any other governmental authority or regulatory authority or stock exchange, or on account of the possible criminal or civil penalties or restraint, or by reason of any provision, present or future, of the Company’s constituent documents or any provision of or governing any Deposited Securities, or by reason of any act of God, war, terrorism, nationalization, expropriation, currency restrictions, work stoppage, strike, civil unrest, revolutions, rebellions, explosions, computer failure or circumstance beyond its control, (ii) by reason of any exercise of, or failure to exercise, any discretion provided for in the Deposit Agreement or in the Company’s constituent documents or provisions of or governing Deposited Securities, (iii) for any action or inaction of the Depositary, the Custodian or the Company or their respective controlling persons or agents (including, without limitation, Agents) in reliance upon the advice of or information from legal counsel, accountants, any person presenting Shares for deposit, any Holder, any Beneficial Owner or authorized representative thereof, or any other person believed by it in good faith to be competent to give such advice or information, including, without limitation, in determining if a proposed distribution, action or transaction under Article IV of the Deposit Agreement is lawful, (iv) for any inability by a Holder or Beneficial Owner to benefit from any distribution, offering, right or other benefit which is made available to holders of Deposited Securities but is not, under the terms of the Deposit Agreement, made available to Holders of ADS or (v) for any special, consequential, indirect or punitive damages for any breach of the terms of the Deposit Agreement or otherwise. Every Holder and Beneficial Owner agrees to, and shall, indemnify the Depositary, the Company, the Custodian and each and every of their respective officers, directors, employees, agents (including, without limitation, Agents) and Affiliates against, and hold each of them harmless from, any claims with respect to taxes, additions to tax (including applicable interest and penalties thereon) arising out of any refund of taxes, reduced rate of withholding at source or other tax benefit obtained for or by such Holder and/or Beneficial Owner. The Depositary shall not incur any liability for, and the Company shall not incur any liability to Holders or Beneficial Owners for, any consequences of Foreign Currency conversion that may be incurred by Holders and/or Beneficial Owners on account of their ownership of American Depositary Shares or otherwise. The Depositary, its controlling persons, its agents (including, without limitation, Agents), any Custodian and the Company, its

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controlling persons and its agents may rely and shall be protected in acting upon any written notice, request, opinion or other document believed by it to be genuine and to have been signed or presented by the proper party or parties. Neither the Depositary nor the Custodian shall be liable for the failure by any Holder or Beneficial Owner to obtain the benefits of credits on the basis of non-U.S. tax paid against such Holder’s or Beneficial Owner’s income tax liability. The Company shall not be liable to Holders or Beneficial Owners for the failure by any Holder or Beneficial Owner to obtain the benefits of credits on the basis of non-U.S. tax paid against such Holder’s or Beneficial Owner’s income tax liability. No disclaimer of liability under the Securities Act is intended by any provision of the Deposit Agreement.

(18) Standard of Care. The Company and the Depositary and their respective directors, officers, Affiliates, employees and agents (including, without limitation, Agents) assume no obligation and shall not be subject to any liability under the Deposit Agreement or the Receipts to Holders or Beneficial Owners or other persons (except for the Company’s and the Depositary’s obligations specifically set forth in Section 5.8 of the Deposit Agreement), provided, that the Company and the Depositary and their respective agents (including, without limitation, Agents) agree to perform their respective obligations specifically set forth in the Deposit Agreement without gross negligence or willful misconduct. Without limitation of the foregoing, neither the Depositary, nor the Company, nor any of their respective controlling persons, directors, officers, Affiliates, employees or agents (including, without limitation, Agents), shall be under any obligation to appear in, prosecute or defend any action, suit or other proceeding in respect of any Deposited Securities or in respect of this Receipt, which in its opinion may involve it in expense or liability, unless indemnity satisfactory to it against all expenses (including fees and disbursements of counsel) and liabilities be furnished as often as may be required (and no Custodian shall be under any obligation whatsoever with respect to such proceedings, the responsibility of the Custodian being solely to the Depositary). The Depositary and its agents (including, without limitation, Agents) shall not be liable for any failure to carry out any instructions to vote any of the Deposited Securities, or for the manner in which any vote is cast (provided that any such action or omission is in good faith) or the effect of any vote. The Depositary shall not incur any liability for any failure to determine that any distribution or action may be lawful or reasonably practicable, for the content of any information submitted to it by the Company for distribution to the Holders or for any inaccuracy of any translation thereof, for any investment risk associated with acquiring an interest in the Deposited Securities, for the validity or worth of the Deposited Securities or for any tax consequences that may result from the ownership of ADSs, Shares or Deposited Securities, for the credit-worthiness of any third party, for allowing any rights to lapse upon the terms of the Deposit Agreement or for the failure or timeliness of any notice from the Company. In connection with the sale of securities, including, without limitation, Deposited Securities, the Depositary shall not have any liability for the price received in connection with any such sale, the timing thereof or any delay in action or omission to act nor shall it be responsible for any error or delay in action, omission to act, default or negligence on the part of the party so retained in connection with any such sale or proposed sale. The Depositary shall not incur any liability for any action or non action by it in reliance upon the opinion, advice of or information from legal counsel, accountants, any person presenting Shares for deposit, any Holder or any other person believed by it in good faith to be competent to give such advice or information. The Depositary and its agents (including, without limitation,

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Agents) shall not be liable for any acts or omissions made by a successor depositary. The Depositary is under no obligation to provide the Holders and Beneficial Owners with any information about the tax status of the Company. The Depositary shall not incur any liability for any tax consequences that may be incurred by Holders and Beneficial Owners on account of their ownership of the American Depositary Shares, including without limitation, tax consequences resulting from the Company (or any of its subsidiaries) being treated as a “Passive Foreign Investment Company” (as defined in the U.S. Internal Revenue Code and the regulations issued thereunder) or otherwise. In no event shall the Depositary or any of its directors, officers, employees, agents (including, without limitation, its Agents) and/or Affiliates, or any of them, be liable for any indirect, special, punitive or consequential damages to the Company, Holders, Beneficial Owners or any other person.

(19) Resignation and Removal of the Depositary; Appointment of Successor Depositary. The Depositary may at any time resign as Depositary under the Deposit Agreement by written notice of resignation delivered to the Company, such resignation to be effective on the earlier of (i) the 90th day after delivery thereof to the Company (whereupon the Depositary shall, in the event no successor depositary has been appointed by the Company, be entitled to terminate the Deposit Agreement as contemplated under the provisions of the Deposit Agreement), or (ii) upon the appointment by the Company of a successor depositary and its acceptance of such appointment as provided in the Deposit Agreement, save that, any amounts, fees, costs or expenses owed to the Depositary under the Deposit Agreement or in accordance with any other agreements otherwise agreed in writing between the Company and the Depositary from time to time shall be paid to the Depositary prior to such resignation. The Company shall use reasonable efforts to appoint such successor depositary, and give notice to the Depositary of such appointment, not more than 90 days after delivery by the Depositary of written notice of resignation as provided in the Deposit Agreement. The Depositary may at any time be removed by the Company by written notice of such removal which removal shall be effective on the later of (i) the 90th day after delivery thereof to the Depositary (whereupon the Depositary shall be entitled to terminate the Deposit Agreement as contemplated under the provisions of the Deposit Agreement), or (ii) upon the appointment by the Company of a successor depositary and its acceptance of such appointment as provided in the Deposit Agreement save that, any amounts, fees, costs or expenses owed to the Depositary under the Deposit Agreement or in accordance with any other agreements otherwise agreed in writing between the Company and the Depositary from time to time shall be paid to the Depositary prior to such removal. In case at any time the Depositary acting hereunder shall resign or be removed, the Company shall use its best efforts to appoint a successor depositary which shall be a bank or trust company having an office in the Borough of Manhattan, the City of New York. The Company shall give notice to the Depositary of the appointment of a successor depositary not more than 90 days after delivery by the Depositary of written notice of resignation or by the Company of removal, each as provided in this Article (19) and the Deposit Agreement. In the event that a successor depositary is not appointed or notice of the appointment of a successor depositary is not provided by the Company in accordance with the preceding sentence, the Depositary shall be entitled to terminate the Deposit Agreement as contemplated under the provisions of the Deposit Agreement. Every successor depositary shall execute and deliver to its predecessor and to the Company an instrument in writing accepting its appointment hereunder, and thereupon such successor

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depositary, without any further act or deed (except as required by applicable law), shall become fully vested with all the rights, powers, duties and obligations of its predecessor. The predecessor depositary, upon payment of all sums due it and on the written request of the Company, shall (i) execute and deliver an instrument transferring to such successor all rights and powers of such predecessor hereunder (other than as contemplated in the Deposit Agreement), (ii) duly assign, transfer and deliver all right, title and interest to the Deposited Securities to such successor, and (iii) deliver to such successor a list of the Holders of all outstanding Receipts and such other information relating to Receipts and Holders thereof as the successor may reasonably request. Any such successor depositary shall promptly mail notice of its appointment to such Holders. Any corporation into or with which the Depositary may be merged or consolidated shall be the successor of the Depositary without the execution or filing of any document or any further act.

(20) Amendment/Supplement. Subject to the terms and conditions of this Article (20), and applicable law, this Receipt and any provisions of the Deposit Agreement may at any time and from time to time be amended or supplemented by written agreement between the Company and the Depositary in any respect which they may deem necessary or desirable without the consent of the Holders or Beneficial Owners. Any amendment or supplement which shall impose or increase any fees or charges (other than charges in connection with foreign exchange control regulations, and taxes and/or other governmental charges, delivery and other such expenses), or which shall otherwise materially prejudice any substantial existing right of Holders or Beneficial Owners, shall not, however, become effective as to outstanding Receipts until 30 days after notice of such amendment or supplement shall have been given to the Holders of outstanding Receipts. Notice of any amendment to the Deposit Agreement or form of Receipts shall not need to describe in detail the specific amendments effectuated thereby, and failure to describe the specific amendments in any such notice shall not render such notice invalid, provided, however, that, in each such case, the notice given to the Holders identifies a means for Holders and Beneficial Owners to retrieve or receive the text of such amendment (i.e., upon retrieval from the Commission’s, the Depositary’s or the Company’s website or upon request from the Depositary). The parties hereto agree that any amendments or supplements which (i) are reasonably necessary (as agreed by the Company and the Depositary) in order for (a) the ADSs to be registered on Form F-6 under the Securities Act or (b) the ADSs or Shares to be traded solely in electronic book-entry form and (ii) do not in either such case impose or increase any fees or charges to be borne by Holders, shall be deemed not to materially prejudice any substantial rights of Holders or Beneficial Owners. Every Holder and Beneficial Owner at the time any amendment or supplement so becomes effective shall be deemed, by continuing to hold such ADS, to consent and agree to such amendment or supplement and to be bound by the Deposit Agreement as amended or supplemented thereby. In no event shall any amendment or supplement impair the right of the Holder to surrender such Receipt and receive therefor the Deposited Securities represented thereby, except in order to comply with mandatory provisions of applicable law. Notwithstanding the foregoing, if any governmental body should adopt new laws, rules or regulations which would require amendment or supplement of the Deposit Agreement to ensure compliance therewith, the Company and the Depositary may amend or supplement the Deposit Agreement and the Receipt at any time in accordance with such changed laws, rules or regulations. Such amendment or supplement to the Deposit Agreement in such circumstances

A-19

may become effective before a notice of such amendment or supplement is given to Holders or within any other period of time as required for compliance with such laws, or rules or regulations.

(21) Termination. The Depositary shall, at any time at the written direction of the Company, terminate the Deposit Agreement by mailing notice of such termination to the Holders of all Receipts then outstanding at least 90 days prior to the date fixed in such notice for such termination provided that, the Depositary shall be reimbursed for any amounts, fees, costs or expenses owed to it in accordance with the terms of the Deposit Agreement and in accordance with any other agreements as otherwise agreed in writing between the Company and the Depositary from time to time, before such termination shall take effect. If 90 days shall have expired after (i) the Depositary shall have delivered to the Company a written notice of its election to resign, or (ii) the Company shall have delivered to the Depositary a written notice of the removal of the Depositary, and in either case a successor depositary shall not have been appointed and accepted its appointment as provided herein and in the Deposit Agreement, the Depositary may terminate the Deposit Agreement by mailing notice of such termination to the Holders of all Receipts then outstanding at least 30 days prior to the date fixed for such termination. On and after the date of termination of the Deposit Agreement, the Holder will, upon surrender of such Holder’s Receipt at the Principal Office of the Depositary, upon the payment of the charges of the Depositary for the surrender of Receipts referred to in Article (2) hereof and in the Deposit Agreement and subject to the conditions and restrictions therein set forth, and upon payment of any applicable taxes and/or governmental charges, be entitled to delivery, to him or upon his order, of the amount of Deposited Securities represented by such Receipt. If any Receipts shall remain outstanding after the date of termination of the Deposit Agreement, the Registrar thereafter shall discontinue the registration of transfers of Receipts, and the Depositary shall suspend the distribution of dividends to the Holders thereof, and shall not give any further notices or perform any further acts under the Deposit Agreement, except that the Depositary shall continue to collect dividends and other distributions pertaining to Deposited Securities, shall sell rights as provided in the Deposit Agreement, and shall continue to deliver Deposited Securities, subject to the conditions and restrictions set forth in the Deposit Agreement, together with any dividends or other distributions received with respect thereto and the net proceeds of the sale of any rights or other property, in exchange for Receipts surrendered to the Depositary (after deducting, or charging, as the case may be, in each case the charges of the Depositary for the surrender of a Receipt, any expenses for the account of the Holder in accordance with the terms and conditions of the Deposit Agreement and any applicable taxes and/or governmental charges or assessments). At any time after the expiration of six months from the date of termination of the Deposit Agreement, the Depositary may, subject to applicable law, sell the Deposited Securities then held hereunder and may thereafter hold uninvested the net proceeds of any such sale, together with any other cash then held by it hereunder, in an unsegregated account, without liability for interest for the pro rata benefit of the Holders of Receipts whose Receipts have not theretofore been surrendered. After making such sale, the Depositary shall be discharged from all obligations under the Deposit Agreement with respect to the Receipts and the Shares, Deposited Securities and ADSs, except to account for such net proceeds and other cash (after deducting, or charging, as the case may be, in each case the charges of the Depositary for the surrender of a Receipt, any expenses for the account of the

A-20

Holder in accordance with the terms and conditions of the Deposit Agreement and any applicable taxes and/or governmental charges or assessments). Upon the termination of the Deposit Agreement, the Company shall be discharged from all obligations under the Deposit Agreement except as set forth in the Deposit Agreement. The obligations under the terms of the Deposit Agreement and Receipts of Holders and Beneficial Owners of ADSs outstanding as of the effective date of any termination shall survive such effective date of termination and shall be discharged only when the applicable ADSs are presented by their Holders to the Depositary for cancellation under the terms of the Deposit Agreement and the Holders have each satisfied any and all of their obligations hereunder (including, but not limited to, any payment and/or reimbursement obligations which relate to prior to the effective date of termination but which payment and/or reimbursement is claimed after such effective date of termination).

(22) Compliance with U.S. Securities Laws; Regulatory Compliance. Notwithstanding any provisions in this Receipt or the Deposit Agreement to the contrary, the withdrawal or delivery of Deposited Securities will not be suspended by the Company or the Depositary except as would be permitted by Instruction I.A.(1) of the General Instructions to the Form F-6 Registration Statement, as amended from time to time, under the Securities Act.

(23) Certain Rights of the Depositary; Limitations. Subject to the further terms and provisions of this Article (23), the Depositary, its Affiliates and their agents, on their own behalf, may own and deal in any class of securities of the Company and its Affiliates and in ADSs. The Depositary may issue ADSs against evidence of rights to receive Shares from the Company, any agent of the Company or any custodian, registrar, transfer agent, clearing agency or other entity involved in ownership or transaction records in respect of the Shares. In its capacity as Depositary, the Depositary may (i) issue ADSs prior to the receipt of Shares (each such transaction a “Pre-Release Transaction) pursuant to Section 2.3 of the Deposit Agreement and (ii) deliver Shares upon the receipt and cancellation of ADSs that were issued in a Pre-Release Transaction, but for which Shares may not have been received. The Depositary may receive ADSs in lieu of Shares under (i) above and receive Shares in lieu of ADSs under (ii) above. Each such Pre-Release Transaction will be (a) subject to a written agreement whereby the person or entity (the “Applicant”) to whom ADSs or Shares are to be Delivered (1) represents that at the time of the Pre-Release Transaction the Applicant or its customer beneficially owns the Shares or ADSs that are to be Delivered by the Applicant under such Pre-Release Transaction, (2) agrees to indicate the Depositary as owner of such Shares or ADSs in its records and to hold such Shares or ADSs in trust for the Depositary until such Shares or ADSs are delivered to the Depositary or the Custodian, (3) unconditionally guarantees to deliver to the Depositary or the Custodian, as applicable, such Shares or ADSs and (4) agrees to any additional restrictions or requirements that the Depositary deems appropriate; (b) at all times fully collateralized with cash, U.S. government securities or such other collateral as the Depositary deems appropriate; (c) terminable by the Depositary on not more than five (5) Business Days’ notice; and (d) subject to such further indemnities and credit regulations as the Depositary deems appropriate. The Depositary will normally limit the number of ADSs and Shares involved in such Pre-Release Transactions at any one time to thirty percent (30%) of the ADSs outstanding (without giving effect to ADSs outstanding under (i) above), provided, however, that the Depositary reserves the right to disregard such limit from time to time as it deems appropriate. The Depositary may also set

A-21

limits with respect to the number of ADSs and Shares involved in Pre-Release Transactions with any one person on a case by case basis as it deems appropriate. The Depositary may retain for its own account any compensation received by it in conjunction with the foregoing. Collateral provided pursuant to (b) above, but not earnings thereon, shall be held for the benefit of the Holders (other than the Applicant).

(24) Ownership Restrictions. Holders and Beneficial Owners shall comply with any limitations on ownership of Shares under the constituent documents of the Company or applicable Danish law as if they held the number of Shares their ADSs represent. The Company shall inform the Holders, Beneficial Owners and the Depositary of any limitations on ownership of Shares that the Holders and Beneficial Owners may be subject to by reason of the number of American Depositary Shares held under the constituent documents of the Company, or applicable Danish law, as such restrictions may be in force from time to time.

(25) Waiver; Jurisdiction; Arbitration. EACH PARTY TO THE DEPOSIT AGREEMENT (INCLUDING, FOR AVOIDANCE OF DOUBT, EACH HOLDER AND BENEFICIAL OWNER AND/OR HOLDER OF INTERESTS IN ADRS) HEREBY IRREVOCABLY WAIVES, TO THE FULLEST EXTENT PERMITTED BY APPLICABLE LAW, ANY RIGHT IT MAY HAVE TO A TRIAL BY JURY IN ANY SUIT, ACTION OR PROCEEDING AGAINST THE DEPOSITARY AND/OR THE COMPANY DIRECTLY OR INDIRECTLY ARISING OUT OF OR RELATING TO THE SHARES OR OTHER DEPOSITED SECURITIES, THE ADSs OR THE ADRs, THE DEPOSIT AGREEMENT OR ANY TRANSACTION CONTEMPLATED HEREIN OR THEREIN, OR THE BREACH HEREOF OR THEREOF (WHETHER BASED ON CONTRACT, TORT, COMMON LAW OR ANY OTHER THEORY).

The Company, the Depositary and by holding an American Depositary Share (or interest therein) Holders and Beneficial Owners each agree that, notwithstanding the foregoing, with regard to any claim or dispute or difference of whatever nature between or involving the parties hereto arising directly or indirectly from the relationship created by this Deposit Agreement, the Depositary, in its sole discretion, shall be entitled to refer such dispute or difference for final settlement by arbitration (“Arbitration”) in accordance with the Commercial Arbitration Rules of the American Arbitration Association (the “Rules”) then in force The arbitration shall be

A-22

conducted by three arbitrators, one nominated by the Depositary, one nominated by the Company, and one nominated by the two party-appointed arbitrators within thirty (30) calendar days of the confirmation of the nomination of the second arbitrator. If any arbitrator has not been nominated within the time limits specified herein and in the Rules, then such arbitrator shall be appointed by the American Arbitration Association in accordance with the Rules. Judgment upon the award rendered by the arbitrators may be enforced in any court having jurisdiction thereof. The seat and place of any reference to arbitration shall be New York City, New York, and the procedural law of such arbitration shall be New York law. The language to be used in the arbitration shall be English. The fees of the arbitrator and other costs incurred by the parties in connection with such Arbitration shall be paid by the party or parties that is (are) unsuccessful in such Arbitration.

(ASSIGNMENT AND TRANSFER SIGNATURE LINES)

FOR VALUE RECEIVED, the undersigned Holder hereby sell(s), assign(s) and transfer(s) unto whose taxpayer identification number is and whose address including postal zip code is , the within Receipt and all rights thereunder, hereby irrevocably constituting and appointing attorney-in-fact to transfer said Receipt on the books of the Depositary with full power of substitution in the premises.

Dated:	Name:
		By:
		Title:

	NOTICE: The signature of the Holder to this assignment must correspond with the name as written upon the face of the within instrument in every particular, without alteration or enlargement or any change whatsoever.

	If the endorsement be executed by an attorney, executor, administrator, trustee or guardian, the person executing the endorsement must give his/her full title in such capacity and proper evidence of authority to act in such capacity, if not on file with the Depositary, must be forwarded with this Receipt.

SIGNATURE GUARANTEED

A-23

TABLE OF CONTENTS

ARTICLE I DEFINITIONS			1

SECTION 1.1		“Affiliate”	1
SECTION 1.2		“Agent”	1
SECTION 1.3		“American Depositary Share(s)” and “ADS(s)”	1
SECTION 1.4		“ADS Record Date”	2
SECTION 1.5		“Beneficial Owner”	2
SECTION 1.6		“Business Day”	2
SECTION 1.7		“Commission”	2
SECTION 1.8		“Company”	2
SECTION 1.9		“Custodian”	2
SECTION 1.10		“Deliver” and “Delivery”	2
SECTION 1.11		“Deposit Agreement”	2
SECTION 1.12		“Depositary”	3
SECTION 1.13		“Deposited Securities”	3
SECTION 1.14		“Dollars” and “$”	3
SECTION 1.15		“DRS/Profile”	3
SECTION 1.16		“DTC”	3
SECTION 1.17		“Exchange Act”	3
SECTION 1.18		“Foreign Currency”	3
SECTION 1.19		“Foreign Registrar”	3
SECTION 1.20		“Holder”	3
SECTION 1.21		“Indemnified Person” and “Indemnifying Person”	3
SECTION 1.22		“Pre-Release Transaction”	4
SECTION 1.23		“Principal Office”	4
SECTION 1.24		“Receipt(s)”; “American Depositary Receipt(s)” and “ADR(s)”	4
SECTION 1.25		“Registrar”	4
SECTION 1.26		“Restricted Securities”	4
SECTION 1.27		“Securities Act”	4
SECTION 1.28		“Shares”	4
SECTION 1.29		“United States” or “U.S.”	5

ARTICLE II APPOINTMENT OF DEPOSITARY; FORM OF RECEIPTS; DEPOSIT OF SHARES; EXECUTION AND DELIVERY, TRANSFER AND SURRENDER OF RECEIPTS			5

SECTION 2.1	Appointment of Depositary		5
SECTION 2.2	Form and Transferability of Receipts		5
SECTION 2.3	Deposits		6
SECTION 2.4	Execution and Delivery of Receipts		8
SECTION 2.5	Transfer of Receipts; Combination and Split-up of Receipts		8
SECTION 2.6	Surrender of Receipts and Withdrawal of Deposited Securities		9

		Page

SECTION 2.7	Limitations on Execution and Delivery, Transfer, etc. of Receipts; Suspension of Delivery, Transfer, etc.	10
SECTION 2.8	Lost Receipts, etc.	11
SECTION 2.9	Cancellation and Destruction of Surrendered Receipts	11
SECTION 2.10	Pre-Release	11

ARTICLE III CERTAIN OBLIGATIONS OF HOLDERS AND BENEFICIAL OWNERS OF RECEIPTS		12

SECTION 3.1	Proofs, Certificates and Other Information	12
SECTION 3.2	Liability for Taxes and Other Charges	13
SECTION 3.3	Representations and Warranties on Deposit of Shares	13
SECTION 3.4	Ownership Restrictions	13
SECTION 3.5	Compliance with Information Requests	14

ARTICLE IV THE DEPOSITED SECURITIES		15

SECTION 4.1	Cash Distributions	15
SECTION 4.2	Distribution in Shares	15
SECTION 4.3	Elective Distributions in Cash or Shares	16
SECTION 4.4	Distribution of Rights to Purchase Shares	16
SECTION 4.5	Distributions Other Than Cash, Shares or Rights to Purchase Shares	17
SECTION 4.6	Conversion of Foreign Currency	17
SECTION 4.7	Fixing of Record Date	18
SECTION 4.8	Voting of Deposited Securities	18
SECTION 4.9	Changes Affecting Deposited Securities	20
SECTION 4.10	Available Information	21
SECTION 4.11	Reports	21
SECTION 4.12	List of Holders	22
SECTION 4.13	Taxation; Withholding	22

ARTICLE V THE DEPOSITARY, THE CUSTODIAN AND THE COMPANY		23

SECTION 5.1	Maintenance of Office and Transfer Books by the Registrar	23
SECTION 5.2	Exoneration	24
SECTION 5.3	Standard of Care	25
SECTION 5.4	Resignation and Removal of the Depositary; Appointment of Successor Depositary	25
SECTION 5.5	The Custodian	26
SECTION 5.6	Notices and Reports	27
SECTION 5.7	Issuance of Additional Shares, ADSs etc.	28
SECTION 5.8	Indemnification	29
SECTION 5.9	Fees and Charges of Depositary	30
SECTION 5.10	Restricted Securities Owners	31

ARTICLE VI AMENDMENT AND TERMINATION		31

			Page

SECTION 6.1	Amendment/Supplement		31
SECTION 6.2	Termination		32

ARTICLE VII MISCELLANEOUS			34

SECTION 7.1		Counterparts	34
SECTION 7.2		No Third-Party Beneficiaries	34
SECTION 7.3		Severability	34
SECTION 7.4		Holders and Beneficial Owners as Parties; Binding Effect	34
SECTION 7.5		Notices	34
SECTION 7.6		Governing Law and Jurisdiction	35
SECTION 7.7		Assignment	37
SECTION 7.8		Compliance with U.S. Securities Laws	37
SECTION 7.9		Titles; References	37
SECTION 7.10		Agents	37
SECTION 7.11		Exclusivity	37
SECTION 7.12		Affiliates etc.	38
SECTION 7.13		Amendment and Restatement of Old Deposit Agreement	38

EXHIBIT A Form of Receipt			A-1

iii

Exhibit 10.1

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

***Text Omitted and Filed Separately with the Securities and Exchange Commission. Confidential Treatment Requested Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406***Text Omitted and Filed Separately with the Securities and Exchange Commission. Confidential Treatment Requested Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406 Object Class: 26101 Amount: $500,000,000 CONTRACTING OFFICER WILL COMPLETE ITEM 17 OR 18 AS APPLICABLE STANDARD FORM 26 (REV. 4-85) Prescribed by GSA, FAR (48 CFR) 53.214(a) NSN 7540-01-152-8069 PREVIOUS EDITION UNUSABLE 26-107 Computer Generated 17. CONTRACTOR'S NEGOTIATED AGREEMENT (Contractor is required to sign this document and return 3 copies to issuing office.) Contractor agrees to furnish and deliver all items or perform all the services set forth or otherwise identified above and on any continuation sheets for the consideration stated herein. The rights and obligations of the parties to this contract shall be subject to and governed by the following documents: (a) this award/contract, (b) the solicitation, if any, and (c) such provisions, representations, certifications, and specifications, as are attached or incorporated by reference herein. (Attachments are listed herein.) 18. AWARD (Contractor is not required to sign this document.) Your offer on Solicitation Number including the additions or changes made by you which additions or changes are set forth in full above, is hereby accepted as to the terms listed above and on any continuation sheets. This award consummates the contract which consists of the following documents: (a) the Government's solicitation and your offer, and (b) this award/contract. No further contractual document is necessary. 19A. NAME AND TITLE OF SIGNER (Type or print) [***], CEO 20A. NAME OF CONTRACTING OFFICER [***] 19B. NAME OF CONTRACTOR [***] (Signature of person authorized to sign) 19C. DATE SIGNED 6/1/2007 20B. UNITED STATES OF AMERICA BY [***] (Signature of Contracting Officer) 20C. DATE SIGNED 6/4/2007 AWARD/CONTRACT 1. THIS CONTRACT IS A RATED ORDER UNDER DPAS (15 CFR 350) RATING N/A PAGEOFPAGES 1 61 2. CONTRACT (Proc. Inst. Ident.) NO. HHSO100200700034C 3. EFFECTIVE DATE See Block 20C 4. REQUISITION/PURCHASE REQUEST/PROJECT NO. N/A 5. ISSUED BYCODE N/A 6. ADMINISTERED BY (If other than Item 6)CODE N/A HHS/OS/ASPR/BARDA 330 INDEPENDENCE AVE S.W., RM G640 WASHINGTON, D.C. 20201 See Block 5 7. NAME AND ADDRESS OF CONTRACTOR (No., street, county, state and ZIP Code) BAVARIAN NORDIC A/S BOGESKOVVEJ9 DK-3490 KVISTGAARD DENMARK 8. DELIVERY FOB ORIGINOTHER (See below) 9. DISCOUNT FOR PROMPT PAYMENT N/A 10. SUBMIT INVOICES ADDRESS SHOWN IN ITEM See Section G. CODEN/A FACILITY CODEN/A 11. SHIP TO/MARK FORCODE N/A 12. PAYMENT WILL BE MADE BYCODE N/A See Block 5 See Block 5 13. AUTHORITY FOR USING OTHER THAN FULL AND OPEN COMPETITION: 10 U.S.C. 2304(c)() 41 U.S.C. 253(c)() 14. ACCOUNTING AND APPROPRIATION DATA CAN: 199999EAppropriation: 75 7005/130714.001 15A. ITEM NO. 15B. SUPPLIES/SERVICES 15C. QUANTITY 15D.UNIT 15E. UNIT PRICE 15F. AMOUNT See Section B $500,000,000 NTE Not-to-Exceed 15G. TOTAL AMOUNT OF CONTRACT $500,000,000 16. TABLE OF CONTENTS () SEC. DESCRIPTION PAGE(S) () SEC. DESCRIPTION PAGE(S) PART I - THE SCHEDULE PART II - CONTRACT CLAUSES A SOLICITATION/CONTRACT FORM 1 I CONTRACT CLAUSES 32 B SUPPLIES OR SERVICES AND PRICE/COST 2 PART III - LIST OF DOCUMENTS, EXHIBITS AND OTHER ATTACH C DESCRIPTION/SPECS./WORK STATEMENT 9 J LIST OF ATTACHMENTS 40 D PACKAGING AND MARKING 18 PART IV - REPRESENTATIONS AND INSTRUCTIONS E INSPECTION AND ACCEPTANCE 18 K REPRESENTATIONS, CERTIFICATIONS AND OTHER STATEMENTS OF OFFERORS 41 F DELIVERIES OR PERFORMANCE 19 G CONTRACT ADMINISTRATION DATA 21 L INSTRS., CONDS., AND NOTICES TO OFFERORS N/A H SPECIAL CONTRACT REQUIREMENTS 25 M EVALUATION FACTORS FOR AWARD N/A

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C

Bavarian Nordic A/S

SECTION B—SUPPLIES OR SERVICES AND PRICES/COSTS

B.1. BRIEF DESCRIPTION OF SUPPLIES OR SERVICES

The Contractor shall supply the necessary supplies and services for the acquisition of 20 million doses (in single-dose vials) of MVA vaccine for the Strategic National Stockpile. In addition, there are options for maintaining cGMP capability (warm base), the purchase of additional quantities of vaccine, and obtaining data to support expanded clinical usage any one of which could result in a five (5) year extension to the period of performance. The urgent nature of this requirement requires an accelerated pace of development, testing, approval, and procurement of an emergency stockpile of vaccine. In the case of intentional smallpox release prior to licensure by the Food and Drug Administration (FDA)/Center for Biologics Evaluation and Review (CBER). it is anticipated that the investigational MVA vaccine could be administered under an “Emergency Use Authorization” (EUA), held by the Centers for Disease Control and Prevention (CDC). Vaccine acceptance into the SNS is solely dependent on the accumulation and submission of the appropriate data that might have the potential to support EUA. However, all vaccine manufactured and acquired under this Contract must meet the regulatory deliverables as required for licensure.

B.2 PRICES/COSTS

A. BASE CONTRACT

1. FIRM FIXED PRICE (FPP)

In consideration for completion of the work to be performed under Contract Line Item Numbers (CLINs) 0001, 0002, and 0003, as shown below, and in accordance with the Statement of Work, the Contactor shall be paid an amount Not-to-Exceed $[***]. See Section G, Paragraph G.8, Payment Conditioned on Substantial Delivery of Usable Product, for special payment requirements.

CLIN’s	SUPPLIES/SERVICES	QTY/ UNIT	UNIT PRICE			EXTENDED PRICE
	THE BELOW ITEMS ARE FIRM FIXED PRICE, INCLUDED IN THE BASE PRICE PER DELIVERED DOSE:
0001	[***]	[***]	$	[***	]	$	[***	]
0002	[***]	[***]	$	[***	]	$	[***	]
0003	[***]	[***]	$	[***	]	$	[***	]

2. ESTIMATED COST AND FIXED FEE (CPFF)

In consideration for completion of the work to be performed under CLINs 0004, 0005, and 0006, as shown below, and in accordance with the Statement of Work, it is estimated that the total cost to the Government for full performance of this contract will be $[***], of which the sum of $[***] represents the estimated reimbursable costs and $[***] represents the fixed-fee. These amounts also represent the total amount of funds currently available for payment and allotted under the CPFF portion of this contract. It is estimated that this amount will cover performance of the contract through the expiration date. See Section F, Paragraph F.2. on the contract’s period of performance.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

CLIN’s

SUPPLIES/SERVICES

EST. COST

FIXED
FEE

TOTAL
EST. CPFF

0004

[***]

[***

]

[***

]

[***

]

0005

[***]

[***

]

[***

]

[***

]

0006

[***]

[***

]

[***

]

[***

]

B. CONTRACT OPTIONS

1. FIRM FIXED PRICE (FPP)

If the Government exercises its option pursuant to Section H, Paragraph H.14. of this contract, the price of the contract may be increased as shown in the below CLIN’s 0007, 0008, 0009 and 0010 in consideration for completion of the work described in the individual CLIN’s and in accordance with the Statement of Work:

CLIN’s	DESCRIPTION	UNITS	UNIT PRICE			TOTAL
0007	[***]	[***]	$	[***	]	To be Determined (TBD)
0008	[***]	[***]	$	[***	]	TBD
0009	[***]	[***]	$	[***	]	TBD
0010	[***]	[***]	$	[***	]	TBD

2. ESTIMATED COST AND FIXED FEE (CPFF)

If the Government exercises its option pursuant to Section H, Paragraph H.14. of this contract, the Government’s total obligation represented by the sum of the estimated cost plus fixed fee may be increased as shown in the below CLIN’s 0011, 0012, 0013, 0014 and 0015 in consideration for completion of the work described in the individual CLIN’s and in accordance with the Statement of Work:

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

CLIN’s

DESCRIPTION

EST. COST

FIXED FEE

TOTAL
EST. CPFF

0011

[***]

[***

]

[***

]

[***

]

0012

[***]

[***

]

[***

]

[***

]

0013

[***]

[***

]

[***

]

[***

]

0014

[***]

[***

]

[***

]

[***

]

0015

[***]

[***

]

[***

]

[***

]

B.3. PROVISIONS APPLICABLE TO DIRECT COSTS

This paragraph applies only to the cost reimbursable CLIN’s. Notwithstanding the clauses, ALLOWABLE COST AND PAYMENT and FIXED FEE, incorporated in this contract, unless authorized in writing by the Contracting Officer, the cost of the following items or activities shall be unallowable as direct costs: 1) Acquisition. by purchase or lease, of any interest in real property; 2) Special rearrangement or alteration of facilities: 3) Purchase or lease of any item of general purpose office furniture or office equipment regardless of dollar value; 4) Subcontract Costs; and 5) Accountable Government Property..

B4. ADVANCE UNDERSTANDINGS

1. Milestones for Advance Payments and Performance Based Payment

I. [***]% Project BioShield Advance Payment - $[***]

A. The HHS Secretary has determined that an advance payment is necessary to ensure success of this project, and has authorized a [***]% advance payment in accordance with 42 USC 247d-6b(c)(7)(C)(ii)(I) PAYMENT CONDITIONED ON DELIVERY. This [***]% advance payment equates to $[***], and is required to be repaid if there is a failure to perform by the Contractor under the contract.

Nothing in the PAYMENT CONDITIONED UPON DELIVERY subclause shall be construed as affecting the rights of vendors under provisions of law or regulation (including the Federal Acquisition Regulation) relating to the termination of contracts for the convenience of the Government

B. Completion of all the below tasks is required prior to the issuance of an advance payment. All of the below tasks shall be submitted to the Project Officer and Contracting Officer and are subject to Government review and concurrence. The Contractor may invoice the entire [***]% advance payment of $[***] after all of the below tasks have been achieved.

[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

2. Payment Schedule — Adjustments for Advance Payments and Withholdings for Achievement of Licensure and Five Year Stability Data

Below is a billing schedule with unit pricing for the following factors: advance payments; Performance Based Payments (PBP); vaccine deliveries made pre-BLA; vaccine deliveries made post-BLA; payments after licensure is achieved (l0% withholding): and payment after achievement of Five (5) year stability data:

Cost per
Dose

Pre-BLA
Deliveries

Post BLA
Deliveries

10%
Licensure

Five (5) Year
Stability Data

Advance Payments
and Performance
Based Payment
(PBP)

Advance Payments and PBP

[***

]

[***

]

[***

]

[***

]

[***

]

[***

]

CLIN 0001 Vaccine

[***

]

[***

]

[***

]

[***

]

[***

]

[***

]

CLIN 0002 Stability Testing

[***

]

[***

]

[***

]

[***

]

[***

]

[***

]

CLIN 0003 Regulatory Submissions

[***

]

[***

]

[***

]

[***

]

[***

]

[***

]

Subtotal Dose Unit Pricing

[***

]

[***

]

[***

]

[***

]

[***

]

[***

]

3. Economic Price Adjustment - PPI Increases to Subcontractor Prices

a. Manufacture of the fixed price product required includes subcontractor costs for filling and finishing. In accordance with standard industry practice, subcontract prices for filling and finishing are adjusted annually to reflect changes in the Producer Price Index (PPI). The contractor certifies that this contract does not include amounts to cover such adjustments beyond the second year of contract performance.

b. The Contractor shall notify the Contracting Officer if, during or after the second year of contract performance, the awardee’s subcontractor(s) request price adjustments from the prime contractor (awardee) applicable to product produced during any year beyond year 2 of the contract. The Contractor shall furnish this notice within 60 days after the price adjustment or within any additional period that the Contracting Officer may approve in writing, but not later than the date of final payment under this contract. The notice shall include the Contractor’s proposal for an adjustment in the contract unit prices of the contract. Such proposal shall include supporting data explaining the effective date, the amount of change in the PPI between the date of this contract and the effective date of the increase, the subcontractor pricing to which the PPI changes apply, and the number of doses to which the adjustment will apply, whether such doses have been shipped before the notification or will be shipped in the future.

c. Promptly after the Contracting Officer receives the notice and data referred to in the previous paragraph of this clause, the Contracting Officer and the Contractor shall negotiate a price adjustment in the contract unit prices and its effective date. The Contractor shall continue performance pending agreement on, or determination of, an adjustment and its effective date. The Contractor shall submit a separate invoice for the adjustment amount applicable to doses previously shipped, if any, and the unit price will be adjusted to reflect the change applicable to undelivered product.

d. Any price adjustment under this clause is subject to the following limitations:

i. Any adjustment shall be limited to the actual amount of change in the PPI, but not to exceed $[***]. There shall be no adjustment for supplies or services for which the production cost is not affected.

ii. No adjustment shall apply to supplies that are delivered before the effective date of the adjustment.

SECTION C - DESCRIPTION/SPECIFICATIONS

C.1. STATEMENT OF WORK

A. Purpose

The primary purpose of this contract is the acquisition of 20 million doses (in single-dose vials) of MVA vaccine for the Strategic National Stockpile (SNS). The primary use of this vaccine will be for prophylaxis of individuals considered to be at risk for smallpox.

B. Scope of Work — Base Contract

Independently, and not as an agent of the USG, the Contractor shall furnish all the necessary services, qualified personnel, materials, supplies, equipment, facilities, transportation and travel not otherwise provided by the USG as required to:

a) Manufacture and deliver to the SNS 20 million doses of usable MVA vaccine within 60 months of the Contract Award date (for definition of “usable” see Specific Technical Requirements below). The vaccine shall be provided in single-dose vials in a frozen liquid suspension. The Sponsor, with concordance from the FDA/CBER, shall propose an optimal titer of virus per dose and formulation of vaccine as determined in Phase 2 studies sponsored by the National Institute of Allergy and Infectious Diseases (NIAID).

b) Perform accelerated stability assessments to support transport and point-of-use storage. Conduct real-time stability assessments to support the proposed dating periods of the Bulk Drug Substance (BDS) and the Final Drug Product (FDP) at the proposed storage temperature. Perform ongoing stability assessments to support extension of the product dating period;

c) Conduct supportive clinical trial(s) and animal studies to support an EUA, as specified by the FDA/CBER, for prophylaxis of immunocompromised individuals considered to be at risk for smallpox;

d) Conduct Phase 3 clinical triaI(s) and animal studies, as per FDA/CBER regulations, to support licensure of the product for post-exposure prophylaxis of healthy individuals considered to be at risk subsequent to a known or suspected smallpox virus release, including demonstration of safety and efficacy of an optimized dosing regimen, single or two-dose, based on supporting data to justify such a regimen;

e) Obtain FDA/CBER licensure for the clinical indication of post-exposure prophylaxis of healthy individuals considered to be at risk subsequent to a known or suspected smallpox virus release, including post-licensure approval for use in pediatric and geriatric subjects; and

f) Perform shipping, validation studies, and quality control and quality assurance monitoring on product in the SNS through the end of the contract.

C. Specific Technical Requirements for Base Contract— Advanced Development and Licensure of MVA Vaccine

The Contractor shall perform all the work required to manufacture and obtain FDA/CBER approval of a licensed MVA vaccine for use in healthy populations. Payments to the Contractor will be solely dependent on the delivery to the SNS of MVA vaccine supported by a sufficient body of safety, efficacy, and cGMP manufacturing data, as determined by FDA/CBER. that may support its use under an EUA for immunocompromised persons, as noted below.

Definition of Usable Product: It is expected that the Contractor will work closely with FDA/CBER to fully define, establish, and fulfill criteria recommended by FDA/CBER (in the most recent “Current Thinking” document shared with the contractor) for product to be considered for potential use during an emergency. There must be a high degree of confidence. as determined by the FDA/CBER, that all manufactured units of FDP from successive lots made at commercial scale will meet acceptable product specifications as demonstrated by satisfactory in-process and release testing. We refer the Contractor to FDA/CBER regarding the data recommended in support of the potential use of MVA vaccines under an EUA for immunocompromised persons who are otherwise contraindicated to receive live-replicating smallpox vaccines. An ongoing stability program must be in place using stability indicating assay(s) that has been agreed upon by FDA/CBER. The product must meet defined stability specifications to the satisfaction of BARDA and FDA/CBER prior to entry into the SNS (as indicated in requirement

2b). Acceptance of FDP for inclusion into the SNS for potential emergency purposes will be based an the Contractor’s submission of required regulatory documentation to their IND with FDA/CBER for review and determination that the minimal product requirements have been met for potential emergency use. Subsequently. the Contractor shall submit the regulatory documentation to CDC to facilitate their preparation of a pre-EUA submission to FDA/CBER. The Contractor shall also conduct longer term studies on an on-going basis as needed for licensure, and incorporate the requirements shown below into a work plan and timeline.

Requirement 1 - Vaccine Production and cGMP Compliance

a) The Contractor shall manufacture and deliver to the SNS MVA vaccine manufactured in accordance with cGMPs throughout the period of performance. The Contractor shall deliver 20 million doses of usable FDP within 60 months of contract award. The BDS and FDP shall be manufactured using cGMPs and meet the specifications determined by the FDA/CBER for licensure.

b) The Contractor shall provide all information requested to the Project Officer and/or the FDA/CBER in order to facilitate a cGMP inspection at the time of production of vaccine lots destined for the SNS.

c) The Contractor shall develop a labeling strategy in consultation with CBER to allow case of transition from IND to licensed product.

d) The Contractor shall provide primary and secondary points of contact that will be available 24 hours per day, seven days per week, to be notified in case of a public health emergency.

Requirement 2 - Assay Validation and Stability Testing of Finished Vaccine

a) The Contractor shall validate critical assays necessary for BDS and FDP release and stability testing. to assess immune response parameters for animals and humans, and for potency evaluation. Validation of all assays will be required for licensure; however, FDA/CBER will determine the validation of critical assay parameters for product use under an EUA to be utilized in the case of a smallpox public health emergency. Validated analytical procedures shall be used irrespective of whether they are for in-process, release, immunogennicity and stability testing. Each quantitative analytical procedure shall be designed to minimize assay variation. Formal quality unit review of analytical test results shall be performed according to established quality standards and procedures.

b) The Contractor shall conduct accelerated and real-time stability studies, including potency testing. on the BDS lots stored by the Contractor and FDP lots placed in the SNS in conformance with FDA/CBER requirements throughout the contract lifetime. Storage temperature conditions of the FDP should be developed and tested with consideration given to the most cost-effective storage and deployment requirements for the SNS. Testing will be performed in accordance with current regulatory guidelines to support an expiry dating period of no less than 36 months.

c) The Contractor shall perform stability studies, including potency testing, to extend the product expiry dating period to at least five years and request an extension of the dating period from FDA/CBER in a license supplement, as appropriate.

d) At the discretion of the USG and independent of testing conducted by the Contractor, the USG reserves the right to conduct inspections and collect samples of product held by the Contractor and in the SNS.

Requirement 3 - Design of Safety, Efficacy, and Immunogenicity Studies, Including Execution of Studies to Support EUA.

a) The Contractor shall develop and submit non-clinical and clinical study plans to support an EUA for post-exposure prophylaxis of immunocompromised individuals considered to be at risk for smallpox.

b) In addition, the Contractor shall develop, submit, and execute non-clinical and clinical plans to demonstrate safety and efficacy under the Animal Efficacy Rule (21 CFR 601.91) and human safety and immunogenicity studies adequate for U.S. licensure. These plans shall be designed in consultation with appropriate USG agencies and should support the licensure of MVA for prophylaxis or healthy individuals considered to be at risk for smallpox. Further, these plans will include studies to demonstrate safety and efficacy of an optimized dosing regimen, single or two-dose, based on supporting data to justify such studies.

c) The Contractor shall submit a Phase 4 post-marketing plan, which should describe in general terms the collection of safety and efficacy data when the product is used in the event of an emergency, which warrants its use. The actual Phase 4 study shall be developed in consultation with FDA/CBER when they think such study proposal is appropriate for submission and review.

Requirement 4 - Conduct of Safety and Efficacy Studies

The Contractor shall initiate and complete Phase 3 clinical trial(s) in support of a Biologics License Application for use of MVA. The initial BLA indication will be for post-exposure prophylaxis of healthy individuals considered to be at risk subsequent to a known or suspected smallpox virus release.

a) All trials shall utilize usable vaccine and initiate only upon approval by the Project Officer and acceptance of plans and protocols by FDA/CBER.

b) The initial BLA should cover both genders within the age range of 18-55 years using the optimal dose regimen and schedule for prophylaxis. Given the uncertainty of the size of the expected Phase 3 trials, CLIN 0001D covers Phase 3 studies up to 3000 human subjects and Optional CLIN 0007 contain, pricing for each group of 100 additional subjects.

c) Vaccine efficacy shall be demonstrated with usable product in at least two animal models as per 21 CFR 601.91. (FDA Animal Rule) regulations.

Requirement 5 - Regulatory Submissions

a) To conduct Phase 3 clinical trials, the Contractor shall prepare and submit to the FDA/CBER, the required regulatory submissions (as they pertain to the IND and/or any Drug Master File(s) as specified in, but not limited to, 21 CFR 312, 314.420, and 601) for lot consistency, safety, and immunogenicity in normal, healthy volunteers. Such volunteers may be integrated with any ongoing clinical trial(s) for the clinical indication of post-exposure prophylaxis of healthy individuals considered to be at risk, subsequent to a known or suspected smallpox virus release. Further, it is anticipated that the Contractor will provide the necessary data to CDC to support the submission of an EUA.

b) The Contractor shall prepare and submit an original BLA for MVA vaccine in order to obtain FDA/CBER licensure for post-exposure prophylaxis of healthy individuals considered to be at risk subsequent to a known or suspected smallpox virus release. The Contractor shall review the criteria for Fast Track designation, consult with FDA/CBER, and then seek such designation during the IND stage for this indication, if appropriate. At the pre-BLA meeting, the Contractor shall request priority status for review of the MVA vaccine BLA for this indication, if appropriate, to allow a “rolling BLA” (i.e. review of the BLA will start before all parts of the BLA have been submitted).

c) All regulatory submissions must comply with current FDA/CBER regulations and policies. The Contractor shall include the Project Officer on all communications with FDA/CBER.

Requirement 6 - Shipment to SNS and Short-Term Storage

a) The Contractor will assume responsibility for the cost of shipping finished product to the SNS for long-term storage once usable product requirements have been met. The USG will assume responsibility for long-term storage of the finished product, and emergency distribution of the finished product. The USG shall incur only the storage costs while the product is held within the USG’s control. The product shall be stored in compliance with cGMP at the Contractor’s facility until the delivery of finished product to the SNS.

b) The Contractor shall ensure that vaccine delivery follows cGMPs to maintain the integrity of the product en route. The Contractor shall perform/execute all necessary pilot transfers and validate the shipping method that will be used for

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

delivery to the SNS prior to first shipment of product. The Contractor shall tile the necessary documentation to the FDA/CBER for the safe movement of the product to include any protocol deviations en route.

c) The Contractor shall be responsible for the secure and segregated storage of held intermediates and the FDP prior to lot release and subsequent arrival at the SNS. The Contractor may also be required to store FDP at its own facility for up to three months. The Contractor may propose a delivery schedule that may not exceed 1 delivery per month. Thirty days advance notice is required prior to shipment to the SNS. However, while the product is in long-term storage with the USG (i.e., in the SNS), the Contractor shall continue to be responsible for all quality control/quality assurance monitoring and subsequent reporting necessary to insure appropriate storage conditions of the product until said product is licensed. The Contractor, via this contract with the USG, will be expected to establish a written Quality Agreement as to the manner in which the product will be stored within the specific USG stockpile facility (ies) that have been identified post contract award. In addition, this Quality Agreement will outline the responsibilities of both the Contractor and the USG (i.e., SNS-Quality Control). These documents shall be drafted and signed by both parties prior to the transport and storage of the product.

Requirement 7 - Disposition of Vaccine Inventory

Upon expiration or termination (including partial termination) of this contract, the USG may effect final distribution of any vaccine remaining in storage at the Contractor’s facility by any one or combination of the following methods:

a) The USG may elect to direct the Contractor to ship to a consignee(s) designated by the USG, all vaccine remaining in storage at the Contractor’s facility.

b) The USG may offer the vaccine to be repurchased by the Contractor at the original purchase price.

c) The USG may elect to request the Contractor to destroy the vaccine in storage at the Contractor’s facility. If the Contractor is required to destroy the vaccine, an equitable adjustment may be required.

The USG may elect to handle disposition of expired vaccines by any one or a combination of the following methods:

a) The USG may elect to request the Contractor to ship all expired vaccines and vaccines scheduled to expire within 30 calendar days to the USG to the location specified by the USG.

b) The USG may elect to request the Contractor to destroy the BDS or FDP in storage at the Contractor’s facility. If the Contractor is required to destroy the product in storage at the Contractor’s facility, an equitable adjustment may be required.

Nothing in this requirement 7 shall be interpreted to affect the Governments rights pursuant to the following clauses:

FAR 52-249-2 and 52.249-8.

Requirement 8 - Security of Contract Operations

[***]

D) CONTRACT OPTIONS

OPTIONS: The Government may exercise any of the below items. Exercise of an option will also extend the contract period of performance by up to five (5) years.

1. Produce, release, maintain and monitor the minimum number of lots per year of BDS, and fill/finish the corresponding lot(s) of FDP, at commercial scale to maintain vaccine cGMP capability (warm base) for the life of the contract extension.

2. Manufacture and deliver to the SNS up to an additional 60 million doses of the MVA vaccine provided in single-dose vials as a frozen liquid suspension. Consideration by the USG for this option will be based on safety, efficacy, and cost information to support use of MVA vaccine in individuals contraindicated for vaccination with live, replication-competent smallpox vaccines. For example, as posted on the NIAID website, safety and immunogenicity data may be obtained in individuals infected with HIV.

a. The BDS and FDP shall be manufactured under cGMP conditions and meet the specifications determined by the FDA/CBER for licensure (Requirement 1a, IV. Specific Technical Requirements).

b. The Contractor shall provide all information requested to the Project Officer and/or the FDA/CBER in order to facilitate a cGMP inspection at the time of production of vaccine lots destined for the SNS (Requirement 1b, IV. Specific Technical Requirements).

3. Add study subjects for the initial BLA, on a Fixed Price basis for each group of IDD additional subjects. Subjects shall cover both genders within the age range of 18-55 years using the optimal dose regimen and schedule for prophylaxis.

4. Conduct post-licensure studies to extend the range of ages for which the vaccine is indicated, to include pediatric and geriatric subjects. The Contractor shall prepare and submit a supplement to the BLA for MVA vaccine in order to extend the range of ages for post-exposure prophylaxis of healthy individuals considered to be at risk subsequent to a known or suspected smallpox virus release, to include pediatric and geriatric subjects.

5. Conduct Phase 3 clinical trial(s) in support of a Biologics License Application Supplement for expanded use of MVA. The expanded clinical indication will be for post-exposure prophylaxis of immunocompromised individuals considered to be at risk subsequent to a known or suspected smallpox virus release.

a. All studies shall utilize vaccine manufactured by the final scale process and shall initiate only upon Project Officer approval and acceptance of plans and protocols by FDA/CBER (Requirement 4a, IV. Specific Technical Requirements);

b. Obtain approval for a BLA Supplement for the expanded indication using the optimal dose regimen and schedule for prophylaxis;

c. The Contractor shall initiate Phase 4 post-marketing studies in the immunocompromised population. As noted in the ‘`Animal Rule,” the Contractor shall conduct post-marketing studies, such as field studies, to verify and describe the biological product’s clinical benefit and to assess its safety when used as indicated when such studies are feasible and ethical. Such post-marketing studies would not be feasible until an exigency arises. When such studies are feasible, the Contractor shall conduct such studies as mandated by CBER with due diligence and in coordination with the CDC.

6. The Contractor shall conduct real-time stability studies, including potency testing, on the BDS lots stored by the Contractor and all FDP lots placed in the SNS in conformance with FDAICBER requirements beyond the base period of the contract (Requirement 2b and 2c, IV. Specific Technical Requirements) and obtain approval for a BLA Supplement to extend the expiry dating period as appropriate.

7. The Contractor shall initiate Phase 4 post-marketing studies in healthy individuals. As noted in the “Animal Rule,” the Contractor shall submit a plan for conducting post-marketing studies at the time of license application in consultation with FDA/CBER. These post-marketing studies, when such studies are feasible and ethical, should include field studies, so as to verify and describe the biological product’s clinical benefit and to assess its safety when used as indicated. Such post-marketing studies would not be feasible until an exigency arises. When such studies are feasible, the Contractor shall conduct such studies with due diligence.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

8. Add to the duration of storage of the FDP at the Contractor’s own facility, beyond the three (3) months period specified in Requirement 6(c) of the Base contract. This is on a Fixed Price basis for each [***].

9. Rental of additional vaccine storage trailer as needed for optional doses of vaccine. This is on a Fixed Price basis for each additional [***] doses of FDP per trailer.

C.2. REPORTING REQUIREMENTS AND DELIVERABLES

A. Deliverables

1. Base Contract Deliverables:

(1) A minimum of 20 million single-dose vials of usable MVA vaccine (see Section 2. Specific Technical Requirements) in frozen liquid suspension to be delivered to the SNS to support use under an EUA, for immunocompromised individuals, to be delivered within 60 months of the contract award date.

(2) An FDA/CBER approval letter for the BLA for WA vaccine for post-exposure prophylaxis of healthy adult individuals considered to be at risk subsequent to a known or suspected smallpox virus release.

(3) Evidence, including a summary of salient results, of an ongoing Quality Control/Quality Assurance Program for the monitoring of SNS stored product and ongoing stability testing of the retained lots of product in SNS over the life of the contract or the expiration date of the vaccine, or until vaccine is used, whichever comes First.

(4) A security plan that has received Government concurrence in advance of initiating work at any facility performing under this contract.

(5) Written Quality Agreement between the Contractor and the SNS Quality Control Unit within 6 months of award.

2. Optional Contract Deliverables:

(1) One (1) lot per year of BDS. and corresponding fill/finish of the FDP, at commercial scale for the life of the contract in order to maintain cGMP capability.

(2) Up to 60 million single-dose vials of usable MVA vaccine (see Section 2. Specific technical requirements) in frozen liquid suspension to be delivered to the SNS to support use under an EUA and subsequent licensure.

(3) An FDA/CSER approval letter for a BLA license supplement for an expanded clinical indication including use in immunocompromised individuals.

(4) An FDA/CBER approval letter for a BLA license supplement to extend the FDP expiry dating period.

(5) A FDA/CBER supplement approval letter for use in pediatric and geriatric subjects.

(6) Evidence, including a summary of salient results, of an ongoing Quality Control/Quality Assurance Program for the monitoring of SNS stored product and ongoing stability testing of the retained lots of product in SNS for the duration of the contract option,

(7) Clinical reports of post-marketing studies for both healthy and immunocompromised individuals. These post-marketing studies, when such studies are feasible and ethical, should include Field studies, so as to verify and describe the biological product’s clinical benefit and to assess its safety when used as indicated. Such post-marketing studies would not be feasible until an exigency arises.

B. Technical Reports

In addition to those reports required by other terms of this contract, the Contractor(s) shall submit to the Contracting Officer and the Project Officer technical progress reports covering the work accomplished during each reporting period on a periodical basis as established by the Project Officer. These reports are subject to the technical inspection and requests for clarification by the Project Officer. These reports shall be brief and factual and prepared in accordance with the following format:

(1) Monthly Technical Progress Reports: On the fifteenth of each month for the previous calendar month, the Contractor shall submit a Monthly Technical Progress Report to the Project Officer and the Contracting Officer. A monthly report will not be required for the period when the final report is due. The Contractor shall submit one copy of the Monthly Progress Report electronically via e-mail. Any attachments to the e-mail report shall be submitted in Microsoft Word, Excel, Project or compatible versions. Such reports shall include the following specific information:

The contract number and title, the period of performance being reported, the Contractor’s name and address, the author(s), and the date of submission:

The Monthly Progress Report shall include an Executive Summary (Section 1.0) in MS PowerPoint format, highlighting the progress, issues, and actions relevant to each of the above items and cross-referenced to the Critical Path Gantt Chart.

The report shall detail the planned progress and actual progress during the period covered, explaining why any differences between the two occurred, and if behind schedule what corrective steps and actions are planned. The project’s plans and schedule must reflect FDA regulatory requirements and guidance. The monthly report shall include the information listed below that is applicable for the performance period during the month being reported:

a) Progress in assay development and validation, and process development and validation of Bulk Drug Substance (BDS) and Final Drug Product manufacture to support scale up to full production capacity, including raw material procurement status;

b) Quality control/quality assurance monitoring:

c) FDA/CBER inspections and consultation results or recommendations;

d) Storage and stability studies for expiration date results (accelerated, stress, and long-term storage conditions); c) Security assessment, problems and recommendations;

f) Progress, results, and final reports of expanded human safety studies;

g) Progress, results, and final reports of efficacy studies performed in animals if following the Animal Rule, or clinical studies required for Accelerated Approval;

h) Progress, results, and final reports of any other studies deemed necessary by FDA/CBER;

i) Progress in providing data to CDC to support CDC submission of an EUA to be utilized in the case of a smallpox event:

j) Progress in obtaining FDA/CBER approval/licensure for post-exposure prophylaxis of healthy individuals considered to be at risk subsequent to a known or suspected smallpox virus release;

k) Progress in execution of any product disposition directions provided by the USG;

I) Progress, results, and final reports of any necessary additional animal and human studies to obtain expanded labeling in special populations, including pediatric and geriatric populations:

m) Potency and stability testing results;

n) Inventory report of total number of vaccine syringes in storage during the month, to include: lot number, expiration date, and bulk quantity (if applicable);

o) Quantity of out-of-date FDP, assessment and recommendations to replacement FDP orders to maintain required stockpile quantities;

p) Physical storage facilities (Contractor and SNS) assessments;

q) Overall project assessment, problems encountered and recommended solutions, etc.

r) Update to risk mitigation plan (every six months)

The following Format shall be used for preparation of the Monthly Progress Report:

1.0 Executive Summary

2.0 In-Process, Release, and Stability Assays

3.0 Bulk Manufacture

3.1 Process Development and Validation

3.2 Quality Assurance

4.0 Final Drug Product Manufacture

4.1 Process Development and Validation

4.2 Quality Assurance

5.0 Nonclinical Development

6.0 Clinical Development

7.0 Regulatory Strategy and Submissions

7.1 Submissions

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SECTION D—PACKAGING, MARKING AND SHIPPING

1. Report Deliverables

Unless otherwise specified by the Contracting Officer or the Contracting Officer’s representative, delivery of reports to be furnished to the government under this contract (including invoices), shall be addressed as follows:

[***]

2. Contract Deliverables

Shipment of deliverables to SNS and Short-Term Storage shall be performed in accordance with Section C, under C.1. BACKGROUND/STATEMENT OF WORK, Part C, Requirement 6.

SECTION E—INSPECTION AND ACCEPTANCE

FAR Clauses

1. FAR Clause No.52.246-2, INSPECTION OF SUPPLIES — FIXED PRICE (AUG 1996)

2. FAR Clause No.52.246-9, INSPECTION OF RESEARCH AND DEVELOPMENT (SHORT FORM) (APR 1984)

3. FAR Clause No.52.246-16, RESPONSIBILITY FOR SUPPLIES (APR 1984)

E.I. INSPECTION AND ACCEPTANCE (JUL 1999)

Inspection and acceptance of the article, services and documentation called for herein shall be accomplished by the Contracting Officer or his duly authorized representative (who for the purposes of this contract shall be the Project Officer) at the destination of the article, service of documentation.

(end of clause)

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SECTION F—DELIVERIES OR PERFORMANCE

FAR Clauses

1. FAR Clause No. 52.242-15, STOP-WORK ORDER (AUGUST 1989) with ALTERNATE I (A.PR 1984

2. FAR Clause 52.242-17. GOVERNMENT DELAY OF WORK (APRIL 1984)

F.1. PLACE AND METHOD OF DELIVERY

a. Delivery of smallpox MVA vaccine required in CLIN 0001 shall be in accordance with FAR 52.247-35 entitled F.O.B. DESTINATION, WITHIN CONSIGNEES PREMISES (APR 1984).

b. Place of Delivery: The product shall be delivered to a Strategic National Stockpile (SNS) site(s) to be announced at time of delivery.

F.2. PERIOD OF PERFORMANCE

The period of performance of this contract is from the date of contract award to 5 years after contract award. Exercise of an option will extend the contract period of performance by up to five (5) additional years.

F.3. TECHNICAL REPORT REQUIREMENT

Item	Deliverable	Quantity	Due Date
1.	Technical Monthly Progress Report	1 Electronic Copy — Project Officer (PO) 1 Electronic Copy — Contracting Officer (CO) 1 Hard Copy - CO	30 days after contract award and by the 15th day of each month during the contract’s period of performance. Not due when Final is due.
2.	Final Report	1 Electronic Copy — P.O. 1 Electronic Copy — C.O. 1 Hard copy - CO	Due on/before the completion date of the contract.

F.4. CONTRACT DELIVERABLES

A. Base Contract Requirements

Milestones	Deliverable	Quantity	Due Date
1.	Usable MVA Vaccine, in accordance with (IAW) C.2., Item A.1(1)	20 million doses	Sixty (60) months after contract award
2.	FDA/CBER approval letter for the BLA for MVA vaccine for post-exposure prophylaxis of healthy adult individuals, IAW C.2., Item A.1(2)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	To be determined by Contracting Officer based upon clinical trial results and CBER review
3.	Evidence of an ongoing Quality Control/Quality Assurance Program, including a summary of salient results, IAW C.2., Item A.1(3)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	[***]
4.	Final Security Plan, IAW C.2., Item A.1(4)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	[***]
5.	Written Quality Agreement between the Contractor and the SNS Quality Control Unit, IAW C.2., Item A.1(5)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

B. Optional Contract Requirements

Milestones	Deliverable	Quantity	Due Date
1.	Filled and finished FDP corresponding to one (1) lot per year of BUS, IAW C.2., Item A.2.(1)	Annual deliveries	To be determined upon mutual agreement between Contractor and Contracting Officer
2.	Up to 60 million additional single-dose vials of usable VIVA vaccine, IAW C.2., Item A.2.(2)	To be determined	To be determined upon mutual agreement between Contractor and Contracting Officer
3.	FDA/CBER approval letter for BLA license supplement for an expanded clinical indication to include immunocompromised individuals, IAW C.2., Item A.2.(3)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	To be determined by Project Officer based upon clinical trial results and CBER review
4.	FDA/CBER approval letter for BLA license supplement to extend the FDP expiry dating period. TAW C.2., ITEM A.2.(4)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	To be determined
5.	FDA/CBER supplement approval letter for pediatric and geriatric subjects, IAW C.2., Item A.2(5)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	To be determined by Contracting Officer based upon clinical trial results and CBER review
5.	Evidence of an ongoing Quality Control/Quality Assurance Program, including a summary of salient results, IAW C.2., Item A.2(6)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	[***]
6.	Clinical reports of post-marketing studies for health and immunocompromised individuals. IAW C.2., Item A.2(7)	1 Hard Copy to PO 1 Electronic Copy to PO 1 Electronic Copy to CO	To be determined by Contracting Officer

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SECTION G.—CONTRACT ADMINISTRATION DATA

G.1. PROJECT OFFICER

The following Project Officer and Alternate Project Officer will represent the Government for the purpose of this contract:

[***]

Performance of the work hereunder shall be subject to the technical directions of the designated Project Officer and Co-Project Officer for this contract.

As used herein, technical directions are directions to the Contractor, which fill in details, suggests possible lines of inquiry, or otherwise completes the general scope of work set forth herein. These technical directions must be within the general scope of work, and may not alter the scope of work or cause changes of such a nature as to justify an adjustment in the stated contract price/cost, or any stated limitation thereof. In the event that the Contractor feels that full implementation of any of these directions may exceed the scope of the contract, he or she shall notify the originator of the technical direction and the Contracting Officer in a letter separate of any required report(s) within two (2) weeks of the date of receipt of the technical direction and no action shall be taken pursuant to the direction. If the Contractor fails to provide the required notification within the said two (2) week period that any technical direction exceeds the scope of the contract, then it shall be deemed for purposes of this contract that the technical direction was within the scope. No technical direction, nor its fulfillment, shall alter or abrogate the rights and obligations fixed in this contract.

A Government Project Officer is not authorized to change any of the terms and conditions of this contract. Changes shall be made only by the Contracting Officer by properly written modilication(s) to the contract. Any changes in Project Officer delegation will be made by the Contracting Officer in writing with a copy being furnished to the Contractor.

G.2. KEY PERSONNEL

This paragraph applies to the cost-reimbursement portion of this contract. Pursuant to the Key Personnel clause incorporated in Section I of this contract, the following individual is considered to be essential to the work being performed hereunder:

Name		Position
[***]		[***]

G3. PAYMENT BY ELECTRONIC FUNDS TRANSFER — CENTRAL CONTRACTOR REGISTRATION OR FAR 52.232-33 PAYMENT BY ELECTORNIC FUNDS TRANSFER — OTHER TRANSATIONS (MARCH 2004)

(a) The Government shall use cicctronic funds transfer to the maximum extent possible when making payments under this contract. FAR 52.232-34, Payment by Electronic Funds Transfer in Section I, requires the contractor to designate in writing a financial institution for recap of electronic funds transfer payments.

(b) The contractor shall make the designation by submitting the form titled “ACH Vendor/Miscellaneous Payment Enrollment Form” This form may be obtained by contacting the Contracting Officer.

(c) In cases where the contractor has previously provided such designation, i.e., pursuant to a prior contract/order, and has enrolled in the program, the form is not required.

(d) The competed form shall be forwarding to the Contracting Officer, no later than 14 calendar days before an invoice is submitted.

G.4. INVOICE SUBMISSION (JULY 1999)

(a) The Contractor shall submit an original and two copies of contract invoices to the address shown below:

DHHS/OS/ASPR/BARDA

Attn: Contracting Officer

330 Independence Ave., S.W.

Room G640

Washington, D.C. 20201

(b) The Contractor agrees to include (as a minimum) the fallowing information on each invoice for firm fixed price CLIN’s:

(1) Contractor’s Narne &Address
(2) Contractor’s Tax Identification Number (TIN)
(3) Contract Number
(4) Invoice Number
(5) Invoice Date
(6) Contract Line Item Number
(7) Quantity
(8) Unit Price & Extended Amount for each line item
(9) Total Amount of Invoice
(10) Name, title and telephone number of person to be notified in the event of a defective invoice
(11) Payment Address, if different from the information in (c)(1).

(End of Clause)

Invoice Submission — (Cost-Plus Fixed-Fee CLIN’s)

(a) Contractor voucher requests for reimbursement shall conform to the form, format, and content requirements of the Billing Instructions for Negotiated Cost Type Contracts, made a part of the contract in Section J.

(b) The Contractor shall, in addition to the above requirements, submit a detailed breakout of costs as supporting backup and shall place the following signed Contractor Certification on each invoice/voucher submitted under this contract:

I certify that this voucher reflects (fill in Contractor’s name) request for reimbursement of allowable and allocable costs incurred in specific performance of work authorized under Contract (fill in contract number)/Task (fill-in task order number, if applicable), and that these costs are true and accurate to the best of my knowledge and belief.

(Original Signature of Authorized Official)
Typed Name and Title of Signatory

(c) The date of receipt of a proper invoice/voucher by the Contracting Officer shall be used for the purpose of Prompt Payment Act time computations.

(End of Clause)

G.5. REIMBURSEMENT OF COST (Apr 2000)

(a) For the performance of the cost-reimbursement portion of this contract, the Government shall reimburse the Contractor the cost determined by the Contracting Officer to be allowable (hereinafter referred to as allowable cost) in accordance with the clause entitled Allowable Cost and Payment in Section I, Contract Clauses. Examples of allowable costs include, but are not limited to, the following:

(1) All direct materials and supplies that are used in the performing of the work provided for under the contract, including those purchased for subcontracts and purchase orders.

(2) All direct labor, including supervisory, that is properly chargeable directly to the contract, plus fringe benefits.

(3) All other items of cost budgeted for and accepted in the negotiation of this basic contract or modifications thereto.

(4) Special expenditures which, upon request from the Contractor, the Contracting Officer approves as being an allowable cost under this contract, such as purchase or lease of office furniture or equipment, etc..

(5) All travel costs plus per diem or actual subsistence for personnel while in an actual travel status in direct performance of the work and services required under this contract. These costs will be in accordance with the Contractor’s policy and subject to the following:

(i) Air travel shall be by the most direct route using “air coach” or “air tourist” (less than first class) unless it is clearly unreasonable or impractical (e.g., not available for reasons other than avoidable delay in making reservations, would require circuitous routing or entail additional expense offsetting the savings an fare, or would not make necessary connections).

(ii) Rail travel shall be by the most direct route, first class with lower berth or nearest equivalent.

(iii) Costs incurred for lodging, meals, and incidental expenses shall be considered reasonable and allowable to the extent that they do not exceed on a daily basis the per diem rates set forth in the Federal Travel Regulation (FTR).

(iv) Travel via privately owned automobile shall be reimbursed at not more than the current General Services Administration (GSA) FTR established mileage rate.

(b) Except as stated herein and under Section B. Paragraph B.4. PROVISIONS APPLICABLE TO DIRECT COSTS, the Contractor shall not incur costs unless the prior written authorization of the Contracting Officer has been obtained. When costs are incurred without such prior authorization, with the intent of claiming reimbursement as direct costs, it shall be at the contractor’s risk.

G. 6. INDIRECT COST RATES (APPLICABLE TO CPFF CLIN’s)

In accordance with Federal Acquisition Regulation (FAR) (48 CFR chapter 1) Clauses 52.216-7(d)(2), “Allowable Cost and Payment” incorporated by reference in this contract in Part II, Section I, the cognizant Contracting Officer representative responsible for negotiating provisional and/or final indirect cost rates is identified as follows:

Director, Division of Financial Advisory Services
Office of Acquisition Management and Policy
National Institutes of health
6100 Building, Room 6B05
6100 Executive Boulevard, MSC 7540
Bethesda, MD 20892-7540

These rates are hereby incorporated without further action of the Contracting Officer.

G. 7. POST AWARD EVALUATION OF PAST PERFORMANCE

Interim and final evaluations of contractor performance shall be conducted on this contract in accordance with FAR 42.15. The final performance evaluation shall be completed at the time of completion of work. Interim and final evaluations will be submitted to the Contractor as soon as practicable. The Contractor will be permitted thirty days to review the document and to submit additional information or a rebutting statement.

SECTION H—SPECIAL CONTRACT REQUIREMENTS

H. 1. HUMAN SUBJECTS

Research involving human subjects shall not be conducted under this contract until the protocol developed in Milestone 2 has been approved by DHHS, written notice of such approval has been provided by the Contracting Officer, and the Contractor has provided to the Contracting Officer a properly completed Optional Form 310 certifying IRB review and approval of the protocol. The human subject certification can be met by submission of the Contractor’s self designated form, provided that it contains the information required by the Optional Form 310.

H. 2. HUMAN MATERIALS

It is understood that the acquisition and supply of all human specimen material (including fetal material) used under this contract will be obtained by the Contractor in full compliance with applicable State and Local laws and the provisions of the Uniform Anatomical Gift Act in the United States and that no undue inducements, monetary or otherwise, will be offered to any person to influence their donation of human material.

H.3. PROHIBITION ON THE USE OF APPROPRIATED FUNDS FOR LOBBYING ACTIVITIES AND HHSAR 352.270-10 ANTI-LOBBYING (Jan 2006)

The Contractor is hereby notified of the restrictions on the use of Department of Health and Human Service’s funding for lobbying of Federal, State and Local legislative bodies.

Section 1352 of Title 10, United Stated Code (Public Law 101-121, effective 12/23/89), among other things, prohibits a recipient (and their subcontractors) of a Federal contract, grant, loan, or cooperative agreement from using appropriated funds (other than profits from a federal contract) to pay any person for influencing or attempting to influence an officer or employee of any agency, a Member of Congress, an officer or employee of Congress, or an employee of a Member of Congress in connection with any of the following covered Federal actions; the awarding of any Federal contract: the making of any Federal grant: the making of any Federal loan; the entering into of any cooperative agreement; or the modification of any Federal contract, grant, loan, or cooperative agreement. For additional information ofprohibitions against lobbying activities, see FAR Subpart 3.8 and FAR Clause 52.203-12.

In addition, as set forth in HHSAR 352270-10 “Anti-Lobbying” (January 2006), the current Department of Health and Human Services Appropriations Act provides that no part of any appropriation contained in this Act shall be used, other than for normal and recognized executive-legislative relationships, for publicity or propaganda purposes, for the preparation, distribution, or use of any kit, pamphlet, booklet, publication, radio, television, or video presentation designed to support, or defeat legislation pending before the Congress, or any State or focal legislature except in presentation to the Congress, or any State or Local legislative body itself.

The current Department of health and Human Services Appropriations Act also provides that no part of any appropriation contained in this Act shall be used to pay the salary or expenses of any contract or grant recipient, or agent acting for such recipient, related to any activity designed to influence legislation or appropriations pending before the Congress, or any State or Local legislature.

(End of Clause)

H.4. PRIVACY ACT APPLICABILITY (Apr 2000)

(a) Notification is hereby given that the Contractor and its employees are subject to criminal penalties for violation of the Privacy Act to the same extent as employees of the Government. The Contractor shall assure that each of its employees knows the prescribed rules of conduct and that each is aware that he or she can be subjected to criminal penalty for violation of the Act. A copy of 45 CFR Part 5b, Privacy Act Regulations, may be obtained at

http://www.gpoaccess.gov/cfr/index.html

(b) The Project Officer is hereby designated as the official who is responsible for monitoring contractor compliance with the Privacy Act.

(c) The Contractor shall follow the Privacy Act guidance as contained in the Privacy Act System of Records number 09-25-0200. This document may be obtained at the following link: http://oma.od.nih.gov/ms/privacv/pa-files/0200.htm

(End of Clause)

Note: Clinical trials cannot be initiated until the System Notice has been published and the Contracting Officer notifies the contractor.

H.5. LABORATORY LICENSE REQUIREMENTS (May 1998)

The Contractor shall comply with all applicable requirements of Section 353 of the Public Health Service Act (Clinical Laboratory Improvement Act as amended). This requirement shall also be included in any subcontract for services under the contract.

(End of Clause)

H.6. DISSEMINATION OF INFORMATION (May 1998)

No information related to data obtained under this contract shall be released or publicized without the prior written consent of the Project Officer.

(End of Clause)

H.7. IDENTIFICATION AND DISPOSITION OF DATA

The Contractor will be required to provide certain data generated under this contract to the Department of Health and Human Services (DHHS). DHHS reserves the right to review any other data determined by DHHS to be relevant to this contract. The contractor shall keep copies of all data required by the Food and Drug Administration (FDA) relevant to this contract for the time specified by the FDA.

H.8. INFORMATION ON COMPLIANCE WITH ANIMAL CARE REQUIREMENTS

Registration with the U. S. Dept. of Agriculture (USDA) is required to use regulated species of animals for biomedical purposes. The USDA office contact information is available at http://www.aphis.usda.gov/ac/acorg.html. They are responsible for the enforcement of the Animal Welfare Act (7 U.S.C. 2131 et. seq.), http://www.nal.usda.gov/awic/legislat/awa.htm.

The Public Health Service (PHS) Policy is administered by the Office of Laboratory Animal Welfare (OLAW) http://grants2.nih.gov/grants/olaw/olaw.htm. An essential requirement of the PHS Policy http://grants2.nih.gov/grants/olaw/references/phspol.htm is that every institution using live vertebrate animals must obtain an approved assurance from OLAW before they can receive funding from any component of the U. S. Public Health Service.

The PHS Policy requires that Assured institutions base their programs of animal care and use on the Guide for the Care and Use of Laboratory Animals http://www.nap.edu/readingroom/books/labrats/ and that they comply with the regulations (9 CFR, Subchapter A) http://www.nal.usda.gov/awic/legislat/usdaleg1.htm issued by the U.S. Department of Agriculture (USDA) under the Animal Welfare Act. The Guide may differ from USDA regulations in some respects. Compliance with the USDA regulations is an absolute requirement of this Policy.

The Association for Assessment and Accreditation of Laboratory Animal Care International (AAALAC) http://www.aaalac.org is a professional organization that inspects and evaluates programs of animal care for institutions at their request. Those that meet the high standards are given the Accredited status. As of the 2002 revision of the PHS Policy, the only accrediting body recognized by PHS is the AAALAC. While AAALAC Accreditation is not required to conduct biomedical research, it is highly desirable. AAALAC uses the Guide as their primary evaluation tool. They also use the Guide for the Care and Use of Agricultural Animals in Agricultural Research and Teaching. It is published by the Federated of Animal Science Societies http://www.fass.org.

H.9. NOTICE TO OFFERORS OF REQUIREMENTS FOR ADEQUATE ASSURANCE OF PROTECTION OF ADEQUATE ASSURANCE OF PROTECTION OF VERTEBILtTE ANIMAL SUBJECTS

The PHS Policy on Humane Care and Use of Laboratory Animals requires that applicant organizations proposing to use vertebrate animals file a written Animal Welfare Assurance with the Office for Laboratory Animal Welfare (OLAW). establishing appropriate policies and procedures to ensure the humane care and use of live vertebrate animals involved in research activities supported by the PHS. The PF1S Policy stipulates that an applicant organization, whether domestic or foreign, bears responsibility for the humane care and use of animals in PHS-supported research activities. Also, the PHS policy defines “animal” as “any live, vertebrate animal used, or intended for use, in research, research training, experimentation, biological testing or for related purposes.” This Policy implements and supplements the US. Government Principles for the Utilization and Care of Vertebrate Animals Used in Testing, Research, and Training, and requires that institutions use the Guide for the Care and Use of Laboratory Animals as a basis For developing and implementing an institutional animal care and use program. This Policy does not affect applicable State or local laws or regulations that impose more stringent standards for the care and use of laboratory animals. All institutions are required to comply, as applicable, with the Animal Welfare Act as amended (7 USC 2131 et. seq.) and other Federal statutes and regulations relating to animals. These documents are available from the Office of Laboratory Animal Welfare, National Institutes of Health, Bethesda, MD 20892, (301) 496-7163. See http://grants.nih.gov/grants/olaw/olaw.htm. No PHS supported work for research involving vertebrate animals will be conducted by an organization. unless that organization is operating in accordance with an approved Animal Welfare Assurance and provides verification that the institutional Animal Care and Use Committee (IACUC) has reviewed and approved the proposed activity in accordance with the PHS policy. Applications may be referred by the PHS back to the institution for further review in the case of apparent or potential violations of the PHS Policy. No award to an individual will be made unless that individual is affiliated with an assured organization that accepts responsibility for compliance with the PHS Policy. Foreign applicant organizations applying for PHS awards for activities involving vertebrate animals are required to comply with PHS Policy or provide evidence that acceptable standards for the humane care and use of animals will be met. Foreign applicant organizations are not required to submit IACUC approval.

H.10. APPROVAL OF REQUIRED ASSURANCE BY OLAW

Under governing regulations, federal funds which are administered by the Department of Health and Human Services. Office of Biomedical Advanced Research and Development Authority (BARDA) shall not be expended by the contractor for research involving live vertebrate animals, nor shall live vertebrate animals be involved in research activities by the contractor under this award unless a satisfactory assurance of compliance with 7 U.S.C. 2316 and 9 CFR Sections 2.25-2.28 is submitted within 30 days of the date of this award and approved by the Office of Laboratory Animal Welfare (OLAW). Each performance site (if any) must also assure compliance with 7 U.S.C. 2316 and 9 CFR Sections 2.25-2.28 with the following restriction: Only activities which do not directly involve live vertebrate animals (i.e. are clearly severable and independent from those activities that do involve live vertebrate animals) may be conducted by the contractor or individual performance sites pending OLAW approval of their respective assurance of compliance with 7 U.S.C. 2316 and 9 CFR Sections 2.25-2.2k. Additional information regarding OLAW may be obtained via the Internet at http://grants2.nih.gov/grants/olaw/olawaddr.htm.

H.11. MANUFACTURING STANDARDS

The current Good Manufacturing Practice regulations (cGMP), e.g. 21 CFR parts, 58. 210, 211. 600 and 610 series as well as other- relevant and applicable FDA guidelines will be the standard to be applied by the contractor for the manufacturing, processing, packaging and release of this vaccine product.

If at any time during the life of the contract, the Contractor fails to comply with cGMP in the manufacturing, processing and packaging of this product and such failure results in a material adverse effect on the safety, purity or potency of the product (a material failure) as identified by CBER and CDER, the Offeror shall have thirty (30) calendar days from the time such material failure is identified to cure such material failure. If the offeror fails to take such an action within the thirty (30) calendar day period, then the contract may be terminated.

H.12. PROHIBITION ON CONTRACTOR INVOLVEMENT WITH TERRORIST ACTIVITIES

The Contractor acknowledges that U.S. Executive Orders and Laws, including but not limited to Executive Order 13224 and Public Law 107-56, prohibit transactions with, and the provision of resources and support to, individuals and organizations associated with terrorism. It is the legal responsibility of the contractor to ensure compliance with these Executive Orders and Laws. This clause must be included in all subcontracts issued under this contract.

H.13 . REGISTRATION WITH THE SELECT AGENT PROGRAM FOR WORK INVOLVING THE POSSESSION, USE, AND/OR TRANSFER OF SELECT BIOLOGICAL AGENTS OR TOXINS

Work involving select biological agents or toxins shall not be conducted under this contract until the contractor and any affected subcontractor(s) are granted a certificate of registration or are authorized to work with the applicable select agents.

For prime or subcontract awards to domestic institutions who possess, use, and/or transfer Select Agents under this contract, the institution must complete registration with the Centers for Disease Control and Prevention (CDC), Department of Health and Human Services (DHHS) or the Animal and Plant Health Inspection Services (APHIS), U.S. Department of Agriculture (USDA), as applicable, before performing work involving Select Agents, in accordance with 42 CFR 73. No Government funds can be used for work involving Select Agents, as defined in 42 CFR 73, if the final registration certificate is denied.

For prime or subcontract awards to foreign institutions who possess, use, and/or transfer Select Agents under this contract, the institution must provide information satisfactory to the Government that a process equivalent to that described in 42 CFR 73 (http://www.cdc.gov/od/sap/docs/42cfr73.pdf) for U.S. institutions is in place and will be administered on behalf of all Select Agent work sponsored by these funds before using these funds for any work directly involving the Select Agents. The contractor must provide information addressing the following key elements appropriate for the foreign institution: safety, security, training, procedures for ensuring that only approved/appropriate individuals have access to the Select Agents, and any applicable laws, regulations and policies equivalent to 42 CFR 73. The Government will assess the policies and procedures for comparability to the U.S. requirements described in 42 CFR Part 73. When requested by the contracting officer, the contractor shall provide key information delineating any laws, regulations, policies, and procedures applicable to the foreign institution for the safe and secure possession, use, and transfer of Select Agents. This includes summaries of safety, security, and training plans, and applicable laws, regulations, and policies. For the purpose of security risk assessments, the contractor must provide the names of all individuals at the foreign institution who will have access to the Select Agents and procedures for ensuring that only approved and appropriate individuals have access to Select Agents under the contract.

Listings of HHS select agents and toxins. biologic agents and toxins, and overlap agents or toxins as well as information about the registration process, can be obtained on the Select Agent Program Web site at http://www.cdc.gov/od/sap/.

H.14. OPTION PROVISION

Unless the Government exercises its option pursuant to the Option Clause set forth in Section I, Paragraph I.3., the contract will consist only of CLIN’s 0001-0006 of the Statement of Work as defined in Sections C and F of the contract. Pursuant to clause 52.217-7 set forth in Section I of this contract, under I.3., the Government may, by unilateral contract modification, require the Contractor to perform any of the additional CLIN’s listed in Section B, Paragraph B.2. and as also defined in Sections C and F of this contract. If the Government exercises this option, notice must be given at least 60 days prior to the expiration date of this contract, and the amount of the contract will be increased as set forth in Section B. Paragraph B.2.

H. 15. LIABILITY PROTECTION UNDER PREP ACT

The Public Readiness and Emergency Preparedness Act (PREP Act), Public Law 109-148, Division C, 119 Stat. 2818 to 2832, amended the Public Health Service Act, 42 U.S.C. 243 et seq., to provide targeted liability protections. The Government agrees that the medical countermeasure delivered by the contractor under this contract will not be administered for use in humans, unless the Secretary executes a declaration in accordance with section 319F-3(b) of the Public Health Service Act, 42 U.S.C. 247d-6d, that the medical countermeasure delivered under this contract is a covered countermeasure to which section 319-F-3(a) applies subject to the terms and conditions of the declaration.

H. 16. EPA ENERGY STAR REQUIREMENTS

performance of a contract shall be equipped with or meet the energy efficient low-power standby feature as defined by the EPA Energy Star program unless the equipment always meets EPA Energy Star efficiency levels. The microcomputer, as configured with all components, must be Energy Star compliant.

This low-power feature must already be activated when the computer equipment is delivered to the agency and be of equivalent functionality of similar power managed models. If the equipment will be used on a local area network, the vendor must provide equipment that is fully compatible with the network environment. In addition, the equipment will run commercial off-the-shelf software both before and after recovery from its energy conservation mode.

H. 17. ACKNOWLEDGMENT OF FEDERAL FUNDING

A. Section 507 of P.L. 104-208 mandates that contractors funded with Federal dollars. in whole or in part, acknowledge Federal funding when issuing statements, press releases, requests for proposals, bid solicitations and other documents. Contractors are required to state (1) the percentage and dollar amounts of the total program or project costs financed with Federal money, and (2) the percentage and dollar amount of the total casts financed by nongovernmental sources.

This requirement is in addition to the continuing requirement to provide an acknowledgment of support and disclaimer on any publication reporting the results of a contract funded activity.

B. Publication and Publicity

The Contractor shall acknowledge the support of the Department of Health and Human Service, Office of Public Health Emergency Preparedness. Office of Research and Development Coordination whenever publicizing the work under this contract in any media by including an acknowledgment substantially as follows:

“This project has been funded in whole or in part with Federal funds from the Office of the Assistant Secretary for Preparedness and Response, Biomedical Advanced Research and Development Authority, under Contract No. HHSO100200700034C.”

C. Press Releases

Pursuant to Section 508 of Public Law 105-78, the contractor shall clearly state, when issuing statements, press releases. requests for proposals, bid solicitations and other documents describing projects or programs Funded in whole or in part with Federal money that: (1) the percentage of the total costs of the program or project which will be Financed with Federal money; (2) the dollar amount of Federal funds for the project or program; and (3) the percentage and dollar amount of the total costs of the project or program that will be financed by nongovernmental sources.

H. 18. REPORTING MATTERS INVOLVING FRAUD, WASTE AND ABUSE

Anyone who becomes aware of the existence or apparent existence of fraud, waste and abuse in DHHS funded programs is encouraged to report such matters to the NHS Inspector General’s Office in writing or on the Inspector General’s Hotline. The toll-free number is 1-800-HHS-TIPS (1-800-447-8477). All telephone calls will be handled confidentially. The e-mail address is Htips@os.dhhs.gov.

Office of Inspector General
Department of Health and Human Services
TIPS HOTLINE
P.O. Box 23489
Washington, DC 20026

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

H. 19. MANUFACTURING STANDARDS

The Current Good Manufacturing Practice Regulations (cGMP) (21 CFR Parts 210-211) will be the standard to be applied for manufacturing, processing and packing of this product.

If at any time during the life of the contract, the Offeror fails to comply with cGMP in the manufacturing, processing and packaging of this product and such failure results in a material adverse effect on the safety, purity or potency of this product (a material failure) as identified by CBER and CDER, the Offeror shall have thirty (30) calendar days from the time such material failure is identified to cure such material failure. If the Offeror fails to take such an action within the thirty (30) calendar day period, then the contract may be terminated.

H.20. INCORPORATION OF TECHNICAL PROPOSAL

[***]

H.21. SUBCONTRACTING PROVISIONS

a. Small Business Subcontracting Plan

(1) The Small Business Subcontracting Plan dated May 23, 2007 is attached hereto and made a part of this contract.

(2) In addition to the goals listed in the attached plan. the following goals are added:

a. Total estimated dollar and percent of planned subcontracting with VETERAN-OWNED SMALL BUSINESSES:

[***]
[***]
[***]
[***]
[***]

b. Total estimated dollar and percent of planned subcontracting with SERVICE-DISABLED VETERAN OWNED SMALL BUSINESSES:

[***]
[***]
[***]
[***]
[***]

b. Subcontracting Reports

(1) Individual Subcontract Reports (ISR)

The Contractor shall submit the original and 1 copy of the Subcontracting Report for Individual Contracts, SF 294, in accordance with the instructions on the report as referenced in Public Law 95-507, Section. 211. The report shall be submitted to the Contracting Officer at the address specified in Section U. Regardless of the effective date of this contract, the Report shall be submitted on the following dates for the entire life of this contract:

April 30th
October 30th

PART II- CONTRACT CLAUSES

SECTION I - CONTRACT CLAUSES

I.1. FAR 52.252-2, CLAUSES INCORPORATED BY REFERENCE (FEBRUARY 1998)

This contract incorporates the following clauses by reference, with the same force and effect as if they were given in full text. Upon request, the Contracting Officer will make their full text available. Also, the full text of a clause may be accessed electronically at these addresses: http://www.arnet.gov and http://www.dhhs.gov/oamp/dap/hhsar.html/

A. Negotiated Fixed Price Suppiv Contract General Clauses

(1) FEDERAL ACQUISITION REGULATION (FAR) (48 CHAPTER 1) CLAUSES

FAR CLAUSE NO.	DATE	TITLE

52.202-1	Jul 2004	Definitions

52.203-3	Apr 1984	Gratuities (Over $100,000)

52.203-5	Apr 1984	Covenant Against Contingent Fees (Over $100,000)

52.203-6	Sep 2006	Restrictions on Subcontractor Sales to the Government (Over $100,000)

52.203-7	Jul 1995	Anti-Kickback Procedures (Over $100,000)

52.203-8	Jan 1997	Cancellation, Rescission, and Recovery of Funds for Illegal or Improper Activity (Over $100,000)

52.203-10	Jan 1997	Price or Fee Adjustment fur Illegal or Improper Activity (Over $100,000)

52.203-12	Sep 2005	Limitation on Payments to Influence Certain Federal Transactions (Over $100,000)

52.204-4	Aug 2000	Printed or Copied Double-Sided on Recycled Paper (Over $100,000)

52.204-7	Jul 2006	Central Contractor Registration

52.200-6	Sep 2006	Protecting the Government’s Interests When Subcontracting With Contractors Debarred, Suspended, or Proposed for Debarment (Over $25,000)

52.211-5	Aug 2000	Material Requirements

52.215-2	Jun 1999	Audit and Records - Negotiation (Over $100,000)

52.215-5	Oct 1997	Order of Precedence - Uniform Contract Format

52.215-10	Oct 1997	Price Reduction for Defective Cost or Pricing Data

52.215-12	Oct 1997	Subcontractor Cost or Pricing Data (Over $500,000)

52.215-14	Oct 1997	Integrity of Unit Prices (Over $100,000)

52.215-15	Oct 2004	Pension Adjustments and Asset Reversions

52.215-18	Jul2005	Reversion or Adjustment of Plans for Post-Retirement Benefits (PRB) other than Pensions

52.215-19	Oct 1997	Notification of Ownership Changes

52.215-21	Oct 1997	Requirements for Cost or Pricing Data or Information Other Than Cost or Pricing Data - Modifications

52.219-8	May 2004	Utilization of Small Business Concerns (Over $100,000)

52.219-9	Sep 2006	Small Business Subcontracting Plan (Over $500.000)

52.219-16	Jan 1999	Liquidated Damages - Subcontracting Plan (Over $500,000)

52.222-19	Jan 2006	Child Labor—Cooperation with Authorities and Remedies

52.222-20	Dec 1996	Walsh-Healey Public Contracts Act

52.222-21	Feb 1999	Prohibition of Segregated Facilities

52.222-26	Mar 2007	Equal Opportunity

52.222-35	Sep 2006	Equal Opportunity ror Special Disabled Veterans, Veterans of the Vietnam Era, and Other Eligible Veterans

52.222-36	Jun 1998	Affirmative Action for Workers with Disabilities and Other Eligible Veterans

52.223-6	May 2001	Drug-Free Workplace

52.223-14	Aug 2003	Toxic Chemical Release Reporting (Over $100,000)

52.225-1	Jun 2003	Buy American Act - Supplies

52.225-13	Feb 2006	Restrictions on Certain Foreign Purchases

52.227-1	Jul 1995	Authorization and Consent

52.227-2	Aug 1996	Notice and Assistance Regarding Patent and Copyright Infringement (Over $100,000)

52.227-3	Apr 1984	Patent Indemnity

52.229-3	Apr 2003	Federal, State and Local Taxes (Over $100,000)

52.232-1	Apr 1984	Payments

52.232-8	Feb 2002	Discounts For Prompt Payment

52.232-9	Apr 1984	Limitation on Withholding of Payments

52.232-11	Apr 1984	Extras

52.232-17	Jun 1996	Interest (Over $100,000)

52.232-23	Jan 1086	Assignment of Claims

52.232-25	Oct 2003	Prompt Payment

52.232-33	Oct 2003	Payment by Electronic Funds Transfer—Central Contractor Registration

52.233-1	Jul 2002	Disputes

52.233-3	Aug 1996	Protest After Award

52.233-4	Oct 2004	Applicable Law for Breach of Contract Claim

52.242-13	Jul 1995	Bankruptcy (Over $100,000)

52.243-1	Aug 1987	Changes - Fixed-Price

52.244-2	Aug 1998	Subcontracts *If written consent to subcontract is required, the identified subcontracts are listed in Section B, Paragraph B.4, Advance Understandings.

52.244-6	Mar 2007	Subcontracts for Commercial Items

52.245-2	May 2004	Government Property (Fixed-Price Contracts)

52.249-2	May 2004	Termination for the Convenience of the Government (Fixed-Price)

52.249-8	Apr 1984	Default (Fixed-Price Supply and Service)(Over $100,000)

52.253-1	Jan 1991	Computer Generated Forms

(2) DEPARTMENT OF HEALTH AND HUMAN SERVICES ACQUISITION REGULATION (HHSAR) (48 CFR CHAPTER 3) CLAUSES

HHSAR CLAUSE NO.	DATE	TITLE

352.202-1	Jan 2006	Definitions

352.232-9	Jan 2006	Withholding olContract Payments

352.270-4	Jan 2001	Pricing of Adjustments

352.270-6	Jan 2006	Publications and Publicity

352.270-7	Jan 2006	Paperwork Reduction Act

[End of GENERAL CLAUSES FOR A NEGOTIATED FIXED PRICE SUPPLY CONTRACT - Rev. 03/2007.

B. Cost-Reimbursement Research and Development General Clauses

(1) FEDERAL ACQUISITION REGULATION (FAR) (48 CFR CHAPTER 1) CLAUSES:

FAR CLAUSE NO.	DATE	TITLE

52.202-1	Jul 2004	Definitions

52.203-3	Apr 1984	Gratuities (Over $100,000)

52.203-5	Apr 1984	Covenant Against Contingent Fees (Over $100,000)

52.203-6	Sep 2006	Restrictions on Subcontractor Sales to the Government (Over $100,000)

52.203-7	Jul 1995	Anti-Kickback Procedures (Over $100,000)

52.203-8	Jan 1997	Cancellation, Rescission, and Recovery of Funds for Illegal or Improper Activity (Over $100,000)

52.203-10	Jan 1997	Price or Fee Adjustment for Illegal or Improper Activity (Over $100,000)

52.203-12	Sep 2005	Limitation on Payments to Influence Certain Federal Transactions (Over $100,000)

52.204-4	Aug 2000	Printed or Copied Double-Sided on Recycled Paper (Over $100,000)

52.204-7	Jul 2006	Central Contractor Registration

52.209-6	Sep 2006	Protecting the Government’s Interests When Subcontracting With Contractors Debarred, Suspended. or Proposed for Debarment (Over $25,000)

52.215-2	Jun 1999	Audit and Records - Negotiation (Over $100,000)

52.215-8	Oct 1997	Order or Precedence - Uniform Contract Format

52.215-10	Oct 1997	Price Reduction for Defective Cost or Pricing Data

52.215-12	Oct 1997	Subcontractor Cost or Pricing Data (Over $500,000)

52.2I5-14	Oct 1997	Integrity of Unit Prices (Over $100,000)

52.215-15	Oct 2004	Pension Adjustments and Asset Reversions

52.215-I$	Jul 2005	Reversion or Adjustment of Plans for Post-Retirement Benefits (PRB) other than Pensions

52.215-19	Oct 1997	Notification of Ownership Changes

52.215-21	Oct 1997	Requirements for Cost or Pricing Data or Information Other Than Cost or Pricing Data - Modifications

52.216-8	Mar 1997	Fixed Fee

52.219-8	May 2004	Utilization of Small Business Concerns (Over $100,000)

52.214-9	Jan 2002	Small Business Subcontracting Plan (Over $500.000)

52.219-16	Jan 1999	Liquidated Damages - Subcontracting Plan (Over $500,000)

52.222-2	Jul 1990	Payment for Overtime Premium (Over $100,000) (Note: The dollar amount in paragraph (a) of this clause is $0 unless otherwise specified in the contract.)

52.222-3	Jun 2003	Convict Labor

52.222-21	Feb 1999	Prohibition of Segregated Facilities

52.222-26	Mar 2007	Equal Opportunity

52.222-35	Dec 2001	Equal Opportunity For Special Disabled Veterans, Veterans of the Vietnam Era. and Other Eligible Veterans

52.222-36	Jun 1948	Affirmative Action For Workers with Disabilities

52.222-37	Sep 2006	Employment Reports on Special Disabled Veterans, Veterans of the Vietnam Era, and Other Eligible Veterans

52.222-50	Apr 2006	Combating Trafficking in Persons

52.223-6	May 2001	Drug-Free Workplace

52.223-14	Aug 2003	Toxic Chemical Release Reporting (Over S100,000)

52.225-1	Jun 2003	Buy American Act - Supplies

52.225-13	Feb 2006	Restrictions on Certain Foreign Purchases

52.227-1	Jul 1995	Authorization and Consent. Alternate 1 (Apr 1984)

52.227-2	Aug 1996	Notice and Assistance Regarding Patent and Copyright Infringement (Over $100,000)

52.227-11	Jun 1997	Patent Rights - Retention by the Contractor (Short Form) (Note: In accordance with FAR 27.303(a)(2), paragraph (f) is modified to include the requirements in FAR 27.303(a)(2)(i)through (iv). The Frequency ofreporting in (i) is annual.

52.227-14	Jun 1987	Rights in Data - General

52-232-9	Apr 1984	Limitation on Withholding of Payments

52.232-17	Jun 1996	Interest (Over $100,000)

52.232-20	Apr 1984	Limitation of Cost

52.232-23	Jan 1986	Assignment of Claims

52.232-25	Oct 2003	Prompt Payment, Alternate I (Feb 2002)

52.232-33	Oct 2003	Payment by Electronic Funds Transfer—Central Contractor Registration

52.233-1	Jul 2002	Disputes

52.233-3	Aug 1996	Protest After Award, Alternate I (Jun 1985)

52.233-4	Oct 2004	Applicable Law for Breach of Contract Claim

52.242-1	Apr 1984	Notice of Intent to Disallow Costs

52.242-3	May 2001	Penalties for Unallowable Costs (Over $500,000)

52.242-4	Jan 1997	Certification of Final Indirect Costs

52.242-13	Jul 1995	Bankruptcy (Over $140,000)

52.243-2	Aug 1987	Changes - Cost Reimbursement, Alternate V (Apr 1984)

52.244-2	Aug 1998	Subcontracts, Alternate II (Aug 1998) *If written consent to subcontract is required, the identified subcontracts are listed in Section B. Paragraph B.4., Advance Understandings.

52.244-5	Dec 1996	Competition in Subcontracting (Over $100,000)

52.244-6	Mar 2007	Subcontracts for Commercial Items

52.245-5	May 2004	Government Property (Cost-Reimbursement, Time and Material, or Labor-Hour Contract)

52.245-9	Aug 2005	Use and Charges

52.241-23	Feb 1997	Limitation of Liability (Over $100,000)

52.249-6	May 2004	Termination (Cost-Reimbursement)

52.249-14	Apr 1984	Excusable Delays

52.253-1	Jan 1991	Computer Generated Forms

(2) DEPARTMENT OF HEALTH AND HUMAN SERVICES ACQUISITION REGULATION (HHSAR) (48 CFR CHAPTER 3) CLAUSES:

HHSAR CLAUSE NO.	DATE	TITLE

352.202-1	Jan 2006	Definitions - with Alternate paragraph (h) (Jan 2001)

352.216-72	Jan 2006	Additional Cost Principles

352.228-7	Dec 1991	Insurance - Liability to Third Persons

352.232-9	Jan 2006	Withholding of Contract Payments

352.233-70	Jan 2006	Litigation and Claims

352.242-71	Apr 1984	Final Decisions on Audit Findings

352.270-5	Jan 2006	Key Personnel

352.270-6	Jan 2006	Publications and Publicity

352.270-7	Jan 2006	Paperwork Reduction Act

[ End of GENERAL CLAUSES FOR A COST-REIMBURSEMENT RESEARCH AND DEVELOPMENT CONTRACT
- Rev. 03/2007].

1.2. AUTHORIZED SUBSTITUTIONS OF CLAUSES

FAR 52.252-6 , Authorized Deviations in Clauses (Apr1984):

FAR 52.216-7, Allowable Cost and Payment (Dec 2002) (DEVIATION). Paragraph (a)(l) is modified to read as follows:

“In accordance with Public Law 108-276, the Contractor may not invoice for payment under contract line item numbers (CLIN’s) 0004, 0005, and 0406 prior to satisfying the paragraph of this contact entitled “Payment conditioned on delivery of usable product.” After satisfaction of the paragraph “Payment conditioned on delivery of usable product,” the Government will make payments to the Contactor when requested as work progresses, but (except for small business concerns) not more often than once every 2 weeks, in amounts determined to be allowable by the Contracting Officer in accordance with Federal Acquisition Regulation (FAR) Subpart 31.2 in effect on the date of this contract and the terms of this contract. The Contractor may submit to an authorized representative of the Contracting Officer, in such form and reasonable detail as the representative may require, an invoice or voucher supported by a statement of the claimed allowable cost for performing this contract.”

I.3. ADDITIONAL CONTRACT CLAUSES

This contract incorporates the following clauses by reference, with the same force and effect, as if they were given in full text. Upon request, the Contracting Officer will make their full text available.

A. FEDERAL ACQUISITION REGULATION (FAR) (48 CFR CHAPTER 1) CLAUSES

(1) 52.217-7 Option for Increased Quantity - Separately Priced Line Item (MARCH 1989).

“....The Contracting Officer may exercise the option by written notice to the Contractor within 60 days prior to the expiration of this contract ......

(2) 52.215-17 Waiver of Facilities Capital Cost of Money (October 1997)

(3) 52.224-1, Privacy Act Notification (April 1984)

(4) 52.224-2, Privacy Act (April 1984)

(5) 52.229-6, Taxes — Foreign Fixed-Price Contracts (June 2003)

(6) 52.229-3 Taxes—Foreign Cost- Reimbursement Contracts.(March 1990)

(7) 52.232-32, Performance-Based Payments (FEB 2002)

“(c)(2) ..The designated payment office will pay approved requested on the 30th day after receipt of the request for the performance-based payment.”

B. DEPARTMENT OF HEALTH AND HUMAN SERVICES ACQUISITION REGULATION (HHSAR) (48 CHAPTER 3) CLAUSES: Full text of these clauses can be found at http://www.dhhs.gov/oamp/dap/hhsar.html/

(1) HHSAR 352.223-70, Safety and Health (JANUARY 2006)

(2) HHSAR 352.224-70, Confidentiality of Information (JANUARY 2006)

Note: The following information is covered by this clause: Data obtained from human subjects

(3) HHSAR 352.270-5, Key Personnel (JANUARY 2006)

I.4. Additional Contract Clauses of SECTION 1— Added in full text

(1) FAR 52,222-39 Notification of Emplovee Rights Concerning Payment of Union Dues or Fees.

Notification of Employee Rights Concerning Payment of Union Dues or Fees (Dec 2004)

(a) Definition. As used in this clause—

“United States” means the 50 States, the District of Columbia. Puerto Rico, the Northern Mariana Islands, American Samoa, Guam, the U.S. Virgin Islands, and Wake Island.

(b) Except as provided in paragraph (e) of this clause, during the term of this contract, the Contractor shall post a notice, in the form of a poster, informing employees of their rights concerning union membership and payment of union dues and fees, in conspicuous places in and about all its plants and offices, including all places where notices to employees are customarily posted. The notice shall include the following information (except that the information pertaining to National Labor Relations Board shall not be included in notices posted in the plants or offices of carriers subject to the Railway Labor Act, as amended (45 U.S.C. 151-188)).

Notice to Employees

Under Federal law, employees cannot be required to join a union or maintain membership in a union in order to retain their jobs. Under certain conditions, the law permits a union and an employer to enter into a union-security agreement requiring employees to pay uniform periodic dues and initiation fees. However, employees who are not union members can object to the use of their payments for certain purposes and can only be required to pay their share of union costs relating to collective bargaining, contract administration, and grievance adjustment.

If you do not want to pay that portion of dues or fees used to support activities not related to collective bargaining, contract administration, or grievance adjustment, you are entitled to an appropriate reduction in your payment. If you believe that you have been required to pay dues or fees used in part to support activities not related to collective bargaining, contract administration, or grievance adjustment, you may be entitled to a refund and to an appropriate reduction in future payments.

For further information concerning your rights, you may wish to contact the National Labor Relations Board (NLRB) either at one of its Regional offices or at the following address or toll free number:

National Labor Relations Board
Division of Information
1099 14th Street, N.W.
Washington, DC 20570
1-866-667-6572
1-866-316-6572 (TTY)
To locate the nearest NLRB office, see NLRB’s website at http://www.nlrb.gov.

(c) The Contractor shall comply with all provisions of Executive Order 13201 of February 17, 2001, and related implementing regulations at 29 CFR Part 470, and orders of the Secretary of Labor.

(d) In the event that the Contractor does not comply with any of the requirements set forth in paragraphs (b). (c), or (g), the Secretary may direct that this contract be cancelled, terminated, or suspended in whole or in part. and declare the Contractor ineligible for further Government contracts in accordance with procedures at 29 CFR Part 470, Subpart B—Compliance Evaluations, Complaint Investigations and Enforcement Procedures. Such other sanctions or remedies may be imposed as are provided by 29 CFR Part 470, which implements Executive Order 13201, or as are otherwise provided by law.

(e) The requirement to post the employee notice in paragraph (b) does not apply to—

(1) Contractors and subcontractors that employ fewer than 15 persons;

(2) Contractor establishments or construction work sites where no union has been formally recognized by the Contractor or certified as the exclusive bargaining representative of the Contractor’s employees;

(3) Contractor establishments or construction work sites located in a jurisdiction named in the definition of the United States in which the law of that jurisdiction forbids enforcement of union-security agreements:

(4) Contractor facilities where upon the written request of the Contractor, the Department of Labor Deputy Assistant Secretary for Labor-Management Programs has waived the posting requirements with respect to any of the Contractor’s facilities if the Deputy Assistant Secretary finds that the Contractor has demonstrated that

(i) The facility is in all respects separate and distinct from activities of the Contractor related to the performance of a contract: and

(ii) Such a waiver will not interfere with or impede the effectuation of the Executive order; or

(5) Work outside the United States that does not involve the recruitment or employment of workers within the United States.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers is extended, is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) N/A 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. CONTRACT ORDER NO. IN ITEM 10A. FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: [***] Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. [***] NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 7th Sep 2007 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED September 17, 2007 (Signature of person authorized to sign) (4) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). 4 C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 2 2. AMENDMENT/MODIFICATION NO. 1 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Bogeskovvej 9 DK-3490 Kvistgaard Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) N/A 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To revise the Contractor's address, as reflected in Block #8 of this form. No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (unchanged) $[***] (unchanged) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***]CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 5/11 07 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED November 13, 2007 (Signature of person authorized to sign) (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). Y C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 1 2. AMENDMENT/MODIFICATION NO. 2 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC. N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) CAN: 1993219 Appropriation: 75 7005/130714.001 Object Class: 26101 Amount: $[***] 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: [***] No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (changed) $[***] (changed) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. [***], Contracting Officer NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***] 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 13/8 ‘08 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED August 14, 2008 (Signature of person authorized to sign) (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). Y C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1 and mutual agreement of the parties D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 3 2. AMENDMENT/MODIFICATION NO. 3 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SPECIAL PROVISIONS

Contract No: HHSO100200700034C
Modification No: 3

This purpose of this modification is to make the following changes:

A. BASE CONTRACT

2. ESTIMATED COST AND FIXED FEE (CPFF)

In consideration for completion of the work to be performed under CLINs 0004, 0005, and 0006, as shown below, and in accordance with the Statement of Work, it is estimated that the total cost to the Government for full performance of this contract will be $[***] , of which the sum of $[***] represents the estimated reimbursable costs and $[***] represents the fixed-fee. These amounts also represent the total amount of funds currently available for payment and allotted under the CPFF portion of this contract. It is estimated that this amount will cover performance of the contract through the expiration date. See Section F, Paragraph F.2. on the contract’s period of performance.

CLIN’s

SUPPLIES/SERVICES

EST. COST

FIXED
FEE

TOTAL
EST. CPFF

0005

Security of Contract Operations, in accordance with Requirement 8

[***]

II. Under Section I — FAR CLAUSES, within 1.4. “Additional Contract Clauses of SECTION I — Added in Full
Text,” the following clause is added:

FAR 52.203-1 - DISPLAY OF HOTLINE POSTER(S) (DEC 2007)

(a) Definition.

“United States,” as used in this clause, means the 50 States, the District of Columbia, and outlying areas.

(b) Display of fraud hotline poster(s). Except as provided in paragraph (c)—

(1) During contract performance in the United States, the Contractor shall prominently display in common work areas within business segments performing work under this contract and at contract work sites—

(i) Any agency fraud hotline poster or Department of Homeland Security (DHS) fraud hotline poster identified in paragraph (b)(3) of this clause; and

(ii) Any DHS fraud hotline poster subsequently identified by the Contracting Officer.

(2) Additionally, if the Contractor maintains a company website as a method of providing information to employees, the Contractor shall display an electronic version of the poster(s) at the website.

(3) Any required posters may be obtained as follows:

Hotline Poster can be obtained (downloaded) from US Department of Health & Human Services, Office of Inspector General at the below website:

http://www.oig.hhs.gov/hotline.html

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) N/A 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To change the Project Officer assignment, and to document that the requirement for a countermeasure declaration under H.15. Liability Protection under PREP Act has been satisfied. No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (unchanged) $[***] (unchanged) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. [***] NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) CEO & PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 16B. UNITED STATES OF AMERICA [***] 16C. DATE SIGNED 11/11/08 (Signature of person authorized to sign) (Signature of Contracting Officer) (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). Y C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1 and mutual agreement of the parties D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 2 2. AMENDMENT/MODIFICATION NO. 4 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC. N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

NO. 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers is extended, is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) N/A 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. THE CONTRACT ORDER NO. IN ITEM 10A. FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSES: (1) To make a correction to Section I, "Contract Clauses"; and (2) to revise Section J, "List of Attachments," to incorporate the executed Quality Agreement into the contract. No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (unchanged) $[***] (unchanged) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***], PRESIDENT & CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 10/6 2009 16B. UNITED STATES OF AMERICA [***] 16C. DATE SIGNED 17 June, 2009 (Signature of person authorized to sign) (Signature of Contracting Officer) () A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 2 2. AMENDMENT/MODIFICATION NO. 5 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC. N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgard Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) N/A 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. THE CONTRACT ORDER NO. IN ITEM 10A. FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: (1) To add an advanced understanding for the Contractor's responsibilities related to the USDA permit for vaccine importation; and (2) to delete the requirement for [***]. No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (unchanged) $[***] (unchanged) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***], PRESIDENT & CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] (Signature of person authorized to sign) 15C. DATE SIGNED Dec 15, 2009 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED Dec 15, 2009 (Y) A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). Y C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D. OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 2 2. AMENDMENT/MODIFICATION NO. 6 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SPECIAL PROVISIONS

Contract No: HHSO100200700034C
Modification No: 6

The following changes are made to the subject contract:

1. Under Section B, Supplies or Services and Prices/Costs, B.4. ADVANCED UNDERSTANDINGS, item #8 is added to incorporate Contractor responsibilities related to the USDA permit for vaccine importation as follows:

8. The Contractor agrees to assume the following responsibilities with regard to the USDA permit for vaccine importation: (1) pay the USDA fee during importation; (2) present and file the USDA permit during importation; and (3) ensure the production/shipments are in compliance with the current USDA permit.

2. In Section H, Special Contract Requirements, H.21. SUBCONTRACTING PROVISIONS is deleted in its entirety.

3. Under Section I, Contract Clauses, I.1. CLAUSES INCORPORATED BY REFERENCE, is amended to delete the following clauses:

FAR CLAUSE NO.	DATE	TITLE
52.219-9	Sep 2006	Small Business Subcontracting Plan (Over $500,000)
52.219-16	Jan 1999	Liquidated Damages- Subcontracting Plan (Over $500,000)

4. In Section J, LIST OF ATTACHMENTS, the following item is deleted in its entirety:

6) Small Business Subcontracting Plan, 8 pages

All other terms and conditions of the contract are unchanged and remain in full force and effect.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offersis extended,is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) N/A 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. ORDER NO. IN ITEM 10A. FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To change the milesone requirement associated with the Performance Based Payment; (2) to update portions of Sections C and F based upon changes to the projects; and (3) to add indirect rates for the cost-reimbursement CLIN’s that apply specifically to this contract. No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (unchanged) $[***] (unchanged) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***], CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] (Signature of person authorized to sign) 15C. DATE SIGNED 04-May-2010 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED May 4, 2010 (4) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT FAR 52.243-1 Changes — Fixed Price (August 1987) B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). 4 C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 5 2. AMENDMENT/MODIFICATION NO. 7 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

2) Under Requirement 2 — Assay Validation and Stability Testing of Finished Vaccine, paragraph b) is modified to add language on the stability monitoring program. The revised paragraph is shown below:

b) The Contractor shall conduct accelerated and real-time stability studies, including potency testing, on the BDS lots stored by the Contractor and FDP lots placed in the SNS in conformance with FDA/CBER requirements throughout the contract lifetime. Additionally, the Contractor shall develop a stability monitoring program to be used for monitoring product stored in the SNS over the life of the contract or the expiration date of the vaccine, or until vaccine is used, whichever comes first. Under the stability monitoring program the
Contractor must develop protocols and Standard Operating Procedures (SOPs), which shall be forwarded to BARDA for review and then submitted to the FDA for approval. Prior to the receipt of FDA approval,, the Contractor shall sample initial deliveries according to a BARDA approved protocol.

3) Under Requirement 4 — Conduct of Safety and Efficacy Studies — paragraph d), e), and f) are added as follows:

d) [***] prior to a FDA submission connected with safety and efficacy studies, the Contractor shall submit to the Project Officer and Contracting Officer for review and concurrence a copy of all final clinical forms, to include the below items:

(i) Final Phase 3 study protocol

(ii) All relevant IRB approval forms and all relevant assurance forms

(iii) Blank copies of case report forms

(iv) Copy of the unsigned consent form

e) The Project Officer and other designated Government representatives reserve the right to conduct a Good Clinical Practices (GCP) review on all Phase 3 Clinical Research Organization (CRO) sites. If a GCP review is conducted, the Project Officer will provide the Contractor with a summary of written findings within [***] following the completion of the last site visit related to the GCP review. Within [***] after receipt of these written findings, the Contractor shall submit a remediation plan with timelines to the Project Officer and Contracting Officer for review and concurrence. If the Government determines that this plan must be further revised, the Project Officer will provide further comments within [***]. The Contractor shall then submit a finalized plan to the Project Officer and Contracting Officer within another [***] for Government concurrence.

f) The Contractor shall initiate the pivotal Phase 3 clinical study to support Biological License Applications (BLA) and provide proof of successful enrollment of the first [***] individuals. Proof of this enrollment maybe a confirmation of the date on which the
[***] individual was enrolled. This information shall be submitted to the Project Officer
and Contracting Officer for review and concurrence.

4) he following changes are made to Requirement 6 —Shipment to SNS and Short-Term Storage: paragraph c) is modified to change the limitation for no more than 1 delivery per month; and paragraph d) is inserted to add a requirement to conduct studies of thawed product. Paragraphs c) and d) are shown below.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

c) The Contractor shall be responsible for the secure and segregated storage of held intermediates and the FDP prior to lot release and subsequent arrival at the SNS. The Contractor may also be required to store FDP at its own facility for up to three months. The Contractor may propose a delivery schedule that shall be agreed upon by BARDA and the SNS. Thirty days advance notice is required prior to shipment to the SNS. However, while the product is in long-term storage with the USG (i.e., in the SNS), the Contractor shall continue to be responsible for all quality control/quality assurance monitoring and subsequent reporting necessary to insure appropriate storage conditions of the product until said product is licensed. The Contractor, via this contract with the USG, will be expected to establish a written Quality Agreement as to the manner in which the product will be stored within the specific USG stockpile facility(ies) that have been identified post contract award. In addition, this Quality Agreement will outline the responsibilities of both the Contractor and the USG (i.e., SNS- Quality Control). These documents shall be drafted and signed by both parties prior to the transport and storage of the product.

d) The Contractor shall be responsible for performing studies of [***] and then monitored for potency over time. These studies are required for potential shipment for use during an emergency. Within [***] of study completion, the Contractor is required to submit data from these studies to BARDA, the CDC and the FDA. The Contractor shall also include these data and information regarding the practical use of thawed product on information provided to the end user.

3. Under Section C — Description/Specifications, C.2. REPORTING REQUIREMENTS AND DELIVERABLES, A. Deliverables, 1. Base Contract Deliverables, is revised to modify item (3) and add items (6) and (7). The revised base contract deliverables section is shown below:

A. Deliverables

1. Base Contract Deliverables:

(2) An FDA/CBER approval letter for the BLA for MVA vaccine for post-exposure prophylaxis of healthy adult individuals considered to be at risk subsequent to a known or suspected smallpox virus release.

(3) Evidence, including a summary of salient results, of an ongoing stability monitoring program for stability testing of the retained lots of product stored in the SNS. Information to be provided to BARDA prior to submission to the FDA for approval includes protocols and SDP’s.

(4) A security plan that has received Government concurrency in advance of initiating work at any facility performing under this contract.

(5) Written Quality Agreement between the Contractor and the SNS Quality Control Unit within 6 months of award.

(6) The following information prior to the FDA submission for safety and efficacy studies: final Phase 3 study protocol; all relevant IRB approval forms and all relevant assurance forms; blank copies of case report forms; copy of the unsigned consent form

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(7) Proof of enrollment for the first 500 individuals on the Phase 3 clinical study.

(8) Data from potency studies at [***].

4. Under Section F — Deliveries or Performance, F.4. CONTRACT DELIVERABLES, is revised to add item #6 to the contract deliverables as shown below. This item relates to the Phase 3 clinical study to support a Biological License Applications (BLA). These deliverables were previously included in the Performance Based Payment.

F.4. CONTRACT DELIVERABLES

A. Base Contract Requirements

Milestones	Deliverable	Quantity	Due Date
6.	[***]	[***]	[***]
7.	[***]	[***]	[***]
8.	[***]	[***]	[***]

5. Under Section G, Contract Administration Data, G. 6. INDIRECT COST RATES (APPLICABLE TO CPFF CLIN’s), is revised to read as follows:

(a) In accordance with Federal Acquisition Regulation (FAR) (48 CFR chapter 1) Clauses 52.216-7(d)(2), “Allowable Cost and Payment” incorporated by reference in this contract in Part II, Section I, the cognizant Contracting Officer representative responsible for negotiating provisional and/or final indirect cost rates is identified as follows:

(b) [***]:

[***]
[***]

All other terms and conditions of the contract are unchanged and remain in full force and effect.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) $0.00 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. IN THE CONTRACT ORDER NO. IN ITEM 10A. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To add a Performance Based Payment (PBP) and conditions at no addittonal cost. No other terms or conditions are changed by this modification. Total Contract Dollar Amount: Total Funds Obligated: Contract Expiration Date: $[***] (unchanged) $[***] (unchanged) June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***], VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 14 Sep 2011 16B. UNITED STATES OF AMERICA [***] 16C. DATE SIGNED 14 Sep 2011 (Signature of person authorized to sign) (Signature of Contracting Officer) (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE FAR 52.243-1 Changes – Fixed Price (August 1987) X B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 4 2. AMENDMENT/MODIFICATION NO. 8 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC. N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

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Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Continuation Sheet

Contract No: HHSO100200700034C
Modification No: 8

Modification No. 008 (the “Mod 8”) to Contract No. HHSO10020700034C (the “Contract”, as modify to the date of Mod 8. (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”). a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A. 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be hound by the terms and conditions hereof,

The Contract is modified as follows:

I. Under Section B, Supplies or Services and Prices/Costs, B,A. ADVANCED
UNDERSTANDINGS, item III. Performance-Based Payment is revised to add a new milestone requirement as shown below:

III. Performance-Based Payment “PBP” - $[***]

By effect of this Mod 8 one. additional PBP is added to the Contract in the amount of $[***] with funding already allotted to the Contract. With the [***] PBP total PBP’s are now
$[***].

In accordance with FAR 32.102, the below listed performance- based payment is authorized based upon the completion of the associated tasks. These performance-based payments are fully recoverable, in the event of default.

[***]

[***]
[***]
[***]
[***]
[***]
[***]
[***]
[***]
[***]
[***]

(End of paragraph 1)

2. [***]

(End of paragraph 2)

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

3. Article F.4. Contract Deliverables will be revised, and made part of the Contract by modification, to include a delivery schedule as a result of achieving an Operational rate of production of [***] at the achievement date of the PBP

(End of paragraph 3)

4. Article F.5. Government Notification prior to Delivery

The Contractor shall notify the Contracting Officer and Contracting Officer Technical Representative in writing (email or letter) at least [***] calendar days prior to each of the Contractor’s proposed deliveries of FDP. After receipt of each notification, the Contracting Officer will either consent or reject that delivery. If the Contracting Officer rejects that delivery, then the Contractor shall not make that delivery. Examples of scenarios when the Contracting Officer may reject the Contractor’s request include but are not limited to USG-personnel unavailability, Contractor non-compliances, or USG excusable delays. If the Contracting Officer consents to that delivery, the Contracting Officer will furnish a location for that delivery to the Contractor at least [***] prior to that delivery.

(End of paragraph 4)

5. Contract Section H - Special Contract Requirements is revised to add the following:

H.22. Conflict of Interest

As of the date of this Modification, the Contractor represents and warrants that, to the best of the Contractor’s knowledge and belief, there are no relevant facts or circumstances which could give rise to an organizational conflict of interest, as defined in FAR Subpart 9.5, or that the Contractor has disclosed all such relevant information. Following execution of this Modification, the Contractor agrees to notify the Contracting Officer promptly that, to the best of its knowledge and belief, no actual or potential conflict of interest exists or to identify to the Contracting Officer any actual or potential conflict of interest the firm may have. In emergency situations, however, work may begin but notification shall be made within five (5) working days. The Contractor agrees that if an actual or potential organizational conflict of interest is identified during performance, the Contractor shall promptly make a full disclosure in writing to the Contracting Officer. This disclosure shall include a description of actions, which the Contractor has taken of proposes to take, after consultation with the Contracting Officer, to avoid, mitigate, or neutralize the actual or potential conflict of interest. The Contractor shall continue performance until notified by the Contracting Officer of any contrary action to be taken. Remedies include termination of this contract for convenience, in whole or in part, if the Contracting Officer deems such termination necessary to avoid an organizational conflict or interest. If the Contractor was aware of a potential organizational conflict of interest as of the date of execution of the Modification or discovered an actual or potential conflict after the date of execution of this Modification and did not disclose it or misrepresented relevant information to the Contracting Officer, the Government may terminate the contract for default, debar the Contractor from Government contracting, or pursue such other remedies as may be permitted by law or this contract.

H.23. Release of Contractor Confidential Information

(a) The Department of Health and Human Services (“HHS”) may find it necessary to release information submitted by the Contractor pursuant to the provisions of this contract, to individuals not employed by HHS with whom HHS has entered into confidentiality/non-disclosure agreements. Information that is ordinarily entitled to confidential treatment under applicable law may be included in the information released to these individuals. Accordingly, by signature on this contract or other contracts, Contractor hereby consents to a

limited release of its confidential information (“CI”) provided that such information is not released to other companies that manufacture MVA.

(b) Possible circumstances where HHS may release the Contractor’s CI to entities that are under confidentiality/non-disclosure agreements with HHS include, but are not limited to, the following:

(1) To HHS support service contractors tasked with assisting HHS in the administration, evaluation, audit, or handling and processing information and documents in the award, administration, or termination of HHS contracts.

(2) To entities such as the Government Accountability Office, boards of contract appeals, and courts of competent jurisdiction in the resolution of solicitation or contract protests and disputes.

(3) To HHS contractor employees engaged in information systems analysis, development, operation, and maintenance, including performing data processing and management functions for HHS.

(4) Pursuant to a court order or court-supervised agreement.

(c) HHS recognizes an obligation to protect the Contractor from competitive harm that may result from the release of CI to a competitor. Except where otherwise provided by law, HHS will only permit the release of CL pursuant to a confidentiality/non-disclosure agreement.

(d) This clause does not authorize HHS to release the Contractor’s CI to the public pursuant to a request filed under the Freedom of Information Act unless required to do so by the Act.

(e) The Contractor agrees to include this clause, including this paragraph (e), in all subcontracts executed after the date of this Modification at any tier awarded pursuant to this contract that require the furnishing of confidential business information by the subcontractor.

(End of paragraph 5)

Each Party represents and warms to the other Party that Mod 8’s terms, conditions. and forms of expressions were negotiated and bargained by and between the Parties. Except for the Contract changes effectuated by Mod 8, each Contract term and condition survives Mod 8 unaltered, unaffected and in full force and effect.

[End of Modification No. 8 and the remainder of this page intentionally left blank)

All other terms and conditions of the contract are unchanged and remain in full force and effect.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

HHSO100200700034C 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) Appr. Yr.: 2011 CAN: 1992002 O.C.:25106 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To add funds for the equitable adjustment; add milestone payments for the SNS stability program; and add funds to the Contract for changes made by Modification 7. No other terms or conditions are changed by this modification. Total contract funding is increased by $[***] from $[***]to $[***] Total contract value is increased by $[***] from $[***] to $[***] Contract Expiration Date: June 3, 2012 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990-0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***], VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 29 Sep 2011 16B. UNITED STATES OF AMERICA [***] 16C. DATE SIGNED 29 Sep 2011 (Signature of person authorized to sign) (Signature of Contracting Officer) (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1 and mutual agreement of the parties D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 7 2. AMENDMENT/MODIFICATION NO. 9 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC. N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6) HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Continuation Sheet Contract No.

HHSO100200700034C Mod9

Modification No. 009 (the “Mod 9”) to Contract No. HHSO10020700034C (the “Contract”, as amended to the date of Mod 8, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The Contract is revised as follows:

1. In consideration for work incurred as a result of government direction the following activities are being reimbursed for payment.

Item		FFP

[***]		$	[***]
[***]		[***]
[***]		[***]
[***]		[***]
	Total:	[***]

BN may invoice for $[***] upon execution of this Mod 9.

2. Funding in the amount $[***] is added to CLIN 0001 for changes made by Mod 7. The funding is subject to Section B.4 Advanced Understandings, III. Performance Based Payments (‘‘PBP”). The milestone payments are shown below:

a.[***]

i.[***]

b.[***]

i.[***]

c.[***]

i.[***]

[***]

1)[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

d.[***]

i.[***]

[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]

e.[***]

i.[***]

[***]

[***]		[***]		[***]		[***]		[***]		[***]
[***]		[***]		[***]		[***]		[***]		[***]

[***]

1)[***]

[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

[***]

3. Additional funding allotted to CLIN 0001 by effect of this Mod 9 is $[***]

Item		FFP
[***]		$	[***]
[***]		[***]
[***]		[***]
[***]		[***]
	Subtotal:	[***]

[***]		[***]
[***]		[***]
[***]	Total:	[***]

Each Party represents and warrants to the other Party that Mod 9’s terms, conditions, and forms of expressions were negotiated and bargained by and between the Parties. Except for the Contract changes effectuated by Mod 9, each Contract term and condition survives Mod 9 unaltered, unaffected and in full tierce and effect.

[End of Modification No. 9 and the remainder of this page intentionally left blank]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

NO. 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATEION DATA (if required) Appr. Yr.: 2011 CAN: 1992002 O.C.:25106 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. FAR 52.217-7 Option for Increased Quantity – Separately Priced Line item (March 1989); and E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To extend the period of performance, including Economic Price Adjustment, add funds and exercise the option for additional [***] subjects to a Phase III study and related costs, purchase product for clinical trials, and include long term storage. No other terms or conditions are changed by this modification. Total contract funding is increased by $[***] from $[***] to $[***] Total contract value is increased by $[***] from $[***] to $[***] Contract Expiration Date: June 3, 2017 (changed from June 3, 2012) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990—0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 15A. NAME AND TITLE OF SIGNER (Type or print) [***], EXECUTIVE VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 9 May 2012 16B. UNITED STATES OF AMERICA [***] 16C. DATE SIGNED 9 May 2012 (Signature of person authorized to sign) (Signature of Contracting Officer) (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 52.243-1 Changes – Fixed Price (August 1987); Mutual agreement of the parties. D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 4 2. AMENDMENT/MODIFICATION NO. 10 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC. OS88708 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Modification No. 0010 (the “Mod 10”) to Contract No. HHSO10020700034C (the “Contract”, as amended to the date of Mod 9, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The Contract is revised as follows:

I. Extend the Period of Performance of this contract from June 3, 2012, until June 3, 2017.

II. Pursuant to Section B.4. Advance Understandings, 3. Economic Price Adjustment — PPI Increases to Subcontractor Prices, three (3) separate EPA requests for prior years’ filling operations are hereby approved.

Table 1 — EPA Request

	EPA Request	2009	2010	2011	Total
CLIN 0016	[***]	[***]	[***]	[***]	[***]
	[***]	[***]	[***]	[***]	[***]
	[***]	[***]	[***]	[***]	[***]
	[***]	[***]	[***]	[***]	[***]

Terms and Conditions for payment: BN may invoice for $[***] upon execution of this Modification # 10.

III. Pursuant to Section H.14 Option Provision, this modification incorporates the additional subjects and work required to complete the FDA approved Phase III study, PDX-MVA-013; the FDA have confirmed the Phase III study design (PDX-MVA-013) on September 14, 2011.

In accordance with Optional CLIN 0007, this modification includes the authorization and charge for the additional [***] subjects at the contract established price ($[***] per additional [***] subjects) for any subjects over the originally planned [***] subjects,

Table 2— Additional Subjects

	Description	Amount (FFP)		Total (FEP)
CLIN 0007	Additional [***] Subjects per CLIN 0007	$	[***]	$	[***]

Terms and Conditions for payment: The above referenced amount may be invoiced in [***] installments:

[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

IV. This modification incorporates the cost for additional work required by the FDA to perform the clinical trial since the per patient cost was negotiated prior to the discovery of cardiac complications associated with second generation smallpox vaccines and prior to the decision of the FDA to add a placebo arm and use co-primary endpoints with two immunological markers of efficacy from the blood draws. The total cost is inclusive of all indirect costs and profit. Additional costs are as follows:

Table 3 — Additional related costs

	Description	Amount		Total (FFP)
CLIN 0017	[***]	$	[***]	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	Total for additional subjects and costs			$	[***]

Terms and Conditions for payment: The above referenced amount may be invoiced in [***] installments:

[***]

V. This modification incorporates the purchase of [***] doses of IMVAMUNE from [***] at the dose price of $[***] per dose.

Table 4— Additional Doses for clinical trials

	Description	Price per dose		Total (FFP)
CLIN 0018	[***]	$	[***]	$	[***]

Terms and Conditions for payment: Invoice shall be submitted upon manufacture and BN Quality Assurance release of the product.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

VI. This modification incorporates the purchase of Optional Long-Term Storage of FDP at BN of up to [***] doses from July 1, 2012 to December 31, 2014.

Table 5— Operational Storage/Shipping Costs

	Description	Price		Total (FFP)
CLIN 0019	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	[***]	$	[***]
	Total Proposed Charges			$	[***]

Terms and Conditions for payment: Payment Schedule is as follows:

Table 6 — Payment Schedule

[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]

[***]

Each Party represents and warrants to the other Party that Mod 10’s terms, conditions, and forms of expressions were negotiated and bargained by and between the Parties. Except for the Contract changes effectuated by Mod 10, each Contract term and condition survives Mod 10 unaltered, unaffected and in full force and effect.

[End of Modification No. 10]

All other terms and conditions of the contract are unchanged and remain in full force and effect.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 2 2. AMENDMENT/MODIFICATION NO. 11 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC OS100645 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/BARDA 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Bogeskovvej 9 3490 Kvistgard Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted. such change may be made by telegram or letter, provided each telegram or letter makes reverence to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Appr. Yr.:2012CAN: 1990001D.O.: 25106 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 52.243-1 Changes – Fixed Price (August 1987); and Mutual agreement of the parties. D.OTHER (Specify type of modification and authority) E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To incorporate studies needed to support long-term storage of frozen Bulk Drug Substance. No other terms or conditions are changed by this modification. Total Contract funding is increased by $[***] from $[***] to $[***] Total contract value 1s increased by $[***] from $[***] to $[***] Contract Expiration Date remains unchanged at June 3, 2017. Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER (Type or print) [***], EXECUTIVE VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 27 Sep. 2012 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED 27 Sep. 17, 2012 (Signature of person authorized to sign)

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Modification No. 0011 (the “Mod 11”) to Contract No. HHSO10020700034C (the “Contract”, as amended to the date of Mod 10, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America — which is represented by the Department of Health and Human Services — and Bavarian Nordie (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The Contract is revised as follows:

1. This modification incorporates the purchase of studies needed to support Long-Term Storage of frozen Bulk Drug Substance (BDS), including studies to determine the appropriate storage container and to collect long-term stability data an frozen BDS, for a firm fixed price (FFP). The technical proposal for these services, dated June 11 1012, is incorporated herein by reference.

Table 1 — Long-Term Storage of frozen Bulk Drug Substance

		Description		Total (FFP)
CLIN 0020		Long-Term Storage of frozen Bulk Drug Substance		$	[***]

Terms and Conditions for payment: The Deliverables and Payment Schedule are as follows:

Table 2 — Deliverables and Payment Schedule

Payment Milestone	Milestone Description	Deliverable	Due Date	Payments		%
Milestone 1	[***]	[***]	[***]	$	[***]	[***]
Milestone 2	[***]	[***]	[***]	$	[***]	[***]
Milestone 3	[***]	[***]	[***]	$	[***]	[***]
Milestone 4	[***]	[***]	[***]	$	[***]	[***]
Milestone 5	[***]	[***]	[***]	$	[***]	[***]
Milestone 6	[***]	[***]	[***]	$	[***]	[***]
Total Proposed Pricing				$	[***]

Milestone payments may be invoiced on the completion of each milestone (as referenced in the·above table).

Each Party represents and warrants to the other Party that Mod 11’s terms, conditions, and forms of expressions were negotiated and bargained by and between the Parties. Except for the contract changes effectuated by Mod 11, each Contract term and condition survives Mod 11 unaltered, unaffected and in full force and effect.

[End of Modification No. 11]

All other terms and conditions of the contract are unchanged and remain in full force and effect.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 3 2. AMENDMENT/MODIFICATION NO. 12 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC OS110225 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgard Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Appr. Yr.:2013CAN: 1990001O.C.: 25106Amount: $[***] 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: Section B.4. Advanced Understandings. 3. Economic Price Adjustment – PPI Increases Subcontractor Prices, and FAR 52.243-1, Changes – Fixed Price (Aug. 1987) D.OTHER (Specify type of modification and authority) E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: 1) To make a payment unde3r Section B.4. Advanced Understandings, 3. Economic Price Adjustment – PPI Increases to Subcontractor Prices under CLIN 0016, and 2) add funding to CLIN 0005 Security of Contract Operations. No other terms or conditions are changed by this modification. Total Contract funding is increased by $[***] from $[***] to $[***] Total contract value 1s increased by $[***] from $[***] to $[***] Contract Expiration Date remains unchanged at June 3, 2017. Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER (Type or print) [***], EXECUTIVE VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 12 Apr. 2013 16B. UNITED STATES OF AMERICA BY [***] (Signature of Contracting Officer) 16C. DATE SIGNED 12 Apr. 2013 (Signature of person authorized to sign)

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Modification No. 0012 (the “Mod 12”) to Contract No. HHSO10020700034C (the “Contract”, as amended to the date of Mod 11, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services — and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The Contract is revised as follows:

I. Under Section B — SUPPLIES OR SERVICES AND PRICES/COSTS, B.2 “Prices/Costs,” within paragraph A.2., CLIN 0005 is revised to reflect an increased dollar amount as the result of an extended delivery schedule. CLIN 0005 is increased by $[***] of which $[***] represents the estimated reimbursable costs and $[***] represents the fixed-fee. These amounts also represent the total amount of funds currently available for payment and allotted under the CPFF portion of this contract. This amount shall cover performance of the contract through the deliverable schedule. CLIN 0005 is revised as follows:

CLIN		Supply Service		Est. Cost		Fixed Fee		Total
0005		Security of Contract Operations		$[***]		$[***]		$[***]

[***].

II. Pursuant to Section B.4. Advance Understandings, 3. Economic Price Adjustment — PPI Increases to Subcontractor Prices, BARDA is providing an Economic Price Adjustment payment in the amount of $[***] under CLIN 0016.

[***].

III. Pursuant to Section B.4. Advance Understandings, 3. Economic Price Adjustment — PPI Increases to Subcontractor Prices, upon award(s) of a single or multiple options greater than [***] doses, beyond the original 20 million dose base contract, BARDA will provide a further Economic Price Adjustment payment in the amount of $[***] under CLIN 0016. If amount of order is less than [***] doses, then Economic Price Adjustment shall be prorated proportional to the size of the order.

Terms and Conditions for payment: BN may invoice for $[***] upon execution of any optional award whereby the total cumulative ordered doses exceed [***]. If the amount of order is less than [***] doses then the Economic Price Adjustment shall be prorated proportional to the size of the order.

IV. Pursuant to Section B.4. Advance Understandings, 5. [***]% Licensure Hold-Back. The text of this clause as currently written into the contract is hereby deleted and replaced with the following:

5. [***]% Licensure Hold-Back on CLIN 1 Base Contract Deliveries

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 3 2. AMENDMENT/MODIFICATION NO. 13 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC OS110225 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgard Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Appr. Yr.:2013CAN: 1990001O.C.: 26402Amount: $[***] 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 52.243-1 Changes – Fixed Price (August 1987); and Mutual agreement of both parties. D.OTHER (Specify type of modification and authority) E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSE: To order [***] doses of MVA; establish dose price tor subsequent order of [***], incorporate delivery schedule tor dose order, and add performance based payments No other tcm1s or conditions arc changed by this modification. Total contract funding is increased by $[***] from $[***] to $[***] Total contract value is increased by $[***] from $[***] to $[***] Contract Expiration Date remains unchanged at June 3, 2017. Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER (Type or print) [***], EXECUTIVE VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 12 Apr. 2013 16B. UNITED STATES OF AMERICA BY [***] (Signature of Contracting Officer) 16C. DATE SIGNED 12 Apr. 2013 (Signature of person authorized to sign)

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Modification No. 0013 (the “Mod 13”) to Contract No. HHSO10020700034C (the “Contract”, as amended to the date of Mod 12, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services — and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The Contract is revised as follows:

I. This modification is for the purchase of [***] doses of IMVAMUNE at a dose price of $[***] per dose for a total of $100,000,000. CLIN 0021 is hereby added to Section B as follows:

CLIN	Description	Units	Unit Price		Total
CLIN 0021	Production of Additional Vaccine Doses	[***]	$	[***]	$	[***]

Optional Order of 4,000,000 doses

CLIN	Description	Units	Unit Price		Total
CLIN 0022	Production of Additional Vaccine Doses	[***]	$	[***]	$	[***]

*Subject to the availability of funds, the government intends to order [***] additional doses at the CLIN 0021 dose price of $[***] per dose and under the same referenced below terms and conditions for payment in fiscal year 2014. Partial orders of the CLIN 0022 dose requirement may occur in fiscal year 2013.

Pending funding availability, ASPR intends to maintain the U.S. stockpile of IMVAMUNE and the necessary manufacturing capacity through future orders, as needed.

Terms and Conditions for payment:

1. Performance-Based Payment (PBP) - [***][***]% of CLIN 21 value)

In accordance with FAR 32.10, the below listed performance- based payments are authorized based upon the completion of the associated tasks. These performance-based payments are fully recoverable, in the event of default of the option exercised in this Modification No. 13.

Task 1: [***]

For payment, BN shall submit to BARDA for review and concurrence [***] documentation supporting the [***] of this CLIN 21 order.

Task 2: [***]

For payment, BN shall submit to BARDA for review and concurrence [***] documentation supporting the [***] of this CLIN 21 order.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Task 3: [***]

For payment, BN shall submit to BARDA for review and concurrence [***] documentation supporting the [***] of this CLIN 21 order.

Task 4: [***]

For payment, BN shall submit to BARDA for review and concurrence [***] documentation supporting the [***] of this CLIN 21 order.

2. Invoice shall be submitted upon delivery of product to government specified location and government acceptance of product. As with the base contract, the $[***] dose price will be proportionally reduced based on the amount of PBPs paid at the time of each delivery. For example, if all [***] is paid out (all four PBPs) the invoiceable dose price will be reduced by [***]) to a revised invoiceable dose price of $[***].

II. Section F.4. Contract Deliverables is revised to add the following delivery schedule for doses received under CLIN 0021.

F.4.C. Delivery Schedule for CLIN 0021

DATE		Quantity
[***]		[***]
[***]		[***]
[***]		[***]
Total		[***]

[***]

Each Party represents and warrants to the other Party that Mod 13’s terms, conditions, and forms of expressions were negotiated and bargained by and between the Parties. Except for the Contract changes effectuated by Mod 13, each Contract term and condition survives Mod 13 unaltered, unaffected and in full force and effect.

[End of Modification No. 13]

Remainder of page intentionally left blank.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

ADMINISTERED BY (If other than Item 6) CODE appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 14 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BY 7. See N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 WASHINGTON, D.C. 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Barvarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE FACILITY CODE 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractor is not, is required to sign this document and return1 Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to (1) update the Contracting Officer and Project Officer in Section D and clause G.1. Project Officer and to (2) remove the requirement for one hard copy of the technical monthly progress report in Clause F.3. Technical Report Requirement. The cost to complete remains unchanged. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER (Type or print) 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR (Signature of person authorized to sign) 15C. DATE SIGNED 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED 9/24/13 NSN 754001-152-8070

Previous Edition Unusable

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C
Modification No: 014	(continuation sheet)

	Contract No: HHSO100200700034C
Continuation Sheet	Modification No: 14

The base contract award is revised as follows:

SECTION D—PACKAGING, MARKING AND SHIPPING

1. Report Deliverables

[***]

F.3. TECHNICAL REPORT REQUIREMENT

Item		Deliverable		Quantity		Due Date
1.		Technical Monthly Progress Report		1 Electronic Copy — Project Officer (PO) 1 Electronic Copy — Contracting Officer (CO)		30 days after contract award and by the 15th day of each month during the contract’s period of performance. Not due when Final is due.

SECTION G.—CONTRACT ADMINISTRATION DATA

G.1. PROJECT OFFICER

The following Project Officer and Alternate Project Officer will represent the Government for the purpose of this contract:

[***]

[End of Modification No. 14 and the remainder of this page intentionally left blank]

page 2 of 2

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

ADMINISTERED BY (If other than Item 6) CODE appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). 52.243-1 Fixed Price-Changes and mutual agreement of both parties AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 15 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BY 7. See N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 WASHINGTON, D.C. 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Barvarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) X 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: $[***] 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractor is not, is required to sign this document and return1 Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to (I) add a lot of Bulk Drug Substance (BDS) material to replace one previously on the contract and (2) update the milestone in the Deliverables and Payment Schedule for the Long-Term Study. The total contract funding is increased $[***] from $[***] to $[***]. The total contract value is increased $[***] from $[***] to $[***]. Contract expiration date remains unchanged from June 3, 2017. Except as provided herein, all terms and conditions of the document referenced in Item 9A or lOA, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER (Type or print) [***], CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 3 July 2014 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED 9/24/13 (Signature of person authorized to sign)

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C
Modification No: 015	(continuation sheet)

	Contract No: HHSO100200700034C
Continuation Sheet	Modification No: 15

The contract is revised as follows:

1. This modification incorporates the purchase of an additional lot of Bulk Drug Substance (BDS) material for the long-term study. The proposal for these services dated May 5, 2014 is herein incorporated by reference. CLIN 20 is increased $[***] from $[***] to $[***].

Table 1— Long Term Storage of Bulk Drug Substance

	Description	Total (FFP)
CLIN 20	Long-Term Storage of frozen Bulk Drug Substance	$	[***]

Terms and Conditions for Payment: The Deliverables and Payment schedule are as follows:

Date	Quantity	Deliverables	Due Date	Payments
Milestone 1	[***]	[***]	[***]	[***]
Milestone 2	[***]	[***]	[***]	[***]
Milestone 3	[***]	[***]	[***]	[***]
Milestone 4	[***]	[***]	[***]	[***]
Milestone 5	[***]	[***]	[***]	[***]
Milestone 6	[***]	[***]	[***]	[***]
Milestone 7	[***]	[***]	[***]	[***]
Milestone 8	[***]	[***]	[***]	[***]
Total				[***]

Page 1 of 2

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C Modification No: 015 Page 1 of 2 (continuation sheet) 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. It by virtue of this amendment, you desire change an offer already submitted. such change may be made by telegram or letter, provided each telegram or letter makes reverence to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Obligation: $[***] EIN: CAN: Appropriation: O.C. 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to (1) make payment under Section B.4. Advanced Understandings 3. Economic Price Adjustment – PPI increase to Subcontractor Price under CLIN 16 and (2) exercise the Optional Order of [***] doses (CLIN 23). Total Contract funding is increased by $[***] from $[***] to $[***]. Total contract value 1s increased by $[***] from $[***] to $[***] Contract Expiration Date remains unchanged at June 3, 2017. Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. [***] 15A. NAME AND TITLE OF SIGNER (Type or print) President & CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 4 September 2014 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED (Signature of person authorized to sign) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1 D.OTHER (Specify type of modification and authority) FAR 17.207 AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 2 2. AMENDMENT/MODIFICATION NO. 16 3. EFFECTIVE DATE See Item 16C. 4. REQUISITION/PURCHASE REQ. NO OS140193 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE N/A 7. A See DMINISTERED BY (If other than Item 6)CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, Room G640 Washington, DC 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Barvarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgård Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE: N/A FACILITY CODE: N/A

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C
Modification No: 016	(continuation sheet)

	Contract No: HHSO100200700034C
Continuation Sheet	Modification No: 16

The contract is revised as follows:

1. In accordance with Modification 12, pursuant to Section 8.4. Advance Understandings, 3, Economic Price Adjustment - PPI Increases to Subcontractor Prices, upon award(s) of a single or multiple options greater than [***] doses, beyond the original [***] does base contract, BARDA will provide a further Economic Price Adjustment payment in the amount of [***] under CLIN 00016.

Terms and Conditions for Payment: BN may invoice for $[***] upon execution of this modification.

2. This modification is for the purchase of [***] doses of IMVAMUNE at a dose price of $[***] per dose for a total of $[***]. CLIN 0023 is exercised.

Optional Order of [***] doses

	Description	Units	Unit Price		Total
CLIN 0023**	Production of Additional Vaccine Doses	[***]	$	[***]	$	[***]

Section F.4. Contract Deliverables is revised to add the following delivery schedule for doses received under CLIN 0023.

F.4.C. Delivery Schedule for CLIN 0023

Date		Quantity
[***]		[***]
[***]		[***]

The Strategic National Stockpile cannot accept early deliveries.

[***]

**CLIN 0023 was previously referred to as CLIN 0022 in Modification 13.

[End of Modification No. 16 and the remainder of this page intentionally left blank]

Page 2 of 2

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. It by virtue of this amendment, you desire change an offer already submitted. such change may be made by telegram or letter, provided each telegram or letter makes reverence to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Obligation: $[***] EIN: CAN: Appropriation: O.C. 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to (1) add $[***] to CLIN 5 for the Indirect Rate Adjustment based on the incurred cost audit for fiscal years 2006, 2011, 2012, and 2013 and (2) update the clause G.2. Key Personnel. The total contract funding is increased by $[***] from $[***] to $[***]. The total contract value is increased by $[***] from $[***] to $[***]. Contract Expiration Date remains unchanged at June 3, 2017. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. [***] 15A. NAME AND TITLE OF SIGNER (Type or print) President & CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 5/11/14 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED (Signature of person authorized to sign) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). X C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 52.243-2 D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 17 3. EFFECTIVE DATE See Item 16C. 4. REQUISITION/ PURCHASE REQ. NO OS140193 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE N/A 7. A See DMINISTERED BY (If other than Item 6)CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, Room G640 Washington, DC 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Barvarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgård Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE: N/A FACILITY CODE: N/A

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 3 2. AMENDMENT/MODIFICATION NO. Modification 18 3. EFFECTIVE DATE See Item 16C. 4. REQUISITION/PURCHASE REQ. NO N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BY CODE N/A 7. ADMINISTERED BY (If other than Item 6) CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, Room G640 Washington, DC 20201 See Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Barvarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgård Denmark • 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. It by virtue of this amendment, you desire change an offer already submitted. such change may be made by telegram or letter, provided each telegram or letter makes reverence to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) EIN: CAN: Appropriation: O.C. Obligation: 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. • A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). • C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: • D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to (1) update the invoicing instructions in G.4 Invoice Submission. The cost to complete remains unchanged. See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER (Type or print) 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR (Signature of person authorized to sign) 15C. DATE SIGNED 4 September 2014 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C
Modification No: 018	(continuation sheet)

	Contract No: HHSO100200700034C
Continuation Sheet	Modification No: 18

The base contract award is revised as follows:

G. 4. INVOICE SUBMISSION

(a) Documents should be delivered electronically to the Contracting Officer (CO), the Contracting Officer’s Representative (COR) and PSC electronically. Unless otherwise specified by the Contracting Officer all deliverables and reports furnished to the Government under the resultant contract (including invoices) shall be addressed as follows:

[***]	[***]	Email invoices to:
[***]	[***]
[***]	[***]	[***]
[***]	[***]
[***]	[***]
[***]	[***]

(b) The Contractor agrees to include (as a minimum) the following information on each invoice for firm fixed price CLIN’s:

(1) Contractor’s Name & Address

(2) Contractor’s Tax Identification Number (TIN)

(3) Contract Number

(4) Invoice Number

(5) Invoice Date

(6) Contract Line Item Number

(7) Quantity

(8) Unit Price & Extended Amount for each line item

(9) Total Amount of Invoice

(10) Name, title and telephone number of person to be notified in the event of a defective invoice

(11) Payment Address, if different from the information in (c)(1).

(End of Clause)

Invoice Submission — (Cost-Plus Fixed-Fee CLIN’s)

(Original Signature of Authorized Official)

Typed Name and Title of Signatory

Page 2 of 3

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGEMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. It by virtue of this amendment, you desire change an offer already submitted. such change may be made by telegram or letter, provided each telegram or letter makes reverence to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Obligation: $[***] EIN: CAN: Appropriation: O.C. 13. THIS ITEM ONLY APPLIES TO MODIFICATION OF CONTRACTS/ORDERS. IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. THE CONTRACT ORDER NO. IN ITEM 10A. paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 1 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to modify the language in (1) Section B.1, (2) Section C.I.D.2, (3) Section C.2.A.2, and (4) Section F.4.B.2. The total contract funding is increased by $[***] from $[***] to $[***]. The total contract value is increased by $[***] from $[***] to $[***]. Contract Expiration Date remains unchanged at June 3, 2017. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. [***] 15A. NAME AND TITLE OF SIGNER (Type or print) President & CEO 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR [***] 15C. DATE SIGNED 5/11/14 16B. UNITED STATES OF AMERICA [***] (Signature of Contracting Officer) 16C. DATE SIGNED (Signature of person authorized to sign) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 52.243-1 D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 3 2. AMENDMENT/MODIFICATION NO. Modification 19 3. EFFECTIVE DATE See Item 16C. 4. REQUISITION/ PURCHASE REQ. NO OS157368 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE N/A 7. A See DMINISTERED BY (If other than Item 6)CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, Room G640 Washington, DC 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Barvarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgård Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100200700034C 10B. DATED (SEE ITEM 13) June 4, 2007 CODE: N/A FACILITY CODE: N/A

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100200700034C
Modification No: 019	(continuation sheet)

	Contract No: HHSO100200700034C
Continuation Sheet	Modification No: 19

The contract is revised as follows:

1. Update Section B. Contract Options, 1. Firm Fixed Price (FFP), CLIN 8 and CLIN 9 to read:

	Description	Units	Unit Price	Total
CLIN 0008	[***]	[***]	[***]	$	[***]
CLIN 0009	[***]	[***]	[***]	$	[***]

2. Update Section C.1. Statement of Work, D. Contract Options, 2 to read:

2. Manufacture and store bulk drug substance to support future manufacturing activities. Consideration by the USG for this option will be based on the availability of long-term stability data to support storage of the intermediate product.

a. The BDS shall be manufactured under cGMP conditions and meet the specifications determined by the FDA/CBER for licensure (Requirement 1a, IV. Specific Technical Requirements). The BDS must minimally meet current specifications as approved by BARDA.

b. [***] (prior to long-term storage and/or eventual filling). All certificates of analysis for the [***] titer results shall be submitted to BARDA for review and approval. The new BDS specification for potency must [***] to potentially support lyophilization.

c. [***] shall be based on the [***] contained within each [***]. Criteria for achieving the minimum [***] will be based on the average for all [***] batches. [***].

d. To ensure that the USG has the flexibility to maintain a BDS stockpile, BN shall establish and validate BDS storage capacity, including: installation and validation of [***] cold-storage containers (for -50°C storage). Cold storage capacity shall be funded by and charged to the USG for a period of [***] starting on [***]. Cold storage capacity shall be charged on a monthly basis as established in CLIN 9 of this modification. Storage periods after the initial [***] shall be charged on a monthly basis and escalated annually at [***].

Page 2 of 3

Exhibit 10.2

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

16. TABLE OF CONTENTS CONTRACTING OFFICER WILL COMPLETE ITEM 17 OR 18 AS APPLICABLE NSN 7540-01-152-8069 PREVIOUS EDITION UNUSABLE 26-107 Computer Generated STANDARD FORM 26 (REV. 4-85) Prescribed by GSA, FAR (48 CFR) 53.214(a) 123269097 v2 17. CONTRACTOR’S NEGOTIATED AGREEMENT (Contractor is 18. AWARD (Contractor is not required to sign this document.) Your offer on required to sign this document and return 2 copies to issuing office.) Contractor agrees to furnish and deliver all items or perform all the services set forth or otherwise identified above and on any continuation sheets for the consideration stated herein. The rights and obligations of the parties to this contract shall be subject to and governed by the following documents: (a) this award/contract, (b) the solicitation, if any, and (c) such provisions, representations, certifications, and specifications, as are attached or incorporated by reference herein. (Attachments are listed herein.) Solicitation Number , including the additions or changes made by you which additions or changes are set forth in full above, is hereby accepted as to the terms listed above and on any continuation sheets. This award consummates the contract which consists of the following documents: (a) the Government’s solicitation and your offer, and (b) this award/contract. No further contractual document is necessary. 19A. NAME AND TITLE OF SIGNER (Type or print) [***] [***] 20A. NAME OF CONTRACTING OFFICER [***] 19B. NAME OF CONTRACTOR /s/ [***] (Signature of person authorized to sign) 19C. DATE SIGNED 13/11 ‘09 20B. UNITED STATES OF AMERICA BY /s/ [***] (Signature of Contracting Officer) 20C. DATE SIGNED November 16, 2009 () SEC. DESCRIPTION PAGE(S) () SEC. DESCRIPTION PAGE(S) PART I - THE SCHEDULE PART II - CONTRACT CLAUSES A SOLICITATION/CONTRACT FORM 1 I CONTRACT CLAUSES 20 B SUPPLIES OR SERVICES AND PRICE/COST 2 PART III - LIST OF DOCUMENTS, EXHIBITS AND OTHER ATTACH. C DESCRIPTION/SPECS./WORK STATEMENT 4 J LIST OF ATTACHMENTS 24 D PACKAGING AND MARKING 8 PART IV - REPRESENTATIONS AND INSTRUCTIONS E INSPECTION AND ACCEPTANCE 9 K REPRESENTATIONS, CERTIFICATIONS AND OTHER STATEMENTS OF OFFERORS 25 F DELIVERIES OR PERFORMANCE 10 G CONTRACT ADMINISTRATION DATA 11 L INSTRS., CONDS., AND NOTICES TO OFFERORS N/A H SPECIAL CONTRACT REQUIREMENTS 14 M EVALUATION FACTORS FOR AWARD N/A AWARD/CONTRACT 1. THIS CONTRACT IS A RATED ORDER UNDER DPAS (15 CFR 350) RATING N/A PAGEOFPAGES 1 25 2. CONTRACT (Proc. Inst. Ident.) NO HHSO100201000011C 3. EFFECTIVE DATE See Block 20C 4. REQUISITION/PURCHASE REQUEST/PROJECT NO N/A 5. ISSUED BYCODE N/A 6. ADMINISTERED BY (If other than Item 6)CODE N/A HHS/OS/ASPR/BARDA 330 INDEPENDENCE AVE S.W., RM G640 WASHINGTON, D.C. 20201 See Block 5 7. NAME AND ADDRESS OF CONTRACTOR (No., street, county, state and ZIP Code) BAVARIAN NORDIC A/S Hejreskovvej 10A 3490 Kvistgård Denmark 8. DELIVERY FOB ORIGINOTHER (See below) 9. DISCOUNT FOR PROMPT PAYMENT N/A 10. SUBMIT INVOICES ADDRESS SHOWN IN ITEM See Section G FACILITY CODEN/A 11. SHIP TO/MARK FORCODE N/A 12. PAYMENT WILL BE MADE BYCODE N/A See Block 5 See Block 5 13. AUTHORITY FOR USING OTHER FULL AND OPEN COMPETITION: 10 U.S.C. 2304(c)() 41 U.S.C. 253(c)() 14. ACCOUNTING AND APPROPRIATION DATA 15A. ITEM NO. 15B. SUPPLIES/SERVICES 15C. QUANTITY 15D. UNIT 15E. UNIT PRICE 15F. AMOUNT See Section B $[***] 15G. TOTAL AMOUNT OF CONTRACT $[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100201000011C

Bavarian Nordic A/S

SECTION B—SUPPLIES OR SERVICES AND PRICES/COSTS

B.1. BRIEF DESCRIPTION OF SUPPLIES OR SERVICES

The Contractor shall supply the necessary supplies and services to produce and validate a freeze-dried IMVAMUNE Final Drug Product (FDP) to generate sufficient data to support the use of this smallpox vaccine in a declared emergency.

B.2 PRICES/COSTS

A. CONTRACT LINE ITEM NUMBERS (CLIN’s)

1. BASE CONTRACT

CLIN’s

SUPPLIES/SERVICES

EST. COST

FIXED
FEE

TOTAL
EST. CPFF

0001

[***]

2. CONTRACT OPTIONS

If the Government exercises its option pursuant to Section H, Paragraph H.13 of this contract, the Government’s total obligation represented by the sum of the estimated cost plus fixed fee may be increased as shown in the below CLIN’s 0002 through 0005, in consideration for completion of the work described in the individual CLIN’s and in accordance with the Statement of Work:

CLIN’s

DESCRIPTION

EST. COST

FIXED FEE

TOTAL
EST. CPFF

0002

[***]

0003

[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

CLIN’s

DESCRIPTION

EST. COST

FIXED FEE

TOTAL
EST. CPFF

0004

[***]

0005

[***]

B.3. PROVISIONS APPLICABLE TO DIRECT COSTS

This paragraph applies only to the cost reimbursable CLIN’s. Notwithstanding the clauses, ALLOWABLE COST AND PAYMENT and FIXED FEE, incorporated in this contract, unless authorized in writing by the Contracting Officer, the cost of the following items or activities shall be unallowable as direct costs: 1) Acquisition, by purchase or lease, of any interest in real property; 2) Special rearrangement or alteration of facilities; 3) Purchase or lease of any item of general purpose office furniture or office equipment regardless of dollar value; 4) Subcontract Costs; and 5) Accountable Government Property.

B.4. ADVANCE UNDERSTANDINGS

1) Man-in-Plant

With 7 days advance notice to the Contractor, the Government may place a man-in-plant in the Contractor’s facility. The man-in-plant is restricted to observing, verifying, and surveying the contractor’s performance under this contract.

2) Security Plan

The Contractor agrees to provide an updated Security Plan, if requested by the Project Officer, and within fifteen (15) working days after receipt of the request. The Contractor shall only produce and store product in a secure facility. In addition, all work performed under this contract shall be in accordance with the implemented security plan- ensuring the security of vaccine production.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SECTION C - DESCRIPTION/SPECIFICATIONS

C.1. STATEMENT OF WORK

A. Independently, and not as an agent of the USG, the Contractor shall furnish all the necessary services, qualified personnel, materials, supplies, equipment, facilities, transportation and travel not otherwise provided by the USG as required to perform the specific Contractor Defined Milestones detailed below for the base contract, as further specified in the Work Statement, which is incorporated into this contract as Attachment #1 under SECTION J.

Description		Statement of Work Section Number
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]

B. CONTRACT OPTIONS

The Government may exercise any of the four options for the continuation of requirements as set forth in the following Contractor Defined Milestones. Exercise of each option also extends the contract’s period of performance by twelve months.

Description		Statement of Work Section Number
Option #1
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]

Option #2
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]

Option #3
[***]		[***]

Option #4
[***]		[***]

C. The Government reserves the right to modify the milestones, progress, schedule, budget, or product to add or delete products, process, or schedule as the need may arise. Because of the nature of this research and development contract, and the complexities inherent in this and prior programs, at designated milestones the Government will evaluate whether work should be redirected, removed, or whether schedule or budget adjustments should be made. In any event, the Government reserves the right to change product, process, schedule or event, and to add or delete part or all of these elements as the need arises.

D. MEETINGS AND CONFERENCES

The Contractor shall participate in regular meetings to coordinate and oversee the contract effort as directed by the Contracting and Project Officers. Such meetings may include, but are not limited to, meeting of all Contractors and subcontractors to discuss clinical manufacturing progress, product development, product assay development, scale up manufacturing development, clinical sample assays development, pre clinical/clinical study designs and regulatory issues; meetings with individual contractors and other HHS officials to discuss the technical, regulatory, and ethical aspects of the program; and meeting with technical consultants to discuss technical data provided by the Contractor.

Monthly teleconferences between the Contractor and subcontractors and BARDA shall be held to review technical progress. BARDA reserves the right to request more frequent teleconferences and face-to-face meetings depending on the criticality and nature of the work being performed. The first reporting period consists of the first full month of performance plus any fractional part of the initial month. Thereafter, the reporting period shall consist of each calendar month. During these calls the Contractor’s Principal Investigator will discuss the activities during the reporting period, any problems that have arisen and the activities planned for the ensuing reporting period. The Contractor will receive feedback from BARDA on contract performance, and will have an opportunity to respond and provide recommendations/ remediation plan during the execution of the contract.

1. Regulatory and Quality Management:

FDA Submissions and meetings:

(a) The contractor shall forward the initial draft minutes and final draft minutes of any formal meeting with the FDA to BARDA.

(b) The contractor shall forward the final draft minutes of any informal meeting with the FDA to BARDA.

(c) The contractor shall forward the dates and times of any meeting with the FDA to BARDA and make arrangements for appropriate BARDA staff to attend FDA meetings.

(d) The contractor shall provide BARDA the opportunity to review and comment upon any documents to be submitted to the FDA. The contractor shall provide BARDA with five (5) business days in which to review and provide comments back to the contractor.

(e) The contractor shall forward Standard Operating Procedures (upon request from Project Officer/Contracting Officer).

(f) The contractor shall provide upon request animal study and/or other technology packages developed under this contract. Packages shall include complete protocols and critical reagents for animal models developed and/or improved with contract funding.

(g) The contractor shall provide upon request raw data and/or specific analysis of data generated with USG funds.

2. Audits / Site Visits:

FDA Audits

Within thirty (30) calendar days of an FDA audit of Contractor or subcontractor facilities, the Contractor shall provide copies of the audit findings, final report, and a plan for addressing areas of nonconformance to FDA regulations and guidance for GLP, GMP or GCP guidelines as identified in the final audit report.

BARDA Audits

The United States Government (USG) reserves the right to conduct an audit of the Contractor with 48 hours notice. The USG reserves the right to accompany the Contractor on routine and for-cause site-visits/audits of subcontractors. At the discretion of the USG and independent of testing conducted by the Contractor, BARDA reserves the right to conduct site visits/audits and collect samples of product held by the Contractor and subcontractors.

C.2. REPORTING REQUIREMENTS AND DELIVERABLES

1) Technical Progress Reports

On the fifteenth (15) day of each month for the previous calendar month, the contractor shall submit to the Project Officer and the Contracting Officer a Technical Progress Report. The frequency of Technical Progress Reporting will be determined by

the Contracting Officer and Project Officer during negotiations of the contract. The format and type of Technical Progress Report and Executive Summary will be provided by the Project Officer. The technical Progress Reports will include project timelines and milestones summaries of product manufacturing, testing, and clinical evaluation. A Technical Progress Report will not be required for the period when the Final Report is due. The Contractor shall submit one copy of the Technical Progress Report electronically via e-mail. Any attachments to the e-mail report shall be submitted in Microsoft Word, Microsoft Excel, Microsoft Project, and/or Adobe Acrobat PDF files. Such reports shall include the following specific information:

(a) Title page containing: Technical Progress Report, the contract number and title, the period of performance or milestone being reported, the contractor’s name, address, and other contact information, the author(s), and the date of submission;

(b) Introduction/Background: An introduction covering the purpose and scope of the contract effort;

(c) Progress: The report shall detail, document and summarize the results of work performed, test results, milestones achieved during the period covered and cumulative milestones achieved. Also to be included is a summary of work planned for the next two (2) reporting periods on a rolling basis;

(d) Issues: Issues resolved, new issues and outstanding issues are enumerated with options and recommendation for resolution. An explanation of any difference between planned progress and actual progress, why the differences have occurred, and, if progress activity is delinquent, then what corrective steps are planned. Revised timelines are provided.

(e) Invoices: Summary of any invoices submitted during the reporting period.

(f) Action Items: Summary table of activities or tasks to be accomplished by certain date and by whom.

(g) Distribution list: A list of persons receiving the Technical Report

(h) Attachments: Results on the project are provided as attachments

2) The Executive Summary, which shall accompany each Technical Progress Report, will be formatted in Microsoft Power Point presentations and include the following:

(a) Title page containing Executive Title, the contract number and title, the period of performance or milestone being reported, the contractor’s name and the date of submission;

(b) Project Progress presented as milestone events, test results, tasks, and other activities achieved during the reporting period as talking point bullets;

3) Final Report: By the expiration date of the contract, the Contractor shall submit a comprehensive Final Report that shall detail, document, and summarize the results of the entire contract work. The report shall explain comprehensively the results achieved. A draft Final Report will be submitted to the Project and Contracting Officers for review and comments, then the Final Report original, four copies, and an electronic file shall be submitted to the Project and Contracting Officers for distribution to the Program office.

4) Updated Integrated Product Development Plan (IPDP)

Within fourteen (14) days of the effective date of the BAA award, the Contractor shall submit an updated IPDP which shall be approved by the Project Officer and the Contracting Officer prior to initiation of any activities related to their implementation.

During the course of contract performance, in response to a need to change the IPDP, the Contractor shall submit a Deviation Report. This report shall request a change in the agreed-upon Plan and timelines. This report shall include:

(a) Discussion of the justification/rationale for the proposed change.

(b) Options for addressing the needed changes from the approved timelines, including a cost-benefit analysis of each option.

(c) Recommendations for the preferred option that includes a full analysis and discussion of the effect of the change on the entire product development program, timelines, and budget.

The Contractor shall carry out activities within the contract Statement of Work only as requested and approved by the Contracting Officer, and may not conduct work on the contract without prior approval from the Contracting Officer, including initiating work that deviates from the agreed-upon IPDP.

5) Updated Gantt Chart

SECTION F—DELIVERIES OR PERFORMANCE

F.1. PERIOD OF PERFORMANCE

The period of performance of this contract is from the date of contract award to twelve (12) months after contract award. Exercise of an option will extend the period of performance by an additional 12 months per contract option.

Delivery will be required F.O.B. Destination as set forth in FAR 52.247-35 F.O.B. DESTINATION WITHIN CONSIGNEE’S PREMISES (APR 1984).

F.2. TECHNICAL REPORT REQUIREMENT

Item	Deliverable	Quantity	Due Date
1.	Technical Monthly Progress Report and Executive Summary	1 Electronic Copy — Project Officer (PO) 1 Electronic Copy — Contracting Officer (CO) 1 Hard Copy - CO	30 days after contract award and by the 15th day of each month during the contract’s period of performance. Not due when Final is due.
2.	Final Report	See above	Due on/before the completion date of the contract.
3.	Quarterly Gantt charts	See above	By the 15th day following the end of each quarterly period.
4.	Quarterly Risk Management Plans	See above	By the 15th day following the end of each quarterly period.

F.3. CONTRACT DELIVERABLES

Item	Deliverable	Quantity	Due Date
1.	Updated Integrated Product Development Plan (IPDP)	1 Electronic Copy — Project Officer (PO) 1 Electronic Copy — Contracting Officer (CO) 1 Hard Copy - CO	14 days after contract award.
2.	FDA audit findings, including final reports, and plans for addressing areas of conformance	1 Electronic Copy — P.O. 1 Electronic Copy — C.O. 1 Hard Copy - CO	Within 30 calendar days of an FDA audit of contractor or subcontractor facilities.

F.4. STOP WORK ORDER

The following clause is incorporated by reference:

FAR 52.242-15 STOP WORK ORDER (AUG 1989) with ALTERNATE I (APR 1984).

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SECTION G—CONTRACT ADMINISTRATION DATA

G.1. CONTRACTING OFFICER

1) The Contracting Officer is the only individual who can legally commit the Government to the expenditure of public funds. No person other than the Contracting Officer can make any changes to the terms, conditions, general provisions, or other stipulations of this contract.

2) The Contracting Officer is the only person with the authority to act as agent of the government under this contract. Only the Contracting Officer has authority to (1) direct or negotiate any changes in the statement of work; (2) modify or extend the period of performance; (3) change the delivery schedule; (4) authorize reimburse to the Contractor of any costs incurred during the performance of this contract; (5) otherwise change any terms and conditions of this contract.

3) No information other than that which may be contained in an authorized modification to this contract, duly issued by the Contracting Officer, which may be received from any person employed by the US Government, other otherwise, shall be considered grounds for deviation from any stipulation of this contract.

G.1. PROJECT OFFICER

The following Project Officers will represent the Government for the purpose of this contract:

[***], Project Officer

[***], Alternate Project Officer

Performance of the work hereunder shall be subject to the technical directions of the designated Project Officers for this contract.

A Government Project Officer is not authorized to change any of the terms and conditions of this contract. Changes shall be made only by the Contracting Officer by properly written modification(s) to the contract. Any changes in Project Officer delegation will be made by the Contracting Officer in writing with a copy being furnished to the Contractor.

G.2. KEY PERSONNEL

Pursuant to the Key Personnel clause incorporated in Section I of this contract, the following individual is considered to be essential to the work being performed hereunder:

[***], Principal Investigator

Prior to diverting any of the specific individuals to other programs, the Contractor shall notify the Contacting officer reasonably in advance and shall submit justification (including proposed substitutions) in sufficient detail to permit evaluation of the impact on the program. No diversion shall be made by the contractor without the written consent of the Contracting Officer; provided that the Contracting Officer may ratify in writing such diversion and such ratification shall constitute the consent of the Contracting Officer. The contract may be modified from time to time during the course of the contract to either add or delete personnel, as appropriate.

G.3. INVOICE/FINANCING REQUEST AND CONTRACT FINANCIAL REPORTING

1) The Contractor shall submit an original and one electronic copy of monthly contract invoices/financial reports to the address shown below:

DHHS/OS/ASPR/BARDA

Attn: Contracting Officer

330 Independence Ave., S.W.

Room G640

Washington, D.C. 20201

2) Contractor invoices/financial reports shall conform to the form, format, and content requirements of the instructions for Invoice/Financing requests and Contract Financial Reporting made a part of the contract in Section J.

3) Monthly invoices must include the cumulative total expenses to date, adjusted (as applicable) to show any amounts suspended by the Government.

4) The contractor agrees to immediately notify the Contracting Officer in writing if there is an anticipated overrun (any amount) or unexpended balance (greater than 10 percent) of the amount allotted to the contract, and the reasons for the variance. Also refer to the requirements of the Limitation of Cost (FAR 52.232-20) clause in the contract.

5) The date of receipt of a proper invoice/voucher by the Contracting Officer shall be used for the purpose of Prompt Payment Act time computations.

G.4. REIMBURSEMENT OF COST (Apr 2000)

1) The Government shall reimburse the Contractor the cost determined by the Contracting Officer to be allowable (hereinafter referred to as allowable cost) in accordance with the clause entitled Allowable Cost and Payment in Section I, Contract Clauses. Examples of allowable costs include, but are not limited to, the following:

a) All direct materials and supplies that are used in the performing of the work provided for under the contract, including those purchased for subcontracts and purchase orders.

b) All direct labor, including supervisory, that is properly chargeable directly to the contract, plus fringe benefits.

c) All other items of cost budgeted for and accepted in the negotiation of this basic contract or modifications thereto.

d) Special expenditures which, upon request from the Contractor, the Contracting Officer approves as being an allowable cost under this contract, such as purchase or lease of office furniture or equipment, etc..

e) All travel costs plus per diem or actual subsistence for personnel while in an actual travel status in direct performance of the work and services required under this contract. These costs will be in accordance with the Contractor’s policy and subject to the following:

(ii) Rail travel shall be by the most direct route, first class with lower berth or nearest equivalent.

(iv) Travel via privately owned automobile shall be reimbursed at not more than the current General Services Administration (GSA) FTR established mileage rate.

2) Except as stated herein and under Section B, Paragraph B.3. PROVISIONS APPLICABLE TO DIRECT COSTS, the Contractor shall not incur costs unless the prior written authorization of the Contracting Officer has been obtained. When costs are incurred without such prior authorization, with the intent of claiming reimbursement as direct costs, it shall be at the contractor’s risk.

G. 5. INDIRECT COST RATES

Director, Division of Financial Advisory Services

Office of Acquisition Management and Policy

National Institutes of Health

6100 Building, Room 6B05

6100 Executive Boulevard, MSC 7540

Bethesda, MD 20892-7540

These rates are hereby incorporated without further action of the Contracting Officer.

G. 6. POST AWARD EVALUATION OF PAST PERFORMANCE

G.7. CONTRACT COMMUNICATIONS/CORRESPONDENCE (JULY 1999)

The Contractor shall identify all correspondence, reports, ad other data pertinent to this contract by imprinting the contract number from Page 1 of the contract.

G.8. GOVERNMENT PROPERTY

1) In addition to the requirements of the clause GOVERNMENT PROPERTY, incorporated in SECTION I of this contract, the Contractor shall comply with the provision of HHS Publication, “Contractor’s Guide for Control of Government Property,” which is incorporated into this contract by reference. This document can be accessed at: httpa://www.knownet.hhs.gov/log/AgncyPolicy/HHSLogPolicy/contractorguide.htm. Among other issues, this publication provides a summary of the Contractor’s responsibilities regarding purchasing authorization and inventory and reporting requirements under the contract. A copy of this publication is available upon request o the Contacts Property Administrator.

2) Notwithstanding the provisions outlined in the HHS Publication, “Contractor’s Guide for control of Government Property,” which is incorporated into this contract in paragraph a. above, the contractor shall use the form entitled “Report of Government Owned, contactor Held Property” for performing annual inventories required udder this contract. This form is included as an attachment in SECTION J of the contract.

SECTION H—SPECIAL CONTRACT REQUIREMENTS

H. 1. HUMAN SUBJECTS

Human Subjects: Research projects involving humans and/or human specimens can only be initiated with written approval by the BARDA Project Officer.

The Good Clinical Practice Regulations (GCP)(21 CFR Parts 50, 54, 56 312)(45 CFR Part 46)(ICH E6) as well as other applicable federal and state regulations will be standards that apply for use of human subject and/or human specimens in clinical studies.

If at any time during the life of the contract, the Contractor fails to comply with GCP as identified by regulations outline above , the Offeror shall have thirty (30) calendar days from the time such material failure is identified to cure such or initiate cure to the satisfaction of the USG Project Officer. If the Offeror fails to take such an action or provide a remediation plan within the thirty (30) calendar day period, then the contract may be terminated.

Research involving human subjects shall not be conducted under this contract until the related protocol has been approved by DHHS and written notice of such approval has been provided by the Contracting Officer. Additionally, prior to conducting the research, the Contractor must provide certification of Institutional Review Board (IRB) review and approval.

H. 2. HUMAN MATERIALS

H.3. PROHIBITION ON THE USE OF APPROPRIATED FUNDS FOR LOBBYING ACTIVITIES AND HHSAR 352.270-10 ANTI-LOBBYING (Jan 2006)

The Contractor is hereby notified of the restrictions on the use of Department of Health and Human Service’s funding for lobbying of Federal, State and Local legislative bodies.

Section 1352 of Title 10, United Stated Code (Public Law 101-121, effective 12/23/89), among other things, prohibits a recipient (and their subcontractors) of a Federal contract, grant, loan, or cooperative agreement from using appropriated funds (other than profits from a federal contract) to pay any person for influencing or attempting to influence an officer or employee of any agency, a Member of Congress, an officer or employee of Congress, or an employee of a Member of Congress in connection with any of the following covered Federal actions; the awarding of any Federal contract; the making of any Federal grant; the making of any Federal loan; the entering into of any cooperative agreement; or the modification of any Federal contract, grant, loan, or cooperative agreement. For additional information of prohibitions against lobbying activities, see FAR Subpart 3.8 and FAR Clause 52.203-12.

In addition, as set forth in HHSAR 352.270-10 “Anti-Lobbying” (January 2006), the current Department of Health and Human Services Appropriations Act provides that no part of any appropriation contained in this Act shall be used, other than for normal and recognized executive-legislative relationships, for publicity or propaganda purposes, for the preparation, distribution, or use of any kit, pamphlet, booklet, publication, radio, television, or video presentation designed to support, or defeat legislation pending before the Congress, or any State or Local legislature except in presentation to the Congress, or any State or Local legislative body itself.

The current Department of Health and Human Services Appropriations Act also provides that no part of any appropriation contained in this Act shall be used to pay the salary or expenses of any contract or grant recipient, or agent acting for such recipient, related to any activity designed to influence legislation or appropriations pending before the Congress, or any State or Local legislature.

(End of Clause)

H.4. PRIVACY ACT APPLICABILITY (Apr 2000)

1) Notification is hereby given that the Contractor and its employees are subject to criminal penalties for violation of the Privacy Act to the same extent as employees of the Government. The Contractor shall assure that each of its employees knows the prescribed rules of conduct and that each is aware that he or she can be subjected to criminal penalty for violation of the Act. A copy of 45 CFR Part 5b, Privacy Act Regulations, may be obtained at

http://www.gpoaccess.gov/cfr/index.html

2) The Project Officer is hereby designated as the official who is responsible for monitoring contractor compliance with the Privacy Act.

3) The Contractor shall follow the Privacy Act guidance as contained in the Privacy Act System of Records number 09-25- 0200. This document may be obtained at the following link: http://oma.od.nih.gov/ms/privacy/pa-files/0200.htm

(End of Clause)

Note: Clinical trials cannot be initiated until the System Notice has been published and the Contracting Officer notifies the contractor.

H.5. LABORATORY LICENSE REQUIREMENTS (May 1998)

(End of Clause)

H.6. DISSEMINATION OF INFORMATION (May 1998)

No information related to data obtained under this contract shall be released or publicized without the prior written consent of the Project Officer.

(End of Clause)

H.7. IDENTIFICATION AND DISPOSITION OF DATA

H.8. INFORMATION ON COMPLIANCE WITH ANIMAL CARE REQUIREMENTS

Registration with the U. S. Dept. of Agriculture (USDA) is required to use regulated species of animals for biomedical purposes. USDA is responsible for the enforcement of the Animal Welfare Act (7 U.S.C. 2131 et. seq.), http://www.nal.usda.gov/awic/legislat/awa.htm.

Subchapter A) http://www.nal.usda.gov/awic/legislat/usdaleg1.htm issued by the U.S. Department of Agriculture (USDA) under the Animal Welfare Act. The Guide may differ from USDA regulations in some respects. Compliance with the USDA regulations is an absolute requirement of this Policy.

H.9. REQUIREMENTS FOR ADEQUATE ASSURANCE OF PROTECTION OF VERTEBRATE ANIMAL SUBJECTS

No PHS supported work for research involving vertebrate animals will be conducted by an organization, unless that organization is operating in accordance with an approved Animal Welfare Assurance and provides verification that the Institutional Animal Care and Use Committee (IACUC) has reviewed and approved the proposed activity in accordance with the PHS policy. Applications may be referred by the PHS back to the institution for further review in the case of apparent or potential violations of the PHS Policy. No award to an individual will be made unless that individual is affiliated with an assured organization that accepts responsibility for compliance with the PHS Policy. Foreign applicant organizations applying for PHS awards for activities involving vertebrate animals are required to comply with PHS Policy or provide evidence that acceptable standards for the humane care and use of animals will be met. Foreign applicant organizations are not required to submit IACUC approval, but should provide information that is satisfactory to the Government to provide assurances for the humane care of such animals.

H.10. APPROVAL OF REQUIRED ASSURANCE BY OLAW

Under governing regulations, federal funds which are administered by the Department of Health and Human Services, Office of Biomedical Advanced Research and Development Authority (BARDA) shall not be expended by the contractor for research involving live vertebrate animals, nor shall live vertebrate animals be involved in research activities by the contractor under this award unless a satisfactory assurance of compliance with 7 U.S.C. 2316 and 9 CFR Sections 2.25-2.28 is submitted within 30 days of the date of this award and approved by the Office of Laboratory Animal Welfare (OLAW). Each performance site (if any) must also assure compliance with 7 U.S.C. 2316 and 9 CFR Sections 2.25-2.28 with the following restriction: Only activities which do not directly involve live vertebrate animals (i.e. are clearly severable and independent from those activities that do involve live vertebrate animals) may be conducted by the contractor or individual performance sites pending OLAW approval of their respective assurance of compliance with 7 U.S.C. 2316 and 9 CFR Sections 2.25-2.28. Additional information regarding OLAW may be obtained via the Internet at http://grants2.nih.gov/grants/olaw/references/phspol.htm

H.11. PROHIBITION ON CONTRACTOR INVOLVEMENT WITH TERRORIST ACTIVITIES

H.12. REGISTRATION WITH THE SELECT AGENT PROGRAM FOR WORK INVOLVING THE POSSESSION, USE, AND/OR TRANSFER OF SELECT BIOLOGICAL AGENTS OR TOXINS

For prime or subcontract awards to foreign institutions who possess, use, and/or transfer Select Agents under this contract, the institution must provide information satisfactory to the Government that a process equivalent to that described in 42 CFR 73 (http://www.cdc.gov/od/sap/docs/42cfr73.pdf ) for U.S. institutions is in place and will be administered on behalf of all Select Agent work sponsored by these funds before using these funds for any work directly involving the Select Agents. The contractor must provide information addressing the following key elements appropriate for the foreign institution: safety, security, training, procedures for ensuring that only approved/appropriate individuals have access to the Select Agents, and any applicable laws, regulations and policies equivalent to 42 CFR 73. The Government will assess the policies and procedures for comparability to the U.S. requirements described in 42 CFR Part 73. When requested by the contracting officer, the contractor shall provide key information delineating any laws, regulations, policies, and procedures applicable to the foreign institution for the safe and secure possession, use, and transfer of Select Agents. This includes summaries of safety, security, and training plans, and applicable laws, regulations, and policies. For the purpose of security risk assessments, the contractor must provide the names of all individuals at the foreign institution who will have access to the Select Agents and procedures for ensuring that only approved and appropriate individuals have access to Select Agents under the contract.

Listings of HHS select agents and toxins, biologic agents and toxins, and overlap agents or toxins as well as information about the registration process, can be obtained on the Select Agent Program Web site at http://www.cdc.gov/od/sap/.

H.13. OPTION PROVISION

Unless the Government exercises its option pursuant to the Option Clause set forth in Section I, Paragraph I.2., the contract will consist only of CLIN 0001 of the Statement of Work as defined in Sections C and F of the contract. Pursuant to clause 52.217-7 set forth in Section I of this contract, under I.3., the Government may, by unilateral contract modification, require the Contractor to perform any of the additional CLIN’s listed in Section B, Paragraph B.2., and as also defined in Sections C and F of this contract. If the Government exercises an option, notice must be given at least 60 days prior to the expiration date of this contract. The amount of the contract will then be increased as set forth in Section B, Paragraph B.2., and the contract’s period of performance will be extended by one year for each option.

H. 14. EPA ENERGY STAR REQUIREMENTS

In compliance with Executive Order 12845 (requiring Agencies to purchase energy efficient computer equipment) all microcomputers, including personal computers, monitors, and printers that are purchased using Government funds in performance of a contract shall be equipped with or meet the energy efficient low-power standby feature as defined by the EPA Energy Star program unless the equipment always meets EPA Energy Star efficiency levels. The microcomputer, as configured with all components, must be Energy Star compliant.

equipment that is fully compatible with the network environment. In addition, the equipment will run commercial off-the-shelf software both before and after recovery from its energy conservation mode.

H. 15. ACKNOWLEDGMENT OF FEDERAL FUNDING

A. Section 507 of P.L. 104-208 mandates that contractors funded with Federal dollars, in whole or in part, acknowledge Federal funding when issuing statements, press releases, requests for proposals, bid solicitations and other documents. Contractors are required to state (1) the percentage and dollar amounts of the total program or project costs financed with Federal money, and (2) the percentage and dollar amount of the total costs financed by nongovernmental sources.

This requirement is in addition to the continuing requirement to provide an acknowledgment of support and disclaimer on any publication reporting the results of a contract funded activity.

B. Publication and Publicity

Publications: Any manuscript or scientific meeting abstract containing data generated under this contract must be submitted for BARDA Project Officer review no less than thirty (30) calendar days for manuscripts and fifteen (15) calendar days for abstracts before submission for public presentation or publication. Contract support shall be acknowledged in all such publications. A “publication” is defined as an issue of printed material offered for distribution or any communication or oral presentation of information.

The Contractor shall acknowledge the support of the Department of Health and Human Service, Office of the Assistant Secretary for Preparedness and Response, Biomedical Advanced Research and Development Authority, whenever publicizing the work under this contract in any media by including an acknowledgment substantially as follows:

C. Press Releases

(a) Pursuant to Section 508 of Public Law 105-78, the contractor shall clearly state, when issuing statements, press releases, requests for proposals, bid solicitations and other documents describing projects or programs funded in whole or in part with Federal money that: (1) the percentage of the total costs of the program or project which will be financed with Federal money; (2) the dollar amount of Federal funds for the project or program; and (3) the percentage and dollar amount of the total costs of the project or program that will be financed by nongovernmental sources.

(b) The Contractor agrees to accurately and factually represent the work conducted under this contract in all press releases. Misrepresenting contract results or releasing information that is injurious to the integrity of BARDA may be construed as improper conduct. Press releases shall be considered to include the public release of information to any medium, excluding peer-reviewed scientific publications. The contractor shall ensure that the Project Officer has received an advance copy of any press release related to this contract not less than four (4) working days prior to the issuance of the press release.

H. 16. REPORTING MATTERS INVOLVING FRAUD, WASTE AND ABUSE

Anyone who becomes aware of the existence or apparent existence of fraud, waste and abuse in DHHS funded programs is encouraged to report such matters to the HHS Inspector General’s Office in writing or on the Inspector General’s Hotline. The toll-free number is 1-800-HHS-TIPS (1-800-447-8477). All telephone calls will be handled confidentially. The e-mail address is Htips@os.dhhs.gov.

Office of Inspector General

Department of Health and Human Services

TIPS HOTLINE

P.O. Box 23489

Washington, DC 20026

PART II — CONTRACT CLAUSES

SECTION I - CONTRACT CLAUSES

I.1. FAR 52.252-2, CLAUSES INCORPORATED BY REFERENCE (FEBRUARY 1998)

A. General Clauses for Cost-Reimbursement Research and Development General Clauses

(1) FEDERAL ACQUISITION REGULATION (FAR) (48 CFR CHAPTER 1) CLAUSES:

FAR CLAUSE NO.	DATE	TITLE
52.202-1	Jul 2004	Definitions
52.203-3	Apr 1984	Gratuities (Over $100,000)
52.203-5	Apr 1984	Covenant Against Contingent Fees (Over $100,000)
52.203-6	Sep 2006	Restrictions on Subcontractor Sales to the Government (Over $100,000)
52.203-7	Jul 1995	Anti-Kickback Procedures (Over $100,000)
52.203-8	Jan 1997	Cancellation, Rescission, and Recovery of Funds for Illegal or Improper Activity (Over $100,000)
52.203-10	Jan 1997	Price or Fee Adjustment for Illegal or Improper Activity (Over $100,000)
52.203-12	Sep 2007	Limitation on Payments to Influence Certain Federal Transactions (Over $100,000)
52.203-13	Dec 2008	Contractor Code of Business Ethics and Conduct (over $5,000,000)
52.203-14	Dec 2007	Display of Hotline Poster
52.204-4	Aug 2000	Printed or Copied Double-Sided on Recycled Paper (Over $100,000)
52.204-7	Apr 2008	Central Contractor Registration
52.209-6	Sep 2006	Protecting the Government’s Interests When Subcontracting With Contractors Debarred, Suspended, or Proposed for Debarment (Over $25,000)
52.215-2	Mar 2009	Audit and Records - Negotiation (Over $100,000)
52.215-8	Oct 1997	Order of Precedence - Uniform Contract Format
52.215-10	Oct 1997	Price Reduction for Defective Cost or Pricing Data
52.215-12	Oct 1997	Subcontractor Cost or Pricing Data (Over $500,000)
52.215-14	Oct 1997	Integrity of Unit Prices (Over $100,000)
52.215-15	Oct 2004	Pension Adjustments and Asset Reversions
52.215-17	Oct 1997	Waiver of Facilities Capital Cost of Money
52.215-18	Jul 2005	Reversion or Adjustment of Plans for Post-Retirement Benefits (PRB) other than Pensions

52.215-19	Oct 1997	Notification of Ownership Changes
52.215-21	Oct 1997	Requirements for Cost or Pricing Data or Information Other Than Cost or Pricing Data — Modifications
52.216-7	Dec 2002	Allowable Cost and Payment (Note: the following language is included in this clause — “(3) The designated payment office will make interim payments for contract financing on the 30th day after the designated billing office receives a proper payment request…”
52.216-8	Mar 1997	Fixed Fee
52.217-7	March 1989	Option for Increased Quantity - Separately Priced Line Item (Note: the following language is included in this clause — “....The Contracting Officer may exercise the option by written notice to the Contractor within 60 days prior to the expiration of this contract ....”)
52.219-8	May 2004	Utilization of Small Business Concerns (Over $100,000)
52.219-9	Apr 2008	Small Business Subcontracting Plan (Over $500,000)
52.219-16	Jan 1999	Liquidated Damages - Subcontracting Plan (Over $500,000)
52.222-2	Jul 1990	Payment for Overtime Premium (Over $100,000) (Note: The dollar amount in paragraph (a) of this clause is $0 unless otherwise specified in the contract.)
52.222-19	Aug 2009	Child Labor — Cooperation with Authorities and Remedies
52.222-3	Jun 2003	Convict Labor
52.222-21	Feb 1999	Prohibition of Segregated Facilities
52.222-26	Mar 2007	Equal Opportunity
52.222-35	Sep 2006	Equal Opportunity for Special Disabled Veterans, Veterans of the Vietnam Era, and Other Eligible Veterans
52.222-36	Jun 1998	Affirmative Action for Workers with Disabilities
52.222-37	Sep 2006	Employment Reports on Special Disabled Veterans, Veterans of the Vietnam Era, and Other Eligible Veterans
52.222-39	Dec 2004	Notification of Employee Rights Concerning Payment of Union Dues or Fees
52.222-50	Feb 2009	Combating Trafficking in Persons
52.222-54	Jan 2009	Employment Eligibility Verification
52.223-6	May 2001	Drug-Free Workplace
52.223-14	Aug 2003	Toxic Chemical Release Reporting (Over $100,000)
52.224-1	April 1984	Privacy Act Notification
52.224-2	April 1984	Privacy Act
52.225-1	Feb 2009	Buy American Act - Supplies
52.225-13	Jun 2008	Restrictions on Certain Foreign Purchases
52.227-1	Dec 2007	Authorization and Consent, Alternate I (Apr 1984)

52.227-2	Dec 2007	Notice and Assistance Regarding Patent and Copyright Infringement (Over $100,000)
52.227-11	Dec 2007	Patent Rights - Retention by the Contractor (Short Form) (Note: In accordance with FAR 27.303(a)(2), paragraph (f) is modified to include the requirements in FAR 27.303(a)(2)(i) through (iv). The frequency of reporting in (i) is annual.
52.227-14	Dec 2007	Rights in Data — General
52.229-8	March 1990	Foreign Cost-Reimbursement Contracts
52.230-4	Oct 2008	Disclosure and Consistency of Cost Accounting Practices for Contracts Awarded to Foreign Concerns
52.232-9	Apr 1984	Limitation on Withholding of Payments
52.232-17	Oct 2008	Interest (Over $100,000)
52.232-20	Apr 1984	Limitation of Cost
52.232-23	Jan 1986	Assignment of Claims
52.232-25	Oct 2008	Prompt Payment, Alternate I (Feb 2002)
52.232-33	Oct 2003	Payment by Electronic Funds Transfer—Central Contractor Registration
52.233-1	Jul 2002	Disputes
52.233-3	Aug 1996	Protest After Award, Alternate I (Jun 1985)
52.233-4	Oct 2004	Applicable Law for Breach of Contract Claim
52.242-1	Apr 1984	Notice of Intent to Disallow Costs
52.242-3	May 2001	Penalties for Unallowable Costs (Over $500,000)
52.242-4	Jan 1997	Certification of Final Indirect Costs
52.242-13	Jul 1995	Bankruptcy (Over $100,000)
52.243-2	Aug 1987	Changes - Cost Reimbursement, Alternate V (Apr 1984)
52.244-2	Jun 2007	Subcontracts, Alternate II (Aug 1998) *If written consent to subcontract is required, the identified subcontracts are listed in Section B, Paragraph B.4., Advance Understandings.
52.244-5	Dec 1996	Competition in Subcontracting (Over $100,000)
52.244-6	Feb 2009	Subcontracts for Commercial Items
52.245-1	June 2007	Government Property
52.245-9	Jun 2007	Use and Charges
52.246-23	Feb 1997	Limitation of Liability (Over $100,000)
52.249-6	May 2004	Termination (Cost-Reimbursement)
52.253-1	Jan 1991	Computer Generated Forms

(2) DEPARTMENT OF HEALTH AND HUMAN SERVICES ACQUISITION REGULATION (HHSAR) (48 CFR CHAPTER 3) CLAUSES:

HHSAR CLAUSE NO.	DATE	TITLE
352.202-1	Jan 2006	Definitions - with Alternate paragraph (h) (Jan 2001)
352.216-72	Jan 2006	Additional Cost Principles
352.223-70	Jan 2006	Safety and Health
352.224-70	Jan 2006	Confidentiality of Information (Note: The following information is covered by this clause- Data obtained from human subjects)
352.228-7	Dec 1991	Insurance - Liability to Third Persons
352.232-9	Jan 2006	Withholding of Contract Payments
352.233-70	Jan 2006	Litigation and Claims
352.242-71	Apr 1984	Final Decisions on Audit Findings
352.249-14	Jan 2006	Excusable Delays
352.270-5	Jan 2006	Key Personnel
352.270-6	Jan 2006	Publications and Publicity
352.270-7	Jan 2006	Paperwork Reduction Act
352.270-9	Jan 2006	Care of Live Vertebrate Animals
352.270-10	Jan 2006	Anti-Lobbying
352.333-7001	Undated	Choice of Law (Overseas)

[End of GENERAL CLAUSES FOR A COST-REIMBURSEMENT RESEARCH AND DEVELOPMENT CONTRACT].

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

NO. 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers is extended, is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (If required) APPROPRIATION: 75-1011-0140; CAN: 1990087; OBJECT CLASS: 25329; ; AMOUNT: $[***] 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. ORDER NO. IN ITEM 10A. E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible) PURPOSES: (1) To modify the dollar amounts for Options #1and #2; (2) to exercise Option #1 based upon the revised dollar amount; (3) to move several milestones in the Statement of Work to different project years; and (4) to add indirect rates that apply specifically to this contract. No other terms or conditions are changed by this modification Funds Obligated: Total Base Contract Dollar Amount: Contract Expiration Date: $[***] $[***] (changed) November 15, 2011(changed) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. (Signature of Contracting Officer) NSN 7540-01-152-8070 OMB No. 0990–0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 123269097 v2 15A. NAME AND TITLE OF SIGNER (Type or print) [***] [***] 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED 17/9/10 16B. UNITED STATES OF AMERICA BY /s/ [***] 16C. DATE SIGNED September 23, 2010 () A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1 and mutual agreement of the parties D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 3 2. AMENDMENT/MODIFICATION NO 1 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) N/A 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (X) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) x 10A. MODIFICATION OF CONTRACT/ORDER HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

SPECIAL PROVISIONS

Contract No: HHSO100201000011C
Modification No: 1

The basic contract award is hereby modified as follows:

1. Contract Option #1 is hereby exercised, but at a reduced amount. The revised Option #1 amount is shown below. This information replaces CLIN 0002, which is set forth under Section B. Supplies or Services and Prices/Costs, A. CONTRACT LINE ITEM NUMBER (CLIN’S), 2. Contract Options.

CLIN’s

DESCRIPTION

EST. COST

FIXED FEE

TOTAL
EST. CPFF

0002

[***]

2. The dollar of Option #2 is increased to offset the reduction to Option #1. The revised Option #2 amount is shown below. This information replaces CLIN 0003, which is set forth under Section B. Supplies or Services and Prices/Costs, A. CONTRACT LINE ITEM NUMBER (CLIN’S), 2. Contract Options.

0003

[***]

3. Under Section C, Description/Specifications, C.1. STATEMENT OF WORK is revised to move several milestones to different project years. Specifically the following Base Contract milestones are moved: [***]

4. The contract’s expiration date is extended by twelve months due to the exercise of Option #1, as set forth in Section F. Deliveries or Performance, under F.1. Period of Performance. The revised expiration date is November 15, 2011.

5. [***]

(a) [***]:

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A NO. 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers is extended, is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) N/A 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. CONTRACT ORDER NO. IN ITEM 10A. office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). E. IMPORTANT: Contractor [X] is not, [ ] is required to sign this document and return copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible) PURPOSE: This modification revises the accounting data that was listed in Modification #1 under Block #12 to read as follows: Appropriation – 7509/100140 Appropriation – 7510/110140 CAN - 1990987 Amount - $[***] CAN - 1990987 Amount - $[***] All other terms and conditions of the contract are unchanged and remain in full force and effect. Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990–0115 STANDARD FORM 30 (REV. 10-83) FAR (48 CFR) 53.243 123269097 v2 15A. NAME AND TITLE OF SIGNER (Type or print) 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR (Signature of person authorized to sign) 15C. DATE SIGNED 16B. UNITED STATES OF AMERICA BY /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 9/30/2010 () A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 1 2. AMENDMENT/MODIFICATION NO 002 3. EFFECTIVE DATE See Block 16C. 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/OS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (x) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) x 10A. MODIFICATION OF CONTRACT/ORDER HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE FACILITY CODE

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A NO. 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) N/A 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ] is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) PURPOSES: [***] No other terms or conditions are changed by this modification. See continuation sheet. Funds Obligated: $0 Total Base Contract Dollar Amount: $[***] Contract Expiration Date: November 15, 2011 (unchanged) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990–0115 STANDARD FORM 30 (REV. 10-83)FAR (48 CFR) 53.243 123269097 v2 15A. NAME AND TITLE OF SIGNER (Type or print) [***], EVP 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED 8 April 2011 16B. UNITED STATES OF AMERICA BY/s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED April 8, 2011 (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). Y C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 5 2. AMENDMENT/MODIFICATION NO 3 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/ASPR/AMCG 330 Independence Avenue, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (x) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) x 10A. MODIFICATION OF CONTRACT/ORDER HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: FACILITY CODE:

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Continuation Sheet

Contract No: HHSO100201000011C
Modification No: 3

Modification No. 003 (the “Mod 3”) to Contract No. HHS0100201000011C, as amended to the date of Mod 3, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The basic contract award is revised as follows:

1. As a result of revisions to the Statement of Work, the dollar amounts for optional CLIN’s 0003, 0004, 0005, and 0006 are modified. Section B. Supplies or Services and Prices/Costs, A. CONTRACT LINE ITEM NUMBER (CLIN’S), 2. Contract Options are therefore modified as shown below:

CLIN’s	DESCRIPTION	EST. COST		FIXED FEE		TOTAL EST. CPFF
0003	[***]	$	[***]	$	[***]	$	[***]
0004	[***]	$	[***]	$	[***]	$	[***]
0005	[***]	$	[***]	$	[***]	$	[***]
0006	[***]	$	[***]	$	[***]	$	[***]

All funding above the funds previously awarded are at a fee of [***]%.

2. Section B.4 Advanced Understandings, are revised as shown below:

3) [***]

[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

[***]

4) Protocols

The Contractor shall distribute draft study plans and protocols for USG review prior to the conduct of a Study Design Review Meeting between the USG and the contractor as part of the preapproval process as described in paragraph B.3.

5) Access to Documentation and Interaction with Regulatory Agencies

The contractor shall provide the USG with a non-redacted copy of any FDA Form-482, Form FDA-483, and Establishment Inspection Report (EIR) within 24 hours of receipt. The contractor shall include the USG in all scheduled meetings and teleconferences with regulatory agencies.

3. Under Section C, Description/Specifications, within C.1. STATEMENT OF WORK, the work statement is completely revised to incorporate changes and update the milestones. As a result, C.1. paragraphs A. and B. are revised as follows:

A. Independently, and not as an agent of the USG, the Contractor shall furnish all the necessary services, qualified personnel, materials, supplies, equipment, facilities, transportation and travel not otherwise provided by the USG as required to perform a revised Statement of Work and Contractor Defined Milestones, as set forth in Attachment #2, which is incorporated into this contract modification.

B. CONTRACT OPTIONS

The Government may exercise any of the three remaining options for the continuation of requirements as set forth in the following Contractor Defined Milestones. Exercise of each option also extends the contract’s period of performance by twelve months. Option periods may be subject to renegotiation by the Parties depending on the current state of the art at the time of option exercise. Additionally, Option #5 as stated below may be exercised at any time during Contract Performance.

SECTION C-DESCRIPTION/SPECIFICATIONS
C.1. Revised Statement of Work
A.

Description exercised Base and Option #1		SOW Section Number
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

B. CONTRACT OPTIONS

Description Option #2		SOW Section Number
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]

Description Option #3		SOW Section Number
[***]		[***]
[***]		[***]
[***]		[***]
[***]		[***]

Description Option #4		SOW Section Number
[***]		[***]

Description Option #5		SOW Section Number
[***]		[***]

4. The Contracting Officer designation in Section D, Packaging, Marking and Shipping, under the heading “Report Deliverables” is revised as follows:

[***]

5. Under Section G - Contract Administration Data, G.1. Project Officer, the Alternate Project Officer, [***] designation is revoked and replaced with [***] as noted below. All references to “Project Officer” are revised to read “Contracting Officer Technical Representative.”

[***]

[***]
[***] Office

6. [***]

[***]
[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A NO. 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS ~ The above numbered solicitation is amended as set forth in Item 14. The hour and date specified for receipt of Offers ~ is extended, ~ is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended, by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers. FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment, your desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 12. ACCOUNTING AND APPROPRIATION DATA (if required) Requisition # OS72587, Appr. Yr. 2011, CAN 1992002, Object Class 265329 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO. AS DESCRIBED IN ITEM 14. FAR 17.207, FAR 1.602-1 and mutual agreement of the parties E. IMPORTANT: Contractor [ ]is not, [X] is required to sign this document and return 2 copies to the issuing office. 14. DESCRIPTION OF MODIFICATION PURPOSES: To exercise Option Period 2 Option Period 2 is exercised herewith based on the revised Period of Performance beginning September 16, 2011, and ending November 15, 2012, for the contract amount of $[***] No other terms or conditions are changed by this modification. Funds Obligated: $[***] Total Contract Dollar Amount: $[***] Contract Expiration Date: November 15, 2012 Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. NSN 7540-01-152-8070 OMB No. 0990–0115 STANDARD FORM 30 (REV. 10-83)FAR (48 CFR) 53.243 123269097 v2 15A. NAME AND TITLE OF SIGNER (Type or print) [***], EXECUTIVE VICE PRESIDENT 16A. NAME AND TITLE OF CONTRACTING OFFICER (Type or print) [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED 12 Sep 011 16B. UNITED STATES OF AMERICA BY /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 16 Sep 2011 (Y) A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). Y C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE PAGE OF PAGES 1 1 2. AMENDMENT/MODIFICATION NO 4 3. EFFECTIVE DATE See Block 16C 4. REQUISITION/PURC N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE 7. ADMINISTERED BY (If other than Item 6)CODE HHS/ASPR/AMCG 330 Independence Ave, SW Room G640 Washington, DC 20201 8. NAME AND ADDRESS OF CONTRACTOR (No., street, county, State and ZIP Code) Bavarian Nordic A/S Hejreskovvej 10A 3490 Kvistgård Denmark (x) 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) x 10A. MODIFICATION OF CONTRACT/ORDER HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: FACILITY CODE:

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A ADMINISTERED BY (IF OTHER THAN ITEM 6)CODE The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers, FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. NSN 7540-01-152-8070 Previous Edition Unusable STANDARD FORM 30 (REV. 10-83) Prescribed by GSA FAR (48 CFR) 53.243 123269097 v2 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO., AS DESCRIBED IN ITEM 14 A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify Authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1, FAR Mutual Agreement of the Parties D.OTHER (Specify type of modification and authority) E. IMPORTANT: Contractoris Notis required to sign this document and return 1 Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible. The purpose of this modification is to (1) to provide a three (3) year no cost extension to the period of performance from November 15, 2012 to November 15, 2015 and (2) transfer monies from CLIN 2 to CLIN 3. The cost to complete remains unchanged. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER [***], EVP 16A. NAME AND TITLE OF CONTRACTING OFFICER [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED 7 Nov 2012 16B. UNITED STATES OF AMERICA /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 9 Nov 2012 AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 005 3. EFFECTIVE DATE See Item 16C 4. REQUISITION/PURCHASE REQ. NO. N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE N/A 7. See N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 Washington, D.C. 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., Street, County, State and Zip Code) Bavarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100201000011C
Modification No: 005		(continuation sheet)

Continuation Sheet

Contract No: HHSO100201000011C
Modification No: 5

Modification No. 005 (the “Mod 5”) to Contract No. HHSO100201000011C, as amended to the date of Mod 5, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The base contract award is revised as follows:

1. The contract’s expiration date is extended by three (3) years for a no cost extension. The revised expiration date for Section F. Deliverables and Performance, F.1. Period of Performance shall be November 15, 2015.

2. The dollar amounts for the CLIN’s 0002 and 0003 are modified. Section B. Supplies or Services and Prices/Costs, A. CONTRACT LINE ITEM NUMBER (CLIN’S), 2. Contract Options are therefore modified as shown below:

CLIN’s

DESCRIPTION

EST.COST

FIXED FEE

TOTAL
EST. CPFF

0002

[***]

0003

[***]

[End of Modification No. 5 and the remainder of this page intentionally left blank]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A ADMINISTERED BY (IF OTHER THAN ITEM 6)CODE The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers, FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. NSN 7540-01-152-8070 Previous Edition Unusable STANDARD FORM 30 (REV. 10-83) Prescribed by GSA FAR (48 CFR) 53.243 123269097 v2 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO., AS DESCRIBED IN ITEM 14 A THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify Authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: FAR 1.602-1, FAR Mutual Agreement of the Parties D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractoris NOTis required to sign this document and return1Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible. The purpose of this modification is to (1) To incorporate a revised Statement of Work and milestones. No other terms or conditions are change by this modification. See continuation sheet. The cost to complete remains unchanged. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER [***], Executive Vice President 16A. NAME AND TITLE OF CONTRACTING OFFICER [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED 2 May 2013 16B. UNITED STATES OF AMERICA /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 5 May 2013 AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE N/A Page 1 of 3 2. AMENDMENT/MODIFICATION NO. Modification 006 3. EFFECTIVE DATE See Item 16C 4. REQUISITION/PURCHASE REQ. NO. N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE N/A 7. See N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 Washington, D.C. 20201 Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., Street, County, State and Zip Code) Bavarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100201000011C
Modification No: 006		(continuation sheet)

Continuation Sheet

Contract No: HHSO100201000011C
Modification No: 6

Modification No. 006 (the “Mod_6”) to Contract No. HHSO100201000011C, as amended to the date of Mod-6, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof.

The base contract award is revised as follows:

1. As a result of revisions to the Statement of Work, the dollar amount for optional CLIN’s 0003, 0004, and 0005 are modified. Section B. Supplies or Services and Prices/Cost. A. CONTRACT LINE ITEM NUMEBR (CLINS), 2. Contract Options are therefore modified as shown below.

CLIN’s	DESCRIPTION	EST. COST		FIXED FEE		TOTAL EST. CPFF
0001	[***]	$	[***]	$	[***]	$	[***]
0002	[***]	$	[***]	$	[***]	$	[***]
0003	[***]	$	[***]	$	[***]	$	[***]
0004	[***]	$	[***]	$	[***]	$	[***]
0005	[***]	$	[***]	$	[***]	$	[***]

2. Under Section C, Description/Specification within C.1. STATEMENT OF WORK, the work statement is completely revised to incorporate changes and update the milestones. The full written copy of the Statement of Work is included as Attachment I to this Modification.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

REVISED - NEW MOD as April 2013

SECTION C - DESCRIPTION/SPECIFICATIONS

C.1. Revised Statement of Work

A.		CONTRACT BASE

Description exercised Base		SOW Section Number
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*

B.		CONTRACT OPTIONS

Description Option #1		SOW Section Number
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*

Description Option #2		SOW Section Number
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*
[]*		[]*

Description Option #3		SOW Section Number
[]*		[]*
[]*		[]*

Description Option #4		SOW Section Number
[]*		[]*

[End of Modification No. 6 and the remainder of this page intentionally left blank]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A N/A The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers, FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. 123269097 v2 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO., AS DESCRIBED IN ITEM 14 A.THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify Authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B.THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C.THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D.OTHER (Specify type of modification and authority) E. IMPORTANT: Contractoris NOTis required to sign this document and return1Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible. The purpose of this modification is to (1) To update Section D – Packaging, Marking, and Shipping and (2) to remove the requirement for one hard copy of the monthly technical progress report and executive summary in Clause F2. Technical Report Requirement. No other terms or conditions are change by this modification. See continuation sheet. The cost to complete remains unchanged. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER 16A. NAME AND TITLE OF CONTRACTING OFFICER [***], Contracting Officer 15B. CONTRACTOR/OFFEROR (Signature of person authorized to sign) 15C. DATE SIGNED 16B. UNITED STATES OF AMERICA /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 9/24/13 AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 007 3. EFFECTIVE DATE See Item 16C 4. REQUISITION/PURCHASE REQ. NO. N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE N/A 7. ADMINISTERED BY (IF OTHER THAN ITEM 6) CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 WASHINGTON, D.C. 20201 See Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., Street, County, State and Zip Code) Bavarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS NSN 7540-01-152-8070 Previous Edition Unusable STANDARD FORM 30 (REV. 10-83) Prescribed by GSA FAR (48 CFR) 53.243 123269097 v2

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100201000011C
Modification No: 007		(continuation sheet)

Continuation Sheet

Contract No: HHSO100201000011C
Modification No: 7

Modification No. 007 (the “Mod _7”) to Contract No. HHSO100201000011C, as amended to the date of Mod-7, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The base contract award is revised as follows:

SECTION D—PACKAGING, MARKING AND SHIPPING

Report Deliverables

Unless otherwise specified by the Contracting Officer or the Contracting Officer’s representative, delivery of reports to be furnished to the Government under this contract (including invoices), shall be addressed as follows:

[***]

F.2. TECHNICAL REPORT REQUIREMENT

Item		Deliverable		Quantity		Due Date
1.		Technical Monthly Progress Report and Executive Summary		1 Electronic Copy — Project Officer (PO) 1 Electronic Copy — Contracting Officer (CO)		30 days after contract award and by the 15th day of each month during the contract’s period of performance. Not due when Final is due.

[End of Modification No. 7 and the remainder of this page intentionally left blank]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A N/A The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers, FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. NSN 7540-01-152-8070 Previous Edition Unusable 123269097 v2 STANDARD FORM 30 (REV. 10-83) Prescribed by GSA FAR (48 CFR) 53.243 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN: 1992003Appropriation: 2014.1992003.25106Obligation: $[***] 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO., AS DESCRIBED IN ITEM 14 A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify Authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: 17.207, FAR 1.602-1 and mutual agreement of the parties D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractoris NOTis required to sign this document and return1Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible. The purpose of this modification is to (1) to modify dollar amounts for Option 4 (CLIN 5), (2) to incorporate a SOW and milestones for this option (3) exercise Option# 4 (CLIN 5) based on the revised dollar amount. Please note, BARDA must review and approve all protocols prior to study initiation. No other terms or conditions are change by this modification. See continuation sheet. Funds Obligated: $[***] (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER [***] Executive Vice President 16A. NAME AND TITLE OF CONTRACTING OFFICER [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED 17, April 2014 16B. UNITED STATES OF AMERICA /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 4/17/14 AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE Page 1 of 21 2. AMENDMENT/MODIFICATION NO. Modification 008 3. EFFECTIVE DATE See Item 16C 4. REQUISITION/PURCHASE REQ. NO. OS130852 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE N/A 7. ADMINISTERED BY (IF OTHER THAN ITEM 6) CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 WASHINGTON, D.C. 20201 See Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., Street, County, State and Zip Code) Bavarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100201000011C
Modification No: 008		(continuation sheet)

Continuation Sheet

Contract No: HHSO100201000011C
Modification No: 8

Modification No. 008 (the “Mod _8”) to Contract No. HHSO100201000011C, as amended to the date of Mod-8, (the “Existing Contract”) entered into and made effective as of the date imprinted in Block 16C of the Standard Form 30, is by and between the United States of America—which is represented by the Department of Health and Human Services, Biomedical Advanced Research and Development Authority—and Bavarian Nordic (“BN”), a company registered in Denmark, with a principal place of business located at Hejreskovvej 10 A, 3490, Kvistgard, Denmark, (USG and BN each being referred to as a “Party” and collectively as the “Parties”) who jointly agree to be bound by the terms and conditions hereof,

The base contract award is revised as follows:

1. As a result of revisions to the Statement of Work, the dollar amount for optional CLIN 0005 is modified. Section B. Supplies or Services and Prices/Cost, A. CONTRACT LINE ITEM NUMEBR (CLINS), 2. Contract Option is therefore modified as shown below.

CLIN’s

DESCRIPTION

EST. COST

FIXED FEE

TOTAL
EST. CPFF

0005

[***]

2. Under Section C. Description/Specification within C.1. STATEMENT OF WORK, the work statement is revised to include a SOW for this option and milestone activities have been added. The full written copy of the Statement of Work for Option #4 is included as Attachment 1 to this Modification. Below is the updated milestones

Activity	Milestone	Completion Date
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]
[***]	[***]	[***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A N/A The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers, FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. NSN 7540-01-152-8070 Previous Edition Unusable STANDARD FORM 30 (REV. 10-83) Prescribed by GSA FAR (48 CFR) 53.243 123269097 v2 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO., AS DESCRIBED IN ITEM 14 A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify Authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractoris NOTis required to sign this document and return1Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible. The purpose of this modification is to (1) To update clause G.2. – Key Personnel. No other terms or conditions are change by this modification. See continuation sheet. The cost to complete remains unchanged. (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER 16A. NAME AND TITLE OF CONTRACTING OFFICER [***], Contracting Officer 15B. CONTRACTOR/OFFEROR (Signature of person authorized to sign) 15C. DATE SIGNED 16B. UNITED STATES OF AMERICA /s/ [***] (Signature of Contracting Officer) 16C. DATE SIGNED 4 Nov 2014 AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 009 3. EFFECTIVE DATE See Item 16C 4. REQUISITION/PURCHASE REQ. NO. N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE N/A 7. ADMINISTERED BY (IF OTHER THAN ITEM 6) CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 WASHINGTON, D.C. 20201 See Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., Street, County, State and Zip Code) Bavarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9A. AMENDMENT OF SOLICITATION NO. 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

N/A N/A The above numbered solicitation is amended as set forth in item 14. The hour and date specified for receipt of Offers is extended is not extended. Offers must acknowledge receipt of this amendment prior to the hour and date specified in the solicitation or as amended by one of the following methods: (a) By completing Items 8 and 15, and returning copies of the amendment; (b) By acknowledging receipt of this amendment on each copy of the offer submitted; or (c) By separate letter or telegram which includes a reference to the solicitation and amendment numbers, FAILURE OF YOUR ACKNOWLEDGMENT TO BE RECEIVED AT THE PLACE DESIGNATED FOR THE RECEIPT OF OFFERS PRIOR TO THE HOUR AND DATE SPECIFIED MAY RESULT IN REJECTION OF YOUR OFFER. If by virtue of this amendment you desire to change an offer already submitted, such change may be made by telegram or letter, provided each telegram or letter makes reference to the solicitation and this amendment, and is received prior to the opening hour and date specified. (Signature of Contracting Officer) NSN 7540-01-152-8070 123269097 v2 STANDARD FORM 30 (REV. 10-83) 12. ACCOUNTING AND APPROPRIATION DATA (If Required) EIN:CAN:Appropriation:O.C.Obligation: 13. THIS ITEM APPLIES ONLY TO MODIFICATIONS OF CONTRACTS/ORDERS, IT MODIFIES THE CONTRACT/ORDER NO., AS DESCRIBED IN ITEM 14 A. THIS CHANGE ORDER IS ISSUED PURSUANT TO: (Specify Authority) THE CHANGES SET FORTH IN ITEM 14 ARE MADE IN THE CONTRACT ORDER NO. IN ITEM 10A. B. THE ABOVE NUMBERED CONTRACT/ORDER IS MODIFIED TO REFLECT THE ADMINISTRATIVE CHANGES (such as changes in paying office, appropriation date, etc.) SET FORTH IN ITEM 14, PURSUANT TO THE AUTHORITY OF FAR 43.103(b). C. THIS SUPPLEMENTAL AGREEMENT IS ENTERED INTO PURSUANT TO AUTHORITY OF: D. OTHER (Specify type of modification and authority) E. IMPORTANT: Contractoris NOTis required to sign this document and return1Copy to the issuing office. 14. DESCRIPTION OF AMENDMENT/MODIFICATION (Organized by UCF section headings, including solicitation/contract subject matter where feasible.) The purpose of this modification is to (1) to provide a one (1) year no cost extension to the period of performance from November 15, 2015 to November 15, 2016 and (2) update G.3. Invoice/Financing Request and Contract Financial Reporting. No other terms or conditions are change by this modification. See continuation sheet. The cost to complete remains unchanged. Contract Expiration Date: November 15, 2016 (See continuation Sheet) Except as provided herein, all terms and conditions of the document referenced in Item 9A or 10A, as heretofore changed, remains unchanged and in full force and effect. 15A. NAME AND TITLE OF SIGNER[***] [***], Director of Finance 16A. NAME AND TITLE OF CONTRACTING OFFICER [***], Contracting Officer 15B. CONTRACTOR/OFFEROR /s/ [***] (Signature of person authorized to sign) 15C. DATE SIGNED Mar-19-2015 16B. UNITED STATES OF AMERICA /s/ [***] 16C. DATE SIGNED AMENDMENT OF SOLICITATION/MODIFICATION OF CONTRACT 1. CONTRACT ID CODE Page 1 of 2 2. AMENDMENT/MODIFICATION NO. Modification 010 3. EFFECTIVE DATE See Item 16C 4. REQUISITION/PURCHASE REQ. NO. N/A 5. PROJECT NO. (If applicable) 6. ISSUED BYCODE N/A 7. ADMINISTERED BY (IF OTHER THAN ITEM 6) CODE N/A U.S. DEPT OF HEALTH & HUMAN SERVICES ASPR/BARDA 330 INDEPENDENCE AVE SW, ROOM G640 WASHINGTON, D.C. 20201 See Item 6 8. NAME AND ADDRESS OF CONTRACTOR (No., Street, County, State and Zip Code) 9A. AMENDMENT OF SOLICITATION NO. Bavarian Nordic A/S Hejreskovvej 10A DK-3490 Kvistgard Denmark 9B. DATED (SEE ITEM 11) 10A. MODIFICATION OF CONTRACT/ORDER NO. HHSO100201000011C 10B. DATED (SEE ITEM 13) November 16, 2009 CODE: N/A FACILITY CODE: N/A 11. THIS ITEM ONLY APPLIES TO AMENDMENTS OF SOLICITATIONS Previous Edition Unusable Prescribed by GSA FAR (48 CFR) 53.243 123269097 v2

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Contract Number HHSO100201000011C
Modification No: 009		(continuation sheet)

Continuation Sheet

Contract No: HHSO100201000011C
Modification No: 10

The base contract award is revised as follows:

G.3. INVOICE/FINANCING REQUEST AND CONTRACT FINANCIAL REPORTING

1) Documents should be delivered electronically to the Contracting Officer (CO), the Contracting Officer’s Representative (COR) and PSC electronically. Unless otherwise specified by the Contracting Officer all deliverables and reports furnished to the Government under the resultant contract (including invoices) shall be addressed as follows:

[***]	[***]	Email invoices to:
[***]	[***]
[***]	[***]	[***]
[***]	[***]
[***]	[***]
[***]	[***]
[***]	[***]

3) Monthly invoices must include the cumulative total expenses to date, adjusted (as applicable) to show any amounts suspended by the Government.

5) The date of receipt of a proper invoice/voucher by the Contracting Officer shall be used for the purpose of Prompt
Payment Act time computations.

[End of Modification No. 10 and the remainder of this page intentionally left blank]

TABLE OF CONTENTS

ARTICLE 1 DEFINITIONS	2

ARTICLE 2 COLLABORATION OVERVIEW	14

ARTICLE 3 GOVERNANCE	15

ARTICLE 4 DEVELOPMENT	18

ARTICLE 5 REGULATORY AFFAIRS	22

ARTICLE 6 COMMERCIALIZATION	23

ARTICLE 7 MANUFACTURING	25

ARTICLE 8 REPORTS AND ACCESS TO KNOW-HOW	26

ARTICLE 9 GRANT OF LICENSES	27

ARTICLE 10 INTELLECTUAL PROPERTY	30

ARTICLE 11 FINANCIAL PROVISIONS	34

ARTICLE 12 PAYMENTS, BOOKS AND RECORDS	36

ARTICLE 13 PUBLICATIONS AND PRESS RELEASES	39

ARTICLE 14 CONFIDENTIALITY	40

ARTICLE 15 REPRESENTATIONS AND WARRANTIES	41

ARTICLE 16 INDEMNIFICATION, LIABILITY AND INSURANCE	42

ARTICLE 17 TERM AND TERMINATION	44

ARTICLE 18 MISCELLANEOUS	46

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

This Collaboration and License Agreement (this “Agreement”) is made and entered into by and between:

CRUCELL HOLLAND B.V., a Dutch company with offices located at Archimedesweg 4, 2333 CN Leiden, the Netherlands, (hereinafter “Crucell”);

and

BAVARIAN-NORDIC A/S (CRV No. 16 27 11 87), a Danish company with offices located at Hejreskovvej 10A, DK-3490 Kvistgård, Denmark, (hereinafter “BN”),

Crucell and BN being hereafter individually referred to as “Party” and collectively as “Parties”.

Recitals

WHEREAS Bavarian Nordic is the owner of a multivalent modified vaccinia Ankara (MVA) vector encoding several Filovirus proteins (the “Multivalent MVA-BN Vector”) and of certain intellectual property relating thereto;

WHEREAS, Crucell is the owner of a monovalent adenovirus26 vector encoding a Zaire strain Ebola protein (the “Monovalent Ad26 ZEBOV Vector”), a multivalent adenovirus 26 vector encoding Filovirus proteins (the “Multivalent Ad26 Vector”) and of certain intellectual property relating to each of the foregoing;

WHEREAS Crucell has entered into a license agreement effective 16 March 2005 with the United States National Institutes of Health concerning certain exclusive and non-exclusive licenses to various patent applications and issued patents(bearing NIH reference number[***]), which agreement has been amended by virtue of a first amendment thereto effective March 1, 2008 (bearing NIH reference number [***]); and a second amendment thereto effective September 1, 2011 (bearing NIH reference number [***]); and a third amendment thereto effective 20 March 2014 (bearing NIH reference number [***]);

WHEREAS, Crucell has entered into an agreement dated 30 September 2008 with the United States National Institutes of Health, National Institute of Allergy and Infectious Diseases concerning supply and testing of certain adenovirus vectors;

WHEREAS Bavarian Nordic and Crucell have each entered into separate Non-Clinical Evaluation Agreements (“NCEA”) dated 17 August 2011 with Crucell and 20 July 2012 with BN) with the National Institute of Allergy and Infectious Diseases (“NIAID”), an agency of the U.S. Government for evaluating the usefulness of, in the case of BN, the Multivalent MVA-BN Vector alone and, in the case of Crucell, a Multivalent Ad26 Vector alone, as candidates for vaccines for the prevention of Ebola virus infection;

WHEREAS Crucell and Bavarian Nordic have entered into a letter of understanding effective as of 18 September, 2013 (“LOU”), for the purpose of having NIAID perform (and pay for) a [***] study to evaluate: (a) Bavarian Nordic’s Multivalent MVA-BN Vector alone as a Filovirus vaccine candidate; and (b) the combination of BN’s Multivalent MVA-BN Vector with a Crucell Multivalent Ad26 vector as a Filovirus vaccine candidate (“Study”);

WHEREAS, on the Effective Date Crucell or an Affiliate of Crucell shall enter into a Subscription Agreement with Bavarian Nordic pursuant to which Crucell or an Affiliate of Crucell shall subscribe for shares in BN and the Parties shall enter into a Development Supply Agreement as defined below.

WHEREAS in view of the Study results, the Parties desire to enter into an agreement for the development and commercialization of vaccine regimens comprising Crucell’s Monovalent Ad26 ZEBOV Vector and Bavarian Nordic’s Multivalent MVA-BN Vector (“ZEBOV Vaccine”) and a Crucell Multivalent Ad26 Vector and Bavarian Nordic’s Multivalent MVA-BN Vector for use against Ebola.

NOW, THEREFORE, in consideration of the mutual covenants and promises set forth herein, the Parties, intending to be legally bound, agree as follows:

Article 1 Definitions

1.1 “Affiliate” means, with respect to a Party, any entity that is owned by or controlled by, owns or controls or who is under common control with that Party. For the purpose of this definition, “control” shall mean, direct or indirect, ownership of more than fifty percent (50%) of the shares of stock entitled to vote for the election of directors, in the case of a corporation, or more than fifty percent (50%) of the equity interest in the case of any other type of legal entity, status as a general partner in any partnership, or any other arrangement whereby the entity or person controls, or has the right to control, the board of directors or equivalent governing body of a corporation or other entity, or the ability to cause the direction of the management or policies of a corporation or other entity.

1.2 “Agreement” is defined in the Preamble.

1.3 “Agreement Term” means that period of time commencing on the Effective Date and continuing until the date on which this Agreement terminates.

1.4 “Applicable Law” shall mean the applicable provisions of any and all national, supranational, regional, state and local laws, treaties, statutes, rules, regulations, administrative codes, legally binding guidance, ordinances, judgments, decrees, directives, injunctions, orders, permits (including Marketing Authorizations) of or from any court, arbitrator, Regulatory Authority or government agency or authority having jurisdiction over or related to the subject item, including applicable GMP, GCP, GLP and health care compliance laws, laws pertaining to the protection of the environment, health, and safety, the United States Federal Corrupt Practices Act, export control laws, and laws and regulations pertaining to domestic or international corruption, commercial bribery, fraud, embezzlement, or money-laundering.

1.5 “Audited Party” shall have that meaning set forth in Section 12.8.

1.6 “Auditing Party” shall have that meaning set forth in Section 12.8.

1.7 “Biologics License Application” and “BLA” mean an application for permission to market a biologic product submitted to a Regulatory Authority to obtain Regulatory Approval for marketing a Licensed Product in a country or region.

1.8 “BN Indemnitee” shall have that meaning set forth in Section 16.2.

1.9 “BN Intellectual Property” and “BN IP” means BN Patent Rights BN Know-How

1.10 “BN Know-How” means Know-How concerning modified vaccinia Ankara vectors (including the Multivalent MVA-BN Vector), as well as the manufacture, use and administration thereof, that is Controlled by BN during the Term including BN’s interest in any Program Know-How (including BN’s interest in Joint Program Know-How). For the sake of clarity, Program Know-How concerning solely either a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector shall be Sole Program Know-How of BN but Program Know-How of BN explicitly excludes Program Know-How concerning solely either a Monovalent Ad26 ZEBOV Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector or Multivalent Adenovirus Vector, which shall be Program Know-How of Crucell.

1.11 “BN Patent Rights” means those Patent Rights Controlled by BN and/or its Affiliate(s) during the Term of this Agreement and that covers any Licensed Product or component thereof (including, in each case, its composition, formulation, combination, product by process, or method of use, manufacture, preparation or administration) or that would be necessary or reasonably useful for the Development,,Manufacture, use and/or Commercialization of Licensed Products in the Field. BN Patent rights shall include BN’s interest in any Joint Program Patent Rights and any Sole Program Patent Rights of BN. A list of certain BN Patent Rights existing as of the Effective Date is identified in Annex B, which list BN shall update as reasonably requested by Crucell in writing.

1.12 “BN Materials” means the Multivalent MVA-BN Vector, as well as other biological, chemical, mechanical and other physical materials of BN (and its Affiliates and Sublicensees) that are transferred or otherwise used in performing the activities hereunder, as well as those Program Materials made solely by employees of BN (and its Affiliates and Sublicensees) in performing the activities hereunder but explicitly excludes the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector which shall be Crucell Materials. As used herein, BN Materials shall include BN’s interest in any Program Materials, including BN’s interest in any Joint Program Materials.

1.13 “BN Regulatory Filings” means those Regulatory Filings Controlled by BN during the Term. BN Regulatory Filings includes but is not limited to those Regulatory Filings Controlled by BN concerning the Multivalent MVA-BN Vector.

1.14 “BN Technology” means BN Materials and BN Know-How.

1.15 “BN Trademarks” means those trademarks specified in Annex B.

1.16 “Business Days” means a day other than: (a) a Saturday or Sunday; or (b) a bank or other public holiday in the Netherlands; or (c) a bank or other public holiday in Denmark.

1.17 “Calendar Quarter” shall mean a financial calendar quarter based on the Johnson & Johnson Universal Calendar for that year; provided, however, that the first Calendar Quarter for the first Calendar Year shall extend from the Effective Date to the end of the then current Calendar Quarter and the last Calendar Quarter shall extend from the first day of such Calendar Quarter until the effective date of the termination or expiration of this Agreement.

1.18 “Calendar Year” shall mean a year during the Agreement Term based on the Johnson & Johnson Universal Calendar for that year (a 2014 copy of which is attached as Annex A) used for Crucell’s internal and external business purposes. The first Calendar Year of the Agreement Term shall begin on the Effective Date and shall end on the last day of then current Johnson & Johnson Universal Calendar Year during which the Effective Date occurs and the last Calendar Year of the Agreement Term shall begin on the first day of the Johnson & Johnson Universal Calendar Year for the year during which termination or expiration of the Agreement will occur, and the last day of such Calendar Year shall be the effective date of such termination or expiration.

1.19 “Change of Control” shall mean an acquisition by a Third Party directly or indirectly, of more than fifty percent (50%) of the shares of stock entitled to vote for the election of directors in the case of a corporation, or more than fifty percent (50%) of the equity interest in the case of any other type of legal entity (or if the jurisdiction where such corporation or other entity is domiciled prohibits foreign ownership of such entity, the maximum foreign ownership interest permitted under such laws, provided that such ownership interest provides actual control over such entity), status as a general partner in any partnership, or any other arrangement whereby an entity controls or has the right to control the Board of Directors or equivalent governing body of the entity.

1.20 “Claim” means all Third Party demands, claims, actions, proceedings and liability (whether criminal or civil, in contract, tort or otherwise) for losses, damages, reasonable legal costs and other reasonable expenses of any nature.

1.21 “Commercialize” and “Commercialization” mean all activities directed to Manufacturing, launching, marketing, promotion, educating, distribution, detailing, stockpiling, using, or sale of a Licensed Product (as well as importing and exporting activities in connection therewith) prior to and following receipt of Marketing Authorization for the Licensed Product in the relevant country, as well as all medical affairs activities, and all activities directed to Phase 4 Studies.

1.22 “Commercially Reasonable Efforts” means: (a) where applied to carrying out specific tasks and obligations of a Party under this Agreement, expending reasonable, diligent, good faith efforts and resources to accomplish such task or obligation (on its own and/or acting through any of its Affiliates or Sublicensees); and (b) as applicable in this Agreement, those efforts and resources commonly used by a Party to develop or commercialize a similar type of product of similar market and profit potential, for a vaccine used in a similar manner (for example, prophylactic vs prophylactic, therapeutic vs therapeutics, injectable vs injectable) and at a similar stage of development and product life cycle, based on scientific, legal, intellectual property, technical, medical, efficacy, safety, regulatory, competitiveness, commercial and other relevant conditions then prevailing. Commercially Reasonable Efforts shall be determined on a Licensed Product-by- Licensed Product basis.

1.23 “Confidential Information” means, all proprietary and unpublished information and data of a financial, legal, commercial, business, operational, scientific or technical nature which either: (a) the Disclosing Party or any of its Affiliates has supplied or otherwise made available (either orally, in writing or in electronic form) to the other Party or any of its Affiliates; or (b) a Party has generated in the course of the collaboration under this Agreement. In addition, and except as otherwise provided for herein, and then only to the extent necessary, the terms of this Agreement are to be kept confidential.

1.24 “Control”, “Controls,” “Controlled” or “Controlling” shall mean; in respect of any Patent Rights or Confidential Information or other intellectual property rights whether owned by or licensed to an entity, the possession of the legal right and ability to grant the respective rights, licenses or sublicenses as provided in this Agreement without violating the terms of any agreement or other arrangement with any Third Party, or misappropriating the proprietary or trade secret information of a Third Party.

1.25 “Crucell Indemnitee” shall have that meaning set forth in Section 16.1.

1.26 “Crucell Intellectual Property” means Crucell Patent Rights and Crucell Know-How.

“Crucell Know-How” means that Know-How concerning adenovirus26 vectors (including the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector), as well as the manufacture, use and administration thereof, that is Controlled by Crucell during the Term, including Crucell’s interest in any Program Know-How (including Crucell’s interest in any Joint Program Know-How). For the sake of clarity Program Know-How concerning solely either a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector shall be Sole Program Know-How of Crucell but Program Know-How of Crucell explicitly excludes Program Know-How concerning solely either a a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, which shall be Program Know-How of BN.

1.27 “Crucell Patent Rights” means those Patent Rights Controlled by Crucell during the Term of this Agreement and that cover any Licensed Product or component thereof (including, in each case, its composition, formulation, combination, product by process, or method of use, manufacture, preparation or administration) or that would be necessary or reasonably useful for the Development, Manufacture, use and/or Commercialization of Licensed Products in the Field. Crucell Patent Rights shall include Crucell’s interest in any Joint Program Patent Rights and any Sole Program Patent Rights of Crucell. A list of certain Crucell Patent Rights existing as of the Effective Date is identified in Annex C, which list Annex C, which list Crucell shall update as reasonably requested by BN in writing.

1.28 “Crucell Materials” means Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, as well as other biological, chemical, mechanical and other physical materials of Crucell (and its Affiliates and Sublicensees) that are transferred or otherwise used in performing the activities hereunder, as well as those Program Materials made solely by employees of Crucell (and its Affiliates and Sublicensees) in performing the activities hereunder but explicitly excludes the a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector which shall be BN Materials. As used herein, Crucell Materials shall include Crucell’s interest in any Program Materials, including Crucell’s interest in any Joint Program Materials.

1.29 “Crucell Regulatory Filings” means those Regulatory Filings Controlled by Crucell during the Term. Crucell Regulatory Filings includes but is not limited to those Regulatory Filings Controlled by Crucell concerning the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector.

1.30 “Crucell Technology” means Crucell Materials and Crucell Know-How.

1.31 “Crucell Trademarks” means those trademarks specified in Annex C.

1.32 “Currency Hedge Rate” means that rate calculated as a weighted average hedge rate of the outstanding external foreign currency forward hedge contract(s) of Johnson & Johnson’s Global Treasury Services Center (GTSC) and its Affiliates with third party banks. The hedge contract(s) is entered into to protect the transactional foreign exchange risk exposures of Crucell by reducing the impact of foreign currency volatility through a systematic build-up of a yearly Currency Hedge Rate(s).

1.33 “Derivatives” shall mean any or all of the following:

(a) unmodified descendants of either a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, as appropriate;

(b) substances, including modified descendants, created from or using a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, as appropriate, or that are expressed by either a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, as appropriate; and

(c) substances created which contain/incorporate either a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, as appropriate, or components thereof.

1.34 “Develop” and “Development” means the collaborative development program, to secure Regulatory Approval for the Licensed Products, as set out in more detail in the Development Plan.

1.35 “Development Plan” means the plan for development (including scientific development, as well as clinical and regulatory development) of a Licensed Product in the Development Program, wherein the activities to be performed by each Party during Development, as well as the timelines, milestones, resource planning, budgets, etc., associated therewith are set forth. Such plan may be updated from time to time in accordance with the provisions of Section 3.2.

1.36 “Development Program” means the collaborative research & development program, to produce the Licensed Product, as set out in more detail in the Development Plans.

1.37 “Discloser” shall have that meaning set forth in Section 14.1.

1.38 “Dispute” mean an issue relating to or arising out of the validity (including any Claim of inducement of this Agreement by fraud or otherwise), application, interpretation or construction of, or the compliance with or breach of, or termination of this Agreement or any ancillary agreement or any other matter designated hereunder or under any ancillary agreement for decision by the Parties or their respective Affiliates.

1.39 “Effective Date” means 22 October 2014.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.40 “Facilities” means those facilities for the development and/or Manufacture of either the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vectoror Licensed Products, as the case may be.

1.41 “Field” means all uses in the diagnosis, treatment and/or prophylaxis Filovirus infection. For the avoidance of doubt the Field does not include the treatment or prophylaxis of any infection by a virus which is not a Filovirus.

1.42 “Filovirus” means strains of any of the Ebola, Marburg and/or Cueva viruses.

1.43 “First Commercial Sale” shall mean the first sale in an arm’s length transaction and shipment of a Licensed Product for which a royalty is due pursuant to Section 11.2(b) to a Third Party by Crucell and its Affiliates or Sublicensees in the Field in the Territory. For the avoidance of doubt, a sale for of a Licensed Product for which no royalty is due pursuant to Section 11.2(a), shall not constitute a First Commercial Sale for purposes of this Agreement.

1.44 “FTE” means one employee full time for one year or more than one person working the equivalent of a full-time person, working directly on performing development activities according to the Development Plan, where “full-time” is determined in accordance with the applicable employment regulation for each relevant employee or, in the absence of such regulation, [***] hours. FTE costs shall be calculate at an FTE rate of [***] increased by the Danish Consumer Prices Index as published by Statistics Denmark from 1 January 2016.

1.45 “Good Clinical Practices” and “GCP” means, as of a given point in time and regulatory jurisdiction, then-current good clinical practices in accordance with the regulations and standards required by applicable Regulatory Authority(ies) in the applicable country/region.

1.46 “Good Laboratory Practices” and “GLP” means, as of a given point in time and regulatory jurisdiction, then-current good laboratory practices in accordance with the regulations and standards required by applicable Regulatory Authority(ies) in the applicable country/region.

1.47 “Good Manufacturing Practices” and “GMP” means, as of a given point in time and regulatory jurisdiction, then-current good manufacturing practices in accordance with the regulations and standards required by applicable Regulatory Authority(ies) in the applicable country/region.

1.48 “Government Authority” means any federal, state, national, state, provincial or local government, or political subdivision thereof, or any multinational organization or any authority, agency or commission entitled to exercise any administrative, executive, judicial, legislative, police, regulatory or taxing authority or power, any court or tribunal (or any department, bureau or division thereof, or any governmental arbitrator or arbitral body).

1.49 “Indemnitee” shall have that meaning set forth in Section16.3.

1.50 “Indemnitor” shall have that meaning set forth in Section 16.3.

1.51 “Initial Development Plan” shall mean: (i) the initial Development Plan for the initial Licensed Product having a Monovalent Ad26 ZEBOV Vector and a Multivalent MVA-BN Vector; and/or (ii) the initial Development Plan for the initial Licensed Product having a Multivalent Ad26 Vector and a Multivalent MVA-BN Vector; each as described in Section 4.2 attached as Annex F and “Initial Development Plans” shall means each aforementioned Initial Development Plan collectively.

1.52 “Invention” means any improvement to, or modification, whether patentable or not, of, the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector or the manufacture, use or administration of either or all of them, individually or combined in any manner as part of the Licensed Product, which is conceived and/or reduced to practice by the Parties, either individually or jointly in any combination, during and as part of the Development Plan and/or of Commercialization.

1.53 “Johnson & Johnson Universal Calendar” means that universal calendar that is set forth in Annex A.

1.54 “Joint Patent Rights” means those Patent Rights specified in the Section labelled “Joint Patent Rights” in Annexes B and C.

1.55 “Joint Program Intellectual Property” means Joint Program Patent Rights and Joint Program Know-How.

1.56 “Joint Program Inventions” means Program Inventions made by at least one BN employee and at least one Crucell employee during the course of, and as part of, any of the Development Programs and Commercialization. For the sake of clarity, Joint Program Inventions explicitly excludes Program Inventions concerning solely the a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, which shall be Sole Program Inventions of BN and Program Inventions concerning solely either the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, which shall be Sole Program Inventions of Crucell.

1.57 “Joint Program Know How” shall have that meaning set forth in Section 10.3(b). Joint Program Know-How shall include any Know-How that relates to the combined regime of

1.58 “Joint Program Materials” means those biological, chemical, mechanical and other physical materials that are made by employees of both Crucell (and its Affiliates and Sublicensees) and BN (and its Affiliates and Sublicensees) in performing the activities according to the Development Plan.

1.59 “Joint Program Patent Rights” shall have that meaning set forth in Section 10.2(b). Joint Program Patent Rights shall be listed in Annex H, which shall be updated from time to time, as set forth in Section 10.2(b).

1.60 “Joint Program Technology” means Joint Program Materials and Joint Program Know-How.

1.61 “Joint Steering Committee” means that committee of the same name, established and operating pursuant to the provisions of Section 3.1 of this Agreement.

1.62 “Know-How” means any information and materials that are not publicly known, including preclinical and clinical data, Regulatory Filings, other regulatory submissions and correspondence, manufacturing information and processes (including any and all information included in the Chemistry, Manufacturing and Control section of any Regulatory Filing or equivalent thereof), formulations, discoveries, improvements, modifications, processes, methods, protocols, formulae, data, procedures, culture medium and growth conditions, results and specifications, inventions, know-how and trade secrets, patentable or otherwise, but excluding any Patents.

1.63 “Licensed Product” means a Filovirus vaccine Developed or Commercialized under the terms of this Agreement comprising a multivalent modified vaccinia Ankara vector and either a monovalent adenovirus vector and/or a multivalent adenovirus vector in each case that encodes at least one antigen from a Filovirus.

1.64 “Manufacture” shall mean, with respect to a Licensed Product, those activities directed to the manufacturing, processing (including cell culturing), formulating, filling, primary and secondary packaging, holding (including storage), and quality control testing (including release) analytical method development, scale-up, validation and release of such Licensed Product or any component thereof. As used herein, Manufacturing may refer to any or all of the foregoing activities, as applicable.

1.65 “Marketing Authorization” or “MA” means, with respect to each country for each Licensed Product, the Regulatory Approval issued by the applicable competent Regulatory Authority in such country allowing for the Commercialization of such Licensed Product in such country.

1.66 “Monovalent Ad26 ZEBOV Vector” means that vector (and components thereof) referred to in the Recitals and specified in Annex D, as well as Derivatives thereof that are either: (i) made under this Agreement; or (ii) made outside this Agreement and mutually agreed to be used in the Development Program.

1.67 “Monovalent Adenovirus Vector” means a vector (and components thereof) derived from an adenovirus that encodes an antigen from one Filoviridae genus.

1.68 “Multivalent Ad26 Vector” means those vectors (and components thereof) referred to in the Recitals and specified in Annex D, as well as Derivatives thereof that are either: (i) made under this Agreement; or (ii) made outside this Agreement and mutually agreed to be used in the Development Program.

1.69 “Multivalent Adenovirus Vector” means a vector (and components thereof) derived from an adenovirus that encodes an antigen from more than one Filoviridae genus.

1.70 “Monovalent MVA Vector” means a vector (and components thereof) derived from an modified vaccinia Ankara virus that encodes an antigen from one Filoviridae genus.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.71 “Multivalent MVA-BN Vector” means that vector (and components thereof) referred to in the Recitals and specified in Annex D, as well as Derivatives thereof that are either: (i) made under this Agreement; or (ii) made outside this Agreement and mutually agreed to be used in the Development Program.

1.72 Multivalent MVA Vector” means a vector (and components thereof) derived from an modified vaccinia Ankara virus that encodes an antigen from more than one Filoviridae genus

1.73 “Net Sales” means, with respect to any Licensed Product, the gross amount invoiced by Crucell, its Affiliates or Sublicensees for sales in the Territory of such Licensed Product to a Third Party purchaser in an arms-length transaction less the following deductions, determined in accordance with US generally accepted accounting principles consistently applied and with its internal policies and procedures and accounting standards, to the extent specifically allocated to such Licensed Product and actually taken, paid, accrued, allowed, included or allocated based on good faith estimates in the gross sales prices with respect to such sales:

(a) [***];

(b) [***] on the sale of the Licensed Product to the extent [***];

(c) [***];

(d) [***];

(e) [***];

(f) [***].

All aforementioned deductions shall only be allowable to the [***], and in compliance with laws and regulations as well as Johnson & Johnsons Healthcare Compliance and other relevant policies, and shall be determined, on a country-by-country basis, as incurred in the ordinary course of business in type and amount consistent with the business practices of Crucell and its Affiliates, or Sublicensees (as the case may be) as applied across its product lines and accounting standards and verifiable based on its internal sales reporting system. All such discounts, allowances, credits, rebates, and other deductions shall be fairly and equitably allocated to the Licensed Product and other products of Crucell and its Affiliates and Sublicensees, such that Licensed Product does not bear a disproportionate portion of such deductions.

Sales between Crucell and its Affiliates or Sublicensees shall be disregarded for purposes of calculating Net Sales.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.74 “NIH License” means that license agreement effective [***] (and having NIH reference number [***]) between, on the one hand, [***], concerning exclusive and non-exclusive licenses to various patent applications and issued patents, as amended by a first amendment [***]; and a second amendment [***]; and a third amendment [***].

1.75 “Notice” shall have that meaning as set forth in Section 18.6 and “Notify” shall be the process of one Party informing another Party of an event hereunder by giving Notice.

1.76 “Operations Committee” means that committee of the same name, established and operating pursuant to the provisions of Section 3.2 of this Agreement.

1.77 “Out-Of-Pocket Expenses” means amounts paid to Third Party vendors or contractors, for services or materials provided by them directly in the performance of activities under this Agreement to the extent such services or materials apply directly to the Development Program and/or Licensed Products. Out-of-Pocket Costs do not include payments for internal: salaries or benefits; facilities; utilities; general office or facility supplies; insurance; information technology, capital expenditures or the like internal expenses.

1.78 “Outbreak” means the outbreak of the Ebola Zaire strain existing as at the Effective Date or thereafter during the Term of this Agreement which shall be considered to have ended on the earlier of (i) no cases of Ebola being reported for a period of [***] and (ii) Regulatory Approval of a Licensed Product.

1.79 “Party” and “Parties” shall have that meaning as set forth in the Preamble.

1.80 “Patent Rights” means all patents and patent applications (which for the purpose of this Agreement shall be deemed to include certificates of invention and applications for certificates of invention), including all divisionals, continuations, substitutions, continuations-in-part, re-examinations, reissues, additions, renewals, revalidations, registrations, pediatric exclusivity periods and Patent Term Extensions in jurisdictions that grants these rights and the like of any such patents and patent applications, and any and all foreign equivalents of the foregoing in jurisdictions that grants these rights.

1.81 “Patent Term Extension” means any term extensions, supplementary protection certificates, and equivalents thereof offering patent or patent-like protection beyond the initial term with respect to any issued patents.

1.82 “Pharmacovigilance Agreement” means that pharmacovigilance and adverse event reporting agreement setting forth the worldwide pharmacovigilance procedures for the Parties with respect to the Product, such as safety data sharing, adverse events reporting and prescription events monitoring.

1.83 “Phase 1” means a controlled human clinical trial of a compound or product that would satisfy the requirements of 21 CFR 312.21(a) or its foreign equivalents.

1.84 “Phase 2” means a controlled human clinical trial of a compound or product that would satisfy the requirements of 21 CFR 312.21(b) or its foreign equivalents.

1.85 “Phase 3” means a controlled or uncontrolled human clinical trial of a compound or product that would satisfy the requirements of 21 CFR 312.21(c) or its foreign equivalents.

1.86 “Phase 4” means any study or data collection effort in respect to any compound or product for a particular indication that is initiated after receipt of a BLA for the compound or product for such indication.

1.87 “Program Intellectual Property” means Program Patent Rights and Program Know-How.

1.88 “Program Inventions” means Inventions and other intellectual property rights conceived and/or reduced to practice in connection with either the Development Program and/or Commercialization.

1.89 “Program Know-How” means Know-How generated by either: (a) Crucell, and/or its Affiliates and/or Sublicensees ; and/or (b) BN or its Affiliates, each in conducting activities under the Development Program and/or Commercialization. For the sake of clarity, Program Know-How concerning solely a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector shall be Sole Program Know-How of BN and Program Know-How concerning solely either a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector shall be Sole Program Know-How of Crucell. As used herein, Program Know-How includes Joint Program Know-How.

1.90 “Program Materials” means collectively: (a) Crucell Materials and (b) BN Materials; and (c) Joint Program Materials. For the sake of clarity, (1) BN shall have full title to any Program Materials concerning the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector but not either the Monovalent Ad26 ZEBOV Vector and/or a Monovalent Adenovirus Vector, and/or a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, and such Program Materials shall thereafter be treated as Program Materials of BN; and (2) Crucell shall have full title to any Program Materials concerning the Monovalent Ad26 ZEBOV Vector and/or a Monovalent Adenovirus Vector, and/or a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector but not the Multivalent MVA-BN Vector, andor Multivalent MVA Vector andor a Monovalent MVA Vector and such Program Materials shall thereafter be treated as Program Materials of Crucell.

1.91 “Program Patent Rights” means those Patent Rights claiming or disclosing Program Inventions first conceived or reduced to practice in conducting activities under the Development Program and/or Commercialization. As used herein, Program Patent Rights includes Joint Patent Rights.

1.92 “Program Technology” means Program Materials and Program Know-How made or generated by either Crucell, its Affiliates and Sublicensees or BN and its Affiliates in conducting activities under either the Development Program or Commercialization. As used herein, Program Technology includes Joint Program Technology.

1.93 “Purpose” shall have the meaning as set forth in Section 2.1.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.94 “Recipient” shall have that meaning set forth in Section 14.1.

1.95 “Regulatory Approval” means, with respect to a Licensed Product in any country or jurisdiction, the approvals by the applicable Regulatory Authority in such country or jurisdiction necessary for the Manufacture and/or Development and/or Commercialization (as applicable) of the Licensed Products in that country or jurisdiction. For the avoidance of doubt, Regulatory Approval includes pricing or reimbursement approvals.

1.96 “Regulatory Authority” means any applicable Government Authority responsible for granting Regulatory Approvals for Licensed Products, including the United States FDA, European Medicines Agency, the World Health Organization and/or the Japanese Ministry of Health and Welfare and any relevant corresponding supranational, national or regional regulatory authorities.

1.97 “Regulatory Filings” means, with respect to any Licensed Product, any submission to a Regulatory Authority of any appropriate regulatory application specific to the Licensed Product or the use or making thereof, and shall include any submission to a regulatory advisory board and any supplement or amendment thereto. “Regulatory Filings” includes any IND, BLA and any Marketing Approval Application.

1.98 “Royalty Term” means, on a Licensed Product-by-Licensed Product basis, the period commencing on the date of the First Commercial Sale of the Licensed Product in the Territory and ending fifteen (15) years from the date of First Commercial Sale of the relevant Licensed Product.

1.99 “Safety Data Exchange” means the processes and system for the exchanging of safety data among the Parties as set forth in Annex F.

1.100 “Sales and Royalty Report” shall have that meaning set forth in Section 12.1

1.101 “Sole Program Inventions” shall means those inventions made solely by the employees, Affiliates or Sublicensees of one Party during the course of, and as part of, any of the Development Programs and Commercialization. For the sake of clarity, Sole Program Inventions concerning solely the a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector shall be Sole Program Inventions of BN and Sole Program Inventions concerning solely either the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector shall be Sole Program Inventions of Crucell regardless of which Party employed the inventors in respect of such Sole Program Inventions.

1.102 “Sole Program Know-How” shall have that meaning set forth in Section 10.3(a).

1.103 “Sole Program Patent Rights” shall have that meaning set forth in Section 10.2(a).

1.104 “Sublicensee” shall mean, with respect to a particular Licensed Product, a Third Party to whom Crucell has granted a license to offer to make, sell, import, use or offer for sell such Licensed Product for administration to human subjects.

1.105 “Supply Agreements” means the Development Supply Agreement and the Commercialization Supply Agreement each as defined in Section 7.3(a) and Supply Agreement shall mean either of them as the context requires.

1.106 “Tax” or “Taxes” means any present or future taxes, levies, imposts, duties, charges, assessments or fees of any nature (including any interest thereon).

1.107 “Term” shall have the meaning set forth in Section 17.1 herein.

1.108 “Territory” means the world.

1.109 “Third Party” means any entity or person other than a Party, or an Affiliate of a Party or a Sublicensee.

1.110 “Valid Claim” shall mean a claim in any applicable Patent Right, which claim has not expired or been held invalid or unenforceable by a non-appealed or unappealable decision by a court or other appropriate body of competent jurisdiction, and which is not admitted to be invalid through disclaimer or dedication to the public.

Article 2 Collaboration Overview

2.1 Purpose. The purpose of this Agreement is to define the terms under which Crucell and BN will collaborate in the Development, Manufacture and Commercialization of Licensed Products (“Purpose”).

2.2 Scope. The activities that are to be conducted to achieve the purpose of this Agreement include Development activities, Manufacturing activities and Commercialization activities, as follows:

(a) In Development, the Parties will perform various activities using the Crucell Technology, Crucell IP, the BN IP and the BN Technology according to a mutually-agreed upon Development Plan to Develop Licensed Products that may be released for emergency use authorization. It is desired, but not required, that these Licensed Products also meet World Health Organization (“WHO”) prequalification requirements so as to enable Crucell to register the Licensed Products in the Field and the Territory and to apply for WHO prequalification for the Licensed Products (as set out in Section 4.4 of this Agreement). The foregoing activities include, but are not limited to:

(1) making clinical supplies of their respective materials for the development work;

(2) cooperating to secure external funding for development costs;

(3) performing an additional Phase 1/2 study with a candidate Licensed Product; and

(4) applying for Marketing Authorization for the candidate Licensed Product.

(b) In Commercialization, the Parties will perform various activities with the Licensed Products, so that Crucell can Commercialize the Licensed Products in the Field and the Territory; and

(c) In both Development and Commercialization, the Parties will perform various activities using the Crucell Technology and the BN Technology to Develop a process to Manufacture Licensed Product and to then Manufacture Licensed Product for Development and Commercialization

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

2.3 Other Project. Nothing in this Agreement shall prevent the Parties from continuing or establishing other programs for the development of Filovirus vaccines or vaccines against any other viruses provided such do not conflict with the exclusivity granted according to this Agreement. Notwithstanding anything to the contrary in this Agreement, BN shall, subject to the provisions of Section 9.6, be free to undertake any development or commercialization of any (i) Monovalent MVA Vector, Multivalent MVA Vector or Multivalent MVA-BN Vector against Filovirus combined with virus approaches (including pox viruses) that are not adenovirus based.; (ii) any monovalent vaccine against a Filovirus that are not adenovirus based; and (iii) any vaccine regardless of the vector against a virus that is not a Filovirus.

Article 3 Governance

3.1 Joint Steering Committee

(a) Committee Responsibilities. Crucell and BN will establish a Joint Steering Committee (JSC) that will:

(1) evaluate the progress of, and approve changes to, the Development Plans;

(2) serve as a forum to discuss strategic and material issues that arise during Development and Commercialization, including the BN budgets and/or costs; and

(3) review and resolve deadlocks of the Operations Committee.

(b) Membership. The JSC shall be comprised of two representatives from each of Crucell and BN, being senior business persons from Crucell and BN, with the necessary authority to make decisions on the issues that shall be handled by the JSC, as provided for herein. The initial members of the JSC shall be appointed by each Party within one (1) week of the Effective Date. BN and Crucell may replace its JSC representatives at any time, with written notice to the other Party.

(c) Decision-Making. The JSC shall strive to obtain unanimity in all its decisions in relation to its responsibilities as defined in Section 3.1. In case no unanimous decision can be reached in the JSC, then: (1) if the matter involves Development activities funded by a party other than Crucell, then each Party shall be entitled to refer the matter to a senior executive designated by each Party (but who is not a member of the JSC or the Operations Committee), who shall use their good faith efforts to mutually agree upon the proper course of action to resolve the matter. In the event said executives are unable to resolve such matter or agree upon a mechanism to resolve such matter within [***] of the referral to said executives resolution under this Section 3.1(c), then subject to 3.1(d) below, the Parties shall resolve such matter in accordance with Section 18.13; (2) if the matter involves the Manufacture of a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, subject to 3.1(d) below, BN shall have the final decision making authority subject to the change control terms of the Supply Agreements or the associated Quality Agreements; and (3) if the matter involves Development activities funded unilaterally by Crucell or Commercialization, then subject to 3.1(d) below, Crucell shall have final decision-making authority relative thereto. For the avoidance of doubt, this right shall not reduce Crucell’s obligations to use Commercially Reasonable Efforts to Develop and Commercialize Licensed Products.

(d) Notwithstanding any other term of this Agreement neither Party may use its final decision making authority in the JSC or Operations Committee to require the other Party to apply more FTEs than provided for in the relevant Development Plan or to spend more money than is provided for in the relevant Development Plan.

(e) After the end of Development Program for a Licensed Product, the JSC will: (i) serve as a forum for the exchange of information and assistance concerning the Licensed Product and Commercialization; (ii) participate in the management and resolution of conflicts between the Parties; and (iii) approve publications.

(f) Committee Meetings. During the Agreement Term, the JSC shall meet at least two times each Calendar Year, either through a conference call or a face-to-face meeting, at least one of said meetings to be held in a manner and location alternating between BN’s choosing and Crucell’s choosing. Moreover, the Parties agree to meet in person or through a conference call as necessary to further the goals of the Development Program and Commercialization. The Parties agree that the first meeting of the JSC shall take place no later than one (1) month from signing this Agreement and, at the end of each JSC meeting, to plan the next meeting. In the event that a Party would like to postpone a JSC meeting, it shall so inform the other Party in a timely manner prior to the date of such planned JSC meeting by notification given to the other Party. However, a JSC meeting cannot be postponed for more than four (4) weeks if the other Party does not consent to such longer postponement.

3.2 Operations Committee

(a) Committee Responsibilities. Crucell and BN will establish a joint Operations Committee that will evaluate the progress of the applicable Development Plan and any changes proposed to the applicable Development Plan, in so far as such changes materially impact any of the following:

(1) the Licensed Products that are included in the Development Plans (i.e., the introduction of a new Licensed Product or the termination of Development of a Licensed Product);

(2) the timelines established for completing the activities under the Development Plans; and

(3) the duties or responsibilities of either Party under the Development Plans.

Such changes shall be subject to approval by the JSC.

Communications between the Parties shall be managed through the Operations Committee.

(b) Membership. The Operations Committee shall be comprised of an equal number of voting representatives from each of Crucell and BN. The exact number of such representatives shall be at least two (2) for each of Crucell and BN, and shall include from each Party, at least one senior business person and the principle senior manager in charge of the collaboration. The initial members of the Operations Committee shall be appointed by each Party within one (1) week of the Effective Date. BN and Crucell may replace its Operations Committee representatives at any time, with written notice to the other Party. The Parties agree that, in addition to the members of the Operations Committee appointed by each Party, participation by certain additional employees, agents or (other) representatives of their respective companies may be necessary or desirable from time to time, depending upon the subject matter

to be discussed at a given meeting. In such event, the Party that wishes that an extra representative attend such Operations Committee meeting, shall without undue delay Notify the other Party in advance of such meeting and shall be responsible for all costs associated with such person’s participation. For the avoidance of doubt, such invited persons shall not be considered members of the Operations Committee and, thus, will have no vote on any decisions to be taken by the Operations Committee.

(c) Decision-Making. The Operations Committee shall strive to obtain unanimity in all its decisions in relation to its responsibilities a defined in Section 3.2(a). Nonetheless, the Operations Committee will make decisions by majority vote. In case no decision can be reached in the Operations Committee, escalation shall be made to the Joint Steering Committee for resolution.

(d) Sub-Committees. From time to time, the Operations Committee may establish subcommittees to which it can delegate the responsibilities of the Operations Committee for particular projects or activities in or for the Development Program, Regulatory Affairs and Manufacturing, as further specified below herein, and such subcommittees will be constituted as the Operations Committee agrees.

(e) Committee Meetings.

(1) During the Development Program, the Operations Committee shall meet at least monthly, either through a conference call or a face-to-face meeting. The Parties agree that at least the meetings of the Operations Committee will be held in a manner and at a location that alternates between a locale of BN’s choosing and a locale of Crucell’s choosing. The Parties agree that the first meeting of the Operations Committee shall take place no later than one (1) month from signing this Agreement and to plan the next meeting of the Operations Committee at the end of each Operations Committee Meeting. In the event that a Party would like to postpone an Operations Committee meeting, it shall so inform the other Party in a timely manner prior to the date of such planned Operations Committee meeting by notification given to the other Party. However, an Operations Committee meeting cannot be postponed for more than one (1) week if the other Party does not consent to such longer postponement.

(2) During Commercialization, the Operations Committee shall meet at the reasonable written request of a Party, either through a conference call or a face-to-face meeting.

(f) Committee Agenda Responsibilities.

(1) During the Development Program, the Operations Committee will: (i) provide scientific guidance to the Parties in connection with the Development Program and monitor and review the progress and results generated in the Development Plans; (ii) evaluate the progress against the Development Plans; (iii) review and approve on an annual basis the Development Plans and the budget therefor, pursuant to Section 4.2 of this Agreement, (iv) propose modifications and amendments to the Development Plans, (v) manage and resolve technical conflicts that may arise during Development; and (vi) approve publications developed during the course of the Development Program.

(g) Chairperson. Crucell’s lead representative shall chair the meetings of the Operations Committee until the Agreement is terminated or until there is no longer a need for an Operations Committee Meeting, as mutually agreed by the Parties.

(h) Minutes. Crucell’s lead representative in the Operations Committee shall be responsible for preparing the agenda and minutes for such meetings. A draft agenda must be submitted to Operations

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Committee members at least [***] prior to the scheduled meeting. Modifications or additions to the agenda shall be incorporated at the reasonable discretion of the chairperson, who shall provide the final agenda at least twenty-four (24) hours prior to the meeting. Minutes shall be prepared and forwarded to all Operations Committee members for comment within two weeks after the close of the meeting. Comments will be incorporated into the minutes if received within two (2) weeks after receipt. If no comments are received within such two-week period, the minutes shall become an official record of the meeting.

Article 4 Development

4.1 Scope. Subject to the terms and conditions set forth herein, Crucell and BN shall cooperate in the performance of the Development Program to develop and register Licensed Products in the Field and Territory. The Parties shall execute the activities according to the Development Plans.

4.2 Development Plans.

(a) Establishment. The Initial Development Plans for the Licensed Product having the Monovalent Ad26 ZEBOV Vector and the Multivalent MVA-BN Vector and the Licensed Product having the Multivalent Ad26 Vector and the Multivalent MVA-BN Vector are attached hereto as Annex F. If Parties mutually agree (without either Party being obliged to do so) to Develop further Licensed Products, the Parties shall mutually agree upon and prepare further Development Plans for each such further Licensed Product (if any) and such plan shall be agreed upon in the Operations Committee before the commencement of the Development activities to be performed thereunder and attached hereto as subsequent annexes to this Agreement.

(b) Content. Each Development Plan shall specify the objectives and work plan activities of both Parties, outline the various steps and activities that shall be conducted to develop the Licensed Product which is the subject of that Development Plan, which Party shall be responsible for and conduct such activities and the headcounts, budgets and other costs and expenses, including consultants and Third Party contractors, associated therewith. Each Development Plan shall also provide for the development of research, pre-clinical and clinical data for use in relevant Regulatory Filings. Each Development Plan shall contain a description of the milestones intended to be reached and the intended target dates for the same to be reached in order to Develop the Licensed Product in question.

(c) Review and Approval. The activities conducted in connection with the applicable Development Plan will be overseen and administered by the Operations Committee as authorized pursuant to Section 3.2. To this end, prior to the beginning of each Calendar Year during each respective Development Plan, the Operations Committee shall review and agree on an updated Development Plan, if needed. Increases in budget for either Party shall be subject to JSC approval subject to the provisions of Section 3.1(d). If the JSC is not able to complete its review and approval of the updated Development Plans for an upcoming Calendar Year, the budget for the applicable Development Plan in effect shall be continued until the Parties can complete the review and approval process.

(d) Modification. If, at any time, circumstances require the modification of a Development Plan, the Operations Committee shall review such Development Plan as soon as possible and shall recommend to the Parties an appropriate modification, which shall be put into effect on both Parties’

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

written approval thereof and, subject to the provisions of Section 3.1(d), a Party receiving such a proposal shall respond as to whether it accepts or rejects such proposal in [***].

4.3 Development Diligence.

(a) Of BN. BN shall be solely responsible for the activities set forth for it to perform in the respective Development Plan, directly or through Affiliates or Third Parties, and in accordance with the said Development Plan and the budget therefore which is then in effect. In this regard, BN shall use Commercially Reasonable Efforts to:

(1) perform those activities and allocate those resources in accordance with the applicable Development Plan and in compliance with Applicable Law;

(2) report to the Operations Committee, on a quarterly basis, the progress of the applicable Development Plans; and

(3) fully adhere to the J&J Policy on the Employment of Young Persons (a copy of which, existing as of the Effective Date, is attached hereto as Annex J, applicable anti-corruption laws, including but not limited to the United States Federal Corrupt Practices Act (FCPA) and health care compliance (HCC) policies, regulations and laws, as well as such other laws, regulations and J&J Policies as the Parties may agree.

(b) Of Crucell. Crucell shall be solely responsible for the activities set forth for it to perform in the respective Development Plan, directly or through Third Parties, and in accordance with the said Development Plan and the budget therefore which is then in effect. In this regard, Crucell shall use Commercially Reasonable Efforts to:

(1) perform those activities and allocate those resources in accordance with the applicable Development Plan and in compliance with Applicable Law;

(2) report to the Operations Committee, on a quarterly basis, the progress of the applicable Development Plans; and

(3) fully adhere to the J&J Policy on the Employment of Young Persons, applicable anti-corruption laws, including but not limited to the United States Federal Corrupt Practices Act (FCPA) and health care compliance (HCC) policies, regulations and laws, as well as such other laws, regulations and J&J Policies as the Parties may agree.

4.4 Development Activities.

(a) BN shall use Commercially Reasonable Efforts to:

(1) ensure that the Manufacturing process and clinical program for the Multivalent MVA-BN Vector is adequate for receipt of Regulatory Approval in the Territory;

(2) ensure that the Manufacturing process and clinical program for the Multivalent MVA-BN Vector is adequate to comply with the World Health Organization (“WHO”) vaccine prequalification program and apply for WHO prequalification for the Multivalent MVA-BN Vector, as well as to make it possible to release the Licensed Product for emergency use authorization pursuant to United States law (although, consistent with Section 2.2(a), it is not an obligation of BN to achieve the foregoing);

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(3) obtain and maintain the licensed and Regulatory Approvals for the Multivalent MVA-BN Vector necessary in the European Union and in the event reasonably requested by Crucell, paid for by Crucell, to support Crucell in relation to the submission of Regulatory Filings of Licensed Products done in the Territory; and

(4) make BN Materials (including but not limited to GMP grade BN Materials) available to Crucell for Development in accordance with the Development Plan or as otherwise set forth in the Supply Agreements or their associated Quality Agreements agreed by the Parties and paid for Crucell for the Development Plan.

(b) Crucell shall use Commercially Reasonable Efforts to:

(1) ensure that the Manufacturing process and clinical program for the Monovalent Ad26 ZEBOV Vector andor the Multivalent Ad26 Vectors are adequate for receipt of Regulatory Approval in the Territory;

(2) ensure that the Manufacturing process and clinical program for the Monovalent Ad26 ZEBOV Vector andor the Multivalent Ad26 Vectors are adequate to comply with the World Health Organization (“WHO”) vaccine prequalification program and apply for WHO prequalification for the Monovalent Ad26 ZEBOV Vector andor the Multivalent Ad26 Vectors as well as to make it possible to release the Licensed Product for emergency use authorization (although, consistent with Section 2.2(a), it is not an obligation of Crucell to achieve the foregoing); and

(3) obtain and maintain all licensed and Regulatory Approvals for the Monovalent Ad26 ZEBOV Vector andor the Multivalent Ad26 Vectors useful to support Crucell in relation to the submission of all Regulatory Filings of Licensed Products done in the Territory.

4.5 Development Program Records. The Parties shall maintain, or cause to be maintained, records of the Development Program in sufficient detail and in good scientific manner, and upon reasonable request of the other Party at least one copy in the English language, as will properly reflect all work done and results achieved in the performance of the Development Program (including all data in the form required under any applicable governmental regulations). Each Party shall allow the other to have access without undue delay to all materials and data generated on behalf of such Party during the Development Program at reasonable times and in a reasonable manner, such information disclosed being subject to Article 14 (Confidentiality).

4.6 Development Reports. Each Party shall, during the term of this Agreement, provide the Operations Committee with a quarterly written report summarizing the progress of its contribution to the Development Program during the preceding Calendar Quarter. Such report shall be submitted no later than [***] after the relevant Calendar Quarter.

4.7 Access to Information and Data.

(a) Each Party shall have the right to receive and use all information generated pursuant to the activities performed by the other Party under the Development Plans, but solely to the extent it is: (i) permitted under this Agreement; and (ii) necessary to Develop and Commercialize Licensed Products; and (iii) specifically subject to Article 14 (Confidentiality).

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(b) Insofar as BN is legally and contractually permitted to do so, BN shall provide to Crucell relevant information that relates to the safety, quality and other critical attributes of the BN Technology to allow Crucell to compile Regulatory Filings.

4.8 Funding.

(a) Initial Development Plans. It is the intention of the Parties that those Development activities in Part A of the Initial Development Plan for the Licensed Product having the Monovalent Ad26 ZEBOV Vector and the Multivalent MVA-BN Vector and Part B of the Initial Development Plan for the Licensed Product having at least the Multivalent Ad26 Vector and the Multivalent MVA-BN Vector shall be funded in whole or in part by the United States National Institutes of Health (NIH) or other governmental or external bodies. In the event that such NIH funding and/or other governmental and/or external funding is not obtained, Crucell shall assume full responsibility for paying the budgeted costs as set forth in the Development Plan for those Development activities in Part A as well as those Development activities in Part B of the Initial Development Plan for the Licensed Product to the extent those activities are not covered by said United States National Institutes of Health (NIH) or other governmental or external bodies.

Crucell anticipates that funding will be obtained from the United States government to support the activities contemplated by this Agreement, BN agrees to be bound by those FAR (Federal Acquisition Regulation) clauses that are incorporated into the agreements providing or resulting from any such US government funding arrangements. Those clauses will be incorporated herein with the same force and effect as imposed upon Crucell or its Affiliates due to the United States government funding arrangements.

(b) Other Development Plans. Crucell shall be responsible for all of the budgeted costs of conducting the Development Plans as set forth in the Development Plans including the Initial Development Plans.

(c) Payments.

(1) [***] under the [***] shall be based on [***], as set forth in the[***]. The total is not to exceed the amounts to be agreed by the Parties and set forth in the [***] provided always where [***] provided for in the [***] it shall not be obliged to conduct further work unless [***].

(2) [***] shall account for and report to [***] in the performance of its [***] under the [***] for which it [***] during each [***] to [***], as described in section[***] below.

(3) During each Calendar Year, [***] will keep [***] informed of any significant [***] for such Calendar Year.

(d) External Funding. Crucell may seek resources to fund activities to be performed under this Agreement either alone or in co-ordination with BN.

(e) Excess Development Plan Costs. Unless otherwise agreed by the Parties, neither Party shall be obligated to incur Development Plan costs beyond those amounts provided for in the approved Development Plans. Nonetheless, the Parties may agree that one Party may elect to pay for Development

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Plan costs in excess of those costs provided for in the respective Development Plan therefor, provided such payment is approved by the JSC subject to the provisions of Section 3.1(d).

4.9 Technical Assistance. Subject to the prior agreement by the Parties as to the allocation of resource and the cost, BN shall provide Crucell with reasonable technical support at Crucell’s cost and expense.

Article 5 Regulatory Affairs

5.1 Responsibilities. Subject to the supervision of the Operations Committee, consistent with the license grants of Article 9 and except as otherwise provided herein, Crucell shall fund and be responsible for the preparation and submission of Regulatory Filings, including Market Authorization Application and Clinical Trial Applications, relating to Licensed Products in its own name with Regulatory Authorities in the Territory. Subject to BN having the FTE resources available, shall provide Crucell with necessary and reasonably relevant assistance requested by Crucell for the preparation and submission of said Regulatory Filings. Crucell shall reimburse all of BN’s FTE and Out-Of-Pocket costs in assisting in preparing such Regulatory Filings.

5.2 [Intentionally Omitted]

5.3 Submission of Clinical Trial Protocols and Regulatory Filings. Notwithstanding any other provision herein, all protocols for clinical trials during Development that BN and/or Crucell plans to conduct for the Licensed Products, shall be submitted to the other Party in English prior to the initiation of such trials and prior to the Regulatory Filing of such protocols with any Regulatory Authority. The submitting Party shall include any comments and recommendations received from the other Party prior to the submission to the Regulatory Authorities, provided the other Party has provided such comments and recommendations within [***] from receipt of the protocol, and such comments and recommendation are substantive and reasonable. If a Party plans not to include comments and recommendations received from the other Party it shall notify the other Party prior to the submission to the Regulatory Authorities.

5.4 Adverse Event Reports. The Parties shall cooperate in the coordination of common reporting to Regulatory Authorities, on a timely basis, of all safety-related and adverse events occurring during clinical development and subsequent to the grant of Regulatory Approvals. Prior to commencing clinical trials on any Licensed Product, the Parties or their authorized agents shall enter into a written agreement concerning policies and procedures for pharmacovigilance and adverse event reporting, which shall be binding on both Parties.

5.5 Access to and Use of Data.

(a) Regulatory Data. Both Parties shall have access to pre-clinical and clinical data for Licensed Products, and the right to use for incorporation in any Regulatory Filing to exercise their rights

and responsibilities under this Agreement. Both Parties shall provide to each other access to that part of all such Regulatory Filings together with the underlying pre-clinical and clinical data, at reasonable times and on reasonable notice, and at the FTE costs and Out-of-Pocket Expenses of the requesting Party. In case that data in a Regulatory Filing of a Licensed Product is required or reasonably useful for a Regulatory Filing for the BN Technology, then Crucell shall provide BN with the appropriate written authorizations to permit BN to send directly such data to the appropriate Regulatory Authority, and Crucell shall diligently cooperate with BN to supply data to that Regulatory Authority in the required formats at the FTE costs and Out-of-Pocket Expenses of BN. In case that data in a Regulatory Filing for the BN Technology is required or reasonably useful for a Regulatory Filing for a Licensed Product, then Crucell shall provide BN with the appropriate written authorizations to permit BN to directly send such data to the appropriate Regulatory Authority.

(b) Third Party and Affiliate Obligation of Data Access. In all agreements with Third Parties, Affiliates or Sublicensees involving the generation of clinical data for Licensed Products, each Party shall require that such Third Parties, Affiliates and Sublicensees provide both Parties full access to all such data, at no charge, to the extent that such data is required to be obtained from such Third Parties, Affiliates and Sublicensees by an appropriate Regulatory Authority.

Article 6 Commercialization

6.1 Scope. Subject to the terms and conditions set forth herein, during Commercialization, BN shall Manufacture and supply the Multivalent MVA-BN Vector and Crucell shall Manufacture and supply the Monovalent Ad26 ZEBOV Vector and/or the Multivalent Ad26 Vectors and the Licensed Product from the foregoing and Crucell shall Commercialize (including, marketing, selling, and offering for sale) the Licensed Products in the Field in the Territory.

6.2 Commercialization Activities.

(a) Of Crucell. Crucell shall have the right and use Commercially Reasonable Efforts to Manufacture import, use, sell, and offer for sale Licensed Products in the Field and in the Territory for which it has received Regulatory Approval or approval to do so under a government procurement process and shall be solely responsible for all Commercialization of Licensed Products in the Territory, either directly or through Third Parties.

(b) Of BN. Subject to the terms of the Commercialization Supply Agreement, BN shall Manufacture and supply to Crucell the Multivalent MVA-BN Vector as necessary for Crucell to Manufacture and Commercialize Licensed Products in the Territory. In this regard, BN shall use Commercially Reasonable Efforts to:

(1) report, on an annual basis, on the progress of the BN Manufacturing plan and Manufacturing results;

(2) Manufacture the Multivalent MVA-BN Vector in accordance with the Quality Agreement and the relevant quality standards and to meet the requirements imposed by the prequalification requirements of the World Health Organization, (although, consistent with Section 2.2(a), it is not an obligation of Bavarian to achieve the foregoing);;

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(3) Manufacture the Multivalent MVA-BN Vector in accordance with Applicable Law, the J&J Policy on the Employment of Young Persons, the United States Federal Corrupt Practices Act (FCPA) and health care compliance laws and regulations and policies (HCC), as well as such other J&J Policies as the Parties may agree from time to time; and

(4) make available the quantities of the Multivalent MVA-BN Vector as ordered by Crucell in accordance with the Commercialization Supply Agreement.

6.3 Diligence.

(a) Of BN. Subject to the terms of the Commercialization Supply Agreement, BN shall use Commercially Reasonable Efforts to Manufacture and supply the Multivalent MVA-BN Vector in sufficient quantities to satisfy the demand (without interruption).

(b) Of Crucell. Crucell shall use Commercially Reasonable Efforts to Commercialize Licensed Products in the Territory for which it has received Regulatory Approval or under a government procurement process.

If Crucell shall have dosed the first patient in a Phase 1 clinical study before July 1 2015 it shall be considered to have met obligation under this Section 6.3(b) up to this point.

If Crucell shall have done any of the following (i) dosed the first patient in a Phase 2 clinical study of a Licensed Product or (ii) dosed the first patient in a Phase 1 clinical study of a combination of a Multivalent MVA Vector and a Multivalent Adenovirus Vector or (iii) selling of [***] doses of Licensed Product, in each case before 31 December 2016, it shall be considered to have met obligation under this Section 6.3(b) up to this point.

If Crucell shall have sold [***] doses of Licensed Products in the aggregate then it shall be considered to have met its obligation under this Section 6.3(b).

(c) Under NIH License. The Parties shall use commercially diligent efforts relative to Licensed Products, as set forth in Sections 10.1-10.3 of the NIH License, as set forth in Annex I.

6.4 Access to Information and Data. Insofar as a Party is legally or contractually permitted to do so and insofar as has been mutually agreed between the Parties in writing, each Party shall provide to the other Party relevant information that relates to the safety, quality and other critical attributes of the Licensed Products in sofar as required to allow Crucell to compile and maintain an acceptable dossier for Regulatory Authorities in relation to Licensed Products.

6.5 JSC. During Commercialization, the JSC shall serve as a vehicle for the exchange of information concerning Commercialization. Notwithstanding the role of the JSC, to the extent that such decisions do not increase the obligations on BN to provide FTE support or incur costs beyond that which BN has already agreed, all business decisions involving the design, sale, price, and promotion of Licensed Products by Crucell, its Affiliates or its Sublicensees under this Agreement shall be within the sole discretion of Crucell.

6.6 Trademarks. Crucell shall be free to market the Licensed Products under such labels and tradenames/trademarks as it may elect, provided that nothing in this Agreement shall be construed as a

trademark license. Notwithstanding the foregoing, the packaging of each Licensed Product shall acknowledge that the Multivalent MVA-BN Vector is manufactured by BN.

6.7 Distributors. Crucell may authorize distributors to market, sell and distribute Licensed Products in the Territory.

6.8 Term of Commercialization Phase. The Commercialization Phase shall start upon the receipt by Crucell of Regulatory Approval for the commercialization of a first Licensed Product and shall end upon the termination of this Agreement for the last Licensed Product.

Article 7 Manufacturing

7.1 Manufacturing Rights and Obligations.

(a) Of BN. BN shall have the exclusive right, and is obligated, to exert Commercially Reasonable Efforts to Manufacture the Multivalent MVA-BN Vector and supply the same to Crucell for incorporation into Licensed Products for Development and Commercialization in the Territory, as set forth in the Supply Agreement.

(b) Of Crucell. Crucell shall have the exclusive right, and is obligated, to exert Commercially Reasonable Efforts to Manufacture the Monovalent Ad26 ZEBOV Vector and the Multivalent Ad26 Vectors for incorporation into Licensed Products, as well as the Licensed Products (using the Multivalent MVA-BN Vector supplied by BN) for Development and Commercialization in the Territory.

7.2 BN Manufacturing Plan. In respect to any Licensed Product, no later than by 31 December 2014, BN shall prepare and mutually agree with Crucell upon a plan for the Manufacture and supply of the Multivalent MVA-BN Vector to Crucell for that Licensed Product (“BN Manufacturing Plan”).

7.3 BN Supply of Multivalent MVA-BN Vector.

(a) On the Effective Date the Parties have entered into a supply agreement outlining the terms for BN’s supply of the Multivalent MVA-BN Vector to Crucell for Development and emergency use in human subjects (the “Development Supply Agreement”). A separate supply agreement for Commercialization (the “Commercialization Supply Agreement”) shall be negotiated before the first filing of a BLA or application for Marketing Approval in accordance with the terms outlined in this Agreement. Together with both the Development Supply Agreement and the Commercialization Supply Agreement (the “Supply Agreements”), separate quality agreements (“Quality Agreements”) shall be entered into between the Parties at the same time outlining their responsibilities regarding assurance of Licensed Product quality, safety, and efficacy. The Quality Agreement relating to the Development Supply Agreement shall also be entered into no later than by 30 November 2014.

(b) The Supply Agreements shall specify:

(1) agreed acceptance criteria (including, but not limited to, specifications) for the Multivalent MVA-BN Vector supplied thereunder;

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(2) ordering and delivery timeframes for the Multivalent MVA-BN Vector, on the basis of firm orders placed in advance by Crucell and such other terms that are customary in such agreements;

(3) a procedure to establish and review quantities of safety stock of the Multivalent MVA-BN Vector to be held by Crucell, where it will be held, the period for which such safety stock will be held and the payment conditions relating thereto.

(c) During the term of this Agreement, Crucell shall have the right, at its expense, upon reasonable written notice, and during normal business hours, to inspect BN’s and BN’s Third Party contractor’s facilities engaged in the Manufacture of Licensed Products and any records relating thereto once per year, or more often with cause, to verify compliance with the terms of this Agreement, the Supply Agreements, the Quality Agreements, and Applicable Law. After such inspections, Crucell shall provide observations to BN in writing, and BN will provide written responses to such observations and provided that such measures are necessary according to Applicable Law or BN agrees that corrective measures are necessary, BN will describe corrective action plan(s) within [***] after receipt of such observations from Crucell. BN shall implement (or cause its Third Party contractors to implement) corrective actions within [***] or allowed in the Applicable Law or such longer period as agreed after providing such response agreeing to the need for corrective measures, or if not possible, a schedule shall be negotiated and agreed to by the Parties.

Article 8 Reports and Access to Know-How

8.1 Performance Reporting. Each Party shall keep the other Party regularly informed via the JSC about the performance of, and technical data concerning, for BN the Multivalent MVA-BN Vector and for Crucell, the Monovalent Ad26 ZEBOV Vector and the Multivalent Ad26 Vectors and shall provide the other Party, on an annual basis within [***] after the anniversary of the Effective Date, with a summary report of the data relating specifically to the respective said Vector’s performance, including specifically any and all substantial positive and/or negative deviations from the standard established operating, culturing and manufacturing parameters found useful in its application for the Manufacture of Licensed Product and as set out in the Development Plan. Each Party shall without undue delay Notify the other Party in writing of any substantial negative deviations from established characteristics and/or performance parameters of its Vector simultaneously with its notification of any other entity other than the appropriate Regulatory Authorities. To facilitate the mutually beneficial resolution of any technical performance issue relating to such a substantial negative deviation, BN hereby agrees to permit Crucell’s technical personnel reasonable access to relevant technical data and to the Facilities to assist in resolving such issues.

8.2 Access to Know How

(a) Crucell shall have the right to review the BN Know How to the extent that it is necessary or reasonably useful for regulatory purposes to perform under this Agreement or concerns either BN’s Program Materials after providing BN with [***] prior Notice requesting such review, and such information requested will be made available insofar BN is legally and contractually permitted to disclose such information.

(b) Each Party acknowledges that the Know How is owned by the other Party is of crucial importance to that other Party. Accordingly, each Party agrees that it shall not be entitled to, and agrees that it will not, characterize, issue releases or certificates of analysis for, or analyze the genome of the vectors of the other Party (being, for BN, the Multivalent MVA-BN Vector, any Multivalent MVA Vector or any Monovalent MVA Vector and, for Crucell, the Monovalent Ad26 ZEBOV Vector, any Monovalent Adenovirus Vector, any Multivalent Adenovirus Vector and/or the Multivalent Ad26 Vector), or engage in any research of the other Party’s Know-How that concern any safety, toxicity or tumorigenicity of that vector without obtaining the prior written approval of the other Party.

(c) Each Party further agrees to use Commercially Reasonable Efforts to without undue delay Notify the other Party of any and all communications to and from Governmental Authorities relating to the safety of any of its technology, and agrees to consult without undue delay to resolve any such concerns with such Governmental Authorities. Noncompliance with the obligation to use its reasonable efforts to without undue delay Notify and consult in its efforts to resolve any such issues with such Governmental Authorities shall be considered a failure to comply with a material condition of this Agreement.

Article 9 Grant of Licenses

9.1 Crucell License Grants to BN. Pursuant to the terms and conditions herein, Crucell hereby grants to BN;

(a) Development Licenses.

(1) a non-exclusive, non-transferable, non-sublicensable (except to Affiliates for performing Development activities for BN hereunder), non-royalty bearing sub-license under the Crucell Patent Rights set forth in Parts 1 and 2 of Annex C to conduct those activities assigned to BN in the Development Plans, including but not limited to the Manufacture and sale to Crucell of the Multivalent MVA-BN Vectors; and

(2) a non-exclusive, non-transferable, non-sublicensable (except to Affiliates for performing Development activities for BN hereunder), non-royalty-bearing license (under the Crucell Patent Rights in Part 3 of Annex C and the Crucell Know-How) to conduct those activities assigned to BN in the Development Plans, including but not limited to the Manufacture and sale to Crucell of the Multivalent MVA-BN Vectors; and

(b) Commercialization Licenses.

(1) a non-exclusive non-transferable, non-sublicensable (except to Affiliates performing Manufacturing activities for BN hereunder) license under the Crucell Patent Rights set forth in Part 2 of Annex C to Manufacture the Multivalent MVA-BN Vector, Multivalent MVA Vectors or Monovalent MVA Vectors as provided for hereunder; and

(2) an-exclusive non-transferable, non-sublicensable (except to Affiliates performing Manufacturing activities for BN hereunder) license under the Crucell Patent Rights set forth in Parts 1 and 3 of Annex C and the Crucell Know-How to Manufacture the Multivalent MVA-BN Vector, Multivalent MVA Vectors or Monovalent MVA Vectors as provided for hereunder.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

The term of each of the licenses set forth in this Section 9.1 shall commence upon the Effective Date and shall continue: (i) in the case of the licenses granted under Section 9.1(a), until the termination of the last Development Plan or valid early termination of this Agreement as provided for in Article 17 and (ii) in the case of the licenses granted under Section 9.1(b), until the termination of this Agreement.

9.2 BN License Grants to Crucell. Pursuant to the terms and conditions herein, BN and its Affiliates hereby grant to Crucell and its Affiliates, the following licenses:

(a) Development License. BN hereby grants to Crucell a non-exclusive, non-transferable, non-sublicensable (except to Affiliates), non-royalty-bearing license under the BN Intellectual Property to import and use the Multivalent MVA-BN Vector, Multivalent MVA Vectors or Monovalent MVA Vectors in the Field and in the Territory to conduct (or to have conducted for it) those activities assigned to Crucell in the respective Development Plans. The term of this license shall commence upon the Effective Date and shall continue until the termination of the last Development Plan or valid early termination of this Agreement as provided for in Article 17.

(b) Commercialization Licenses.

(1) BN hereby grants to Crucell an exclusive, sub-licensable, license under the BN Intellectual Property to import and use the Multivalent MVA-BN Vector, Multivalent MVA Vectors or Monovalent MVA Vectors and to develop, import, make, register, use, sell and offer for sale (and to have any of the foregoing done for it by a Third Party) Licensed Products in the Field and in the Territory. Crucell will notify BN of the grant of sublicenses hereunder to parties who are neither Affiliates nor distributors within [***] of the granting of such license. Crucell shall remain liable for any action or omission by a sublicensee which would, if an action or omission of Crucell, have been a breach of this Agreement.

(3) Notwithstanding anything to the contrary in this Agreement, (i) Crucell shall have no right to Manufacture the Multivalent MVA-BN Vector, Multivalent MVA Vectors or Monovalent MVA Vectors; and (ii) subject to Section 9.2(b)(3) nothing shall preclude BN from undertaking alone or, with any Third Party any development or commercialization of any (A) Multivalent MVA Vector or Monovalent MVA Vector against Filovirus combined with virus approaches (including pox viruses) that do not use an adenovirus as the vector or containing fragments thereof; (B) any monovalent vaccine against a Filovirus that does not use an adenovirus as the vector or containing fragments thereof; and (iii) any vaccine regardless of the vector against a virus that is not a Filovirus.

(4) Crucell shall not and shall procure that its Affiliates and sub-licensees do not, develop, import, make, register, use, sell and/or offer for sale Licensed Products outside of the Field, and shall effectively ensure that any such Prohibited Activities are prohibited and do not take place. Furthermore, Crucell may not undertake any promotion or inducement, or any kind of activities directly or indirectly related to, the potential furtherance of any Prohibited Activities.

(5) In the event that Crucell has, other than for reasons within BN’s control, not dosed the first patient in a Phase 1 clinical study before July 1 2015BN shall have the right but not the obligation by written notice to be received by Crucell on or before 1 September 2015 to convert the licenses granted in this Section 9.2(b) to non-exclusive licenses.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

In the event that Crucell has not, other than for reasons within BN’s control, done at least one of the following (i) dosed the first patient in a Phase 2 clinical study of a Licensed Product or (ii) dosed the first patient in a Phase 1 clinical study of a combination of a Multivalent MVA Vector and a Multivalent Adenovirus Vector or (iii) selling of [***] doses of Licensed Product, in each case before 31 December 2016, BN shall have the right but not the obligation by written notice to be received by Crucell on or before 1 March 2016 to convert the licenses granted in this Section 9.2(b) to non-exclusive licenses.

9.3 Public Health Concerns.

(a) Emergency Outbreaks. The provisions of Sections 9.1 and 9.2 notwithstanding, for the Outbreak then either BN or Crucell may develop, import, make, register, use, sell and offer for sale (and to have any of the foregoing done for it by a Third Party) in the case of BN, a Multivalent MVA Vector andor a Monovalent MVA Vector or in the case of Crucell, Licensed Products for use only for the relevant Outbreak but the foregoing exception shall not include any sale or other disposal commercial sales made for stockpiling.

(b) Other Public Health Concerns. In the event of public health concerns, other than Outbreaks as provided for in Section 9.3(a), then the Parties shall discuss in good faith what measures that the Parties can agree to take hereunder to furnish Licensed Products or take other measures to address such public health concerns.

9.4 Sublicenses. BN acknowledges that the Crucell Patent Rights identified in Part 1 and Part 2 of Annex C are the subject of the NIH License to Crucell and that, in the event of a conflict between the terms and conditions of this Agreement and the terms and conditions of the NIH License, then the terms and conditions of the NIH License shall prevail. In this regard, BN agrees that any sublicenses granted hereunder to the Patent Rights listed in Parts 1 or 2 of Annex C shall be subject to the obligations to the licensor of the NIH License set forth in Annex I.

9.5 NIH Licenses. The Parties recognize that the licenses granted under §9.01 are subject to the rights of the licensor of the NIH License as is set forth in the NIH License, including without limitation in Sections 5.01-5.04 of the NIH License, as set forth in Annex I.

9.6 Right of First Refusal. During the Term of this Agreement, BN grants Crucell a right of first refusal to acquire the rights and licenses for commercialization (and development) to products developed wholly or in part by BN during the term of Development and having a Multivalent MVA-BN Vector, or Multivalent MVA Vector or a Monovalent MVA Vector for the treatment of, or prophylaxis against, a Filovirus. To this end, BN shall Notify Crucell of the availability of the product for licensing at any time before the expiry of [***] after the completion of Phase 1 for that product and, within [***] of Crucell’s receipt of the said Notice from BN, Crucell shall Notify BN of its desire to enter into good faith negotiations on the terms and conditions for said rights and licenses. In the event that Crucell declines to enter into such negotiations, then BN shall be free to offer the product to other parties. In the event that Crucell accepts to enter into such negotiations, the Parties shall enter into good faith negotiations to conclude such negotiations within [***] of BN’s receipt of Crucell’s Notice of its desire to have the negotiations. A written agreement between the Parties on the terms and conditions for

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

such product shall be required. In the event that such negotiations are not concluded in the said [***] period, then BN shall be free to offer the product to other parties on such terms as it sees fit.

Article 10 Intellectual Property

10.1 Ownership of Inventions and Materials.

(a) Inventorship of Program Inventions shall be determined in accordance with the patent and other intellectual property laws of the country in which the invention was made.

(b) A Party shall solely own title to all of its Sole Program Inventions. For the sake of clarity, Sole Program Inventions concerning solely the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector shall be Sole Program Inventions of BN and Sole Program Inventions concerning solely either the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or a Multivalent Ad26 Vector shall be Sole Program Inventions of Crucell regardless of which Party employed the inventors in respect of such Sole Program Inventions and each Party hereby does and shall assign any Patent Rights or other intellectual property rights in such Sole Program Inventions to the Party entitled to such Sole Program Invention pursuant to this Section 10.1(b). Each Party shall cooperate in executing whatever documents are necessary to establish legal title in and ownership of Patent Rights disclosing or claiming such Sole Program Inventions..

(c) BN shall have full title to those Program Materials concerning the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector but not either the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, and such Program Materials shall thereafter be treated as Program Materials of BN; and (2) Crucell shall have full title to those Program Materials concerning the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 but not the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector and such Program Materials shall thereafter be treated as Program Materials of Crucell and each Party hereby does and shall assign any Materials, Patent Rights or other intellectual property rights in such Program Materials to the Party entitled to such Program Materials pursuant to this Section 10.1(c). Each Party shall cooperate in executing whatever documents are necessary to establish legal title in and ownership of Patent Rights disclosing or claiming such Program Materials.

(d) The Parties shall jointly own title to all Joint Program Inventions, including Joint Program Inventions concerning both the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector and either the the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26, such as their use together in a single therapy regime. As an exception to the foregoing: (1) BN shall have full title to those Joint Program Inventions concerning the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector but not either the the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26, which shall thereafter be treated as Sole Program Inventions of BN; and (2) Crucell shall have full title to those Joint Program Inventions concerning the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector but not the Multivalent MVA-BN

Vector, Multivalent MVA Vector or a Monovalent MVA Vector which shall thereafter be treated as Sole Program Inventions of Crucell and each Party hereby does and shall assign any Patent Rights or other intellectual property rights in such Joint Program Inventions to the Party entitled to such Joint Program Invention pursuant to this Section 10.1(d).Each Party shall cooperate in executing whatever documents are necessary to establish legal title in and ownership of Patent Rights disclosing or claiming such Joint Program Inventions.

10.2 Patent Prosecution.

(a) Sole Program Inventions. BN or Crucell, as the case may be, shall, at its own expense, control the preparing, filing, prosecuting and maintaining the Patent Rights relating to its Sole Program Inventions (“Sole Program Patent Rights”) worldwide, in such countries as it deems appropriate, and conducting any interferences, re-examinations, reissues, oppositions or requests for patent term extensions relating thereto using counsel of that Party’s choice.

(b) Joint Program Inventions. To provide for the most sensible, efficient, and cost effective means to protect Joint Program Inventions, patent counsel for BN and Crucell shall consult with each other. As a result of such consultation, mutually-agreed external patent counsel will be chosen to prepare, file, prosecute and maintain patent applications and patents worldwide on such Joint Program Inventions (“Joint Program Patent Rights”), and to send each Party updates Annex H, as needed, and the Parties shall equally share the costs thereof. In the event that Parties disagree in respect of preparing, filing, prosecuting and maintaining patent applications and patents worldwide on such Joint Program Inventions, such Dispute shall be solved according to Section 18.13 giving the arbitration court full discretion in deciding the disputed issue.

(c) Prosecution by Other Party. In the event that either BN or Crucell, as the case may be (the “Owner”), declines to file or, having filed, declines to further prosecute and maintain any of its Patent Rights to Sole Program Inventions under Sections 10.2(a) or (b), respectively, or conduct any interferences or oppositions or request any re-examinations, reissues or extensions of patent term with respect to its Patent Rights to Sole Program Inventions under Section 10.2(a) or (b), respectively, in any country, such Owner shall notify the other Party hereto.

(d) Cooperation. Each of BN and Crucell shall keep the other reasonably informed as to the status of such patent matters within the other Party’s Territory relating to Patent Rights to Sole or Joint Program Inventions under Section 10.2(a) or (b), respectively to the other Party, including, without limitation, by providing the other the opportunity to review and comment on any documents which will be filed in any patent office, and providing the other copies of any documents that such Party receives from such patent offices, including notice of all interferences, re-examinations, oppositions or requests for patent term extensions. BN and Crucell shall each cooperate with and assist the other in connection with such activities, at the others’ request and expense.

(e) Third Party Rights. The provisions of Section 10(d) shall be subject to, and limited by, any agreements pursuant to which BN and Crucell, as the case may be, acquired any particular Patent Right. It is understood that such agreements may require, for example, that the licensor Party from whom BN or Crucell acquired a license to such Patent Right control the prosecution of particular patents and patent applications and does not permit access or an opportunity to comment on any documents filed in patent offices.

(f) Patent Rights in Part 1 and Part 2 of Annex C. The prosecution and maintenance of those Patent Rights listed in Part 1 and Part 2 of Annex C shall be done at the sole discretion of Crucell. In this regard, BN recognizes that the licensor of the NIH License may participate in, or control, such prosecution and/or maintenance.

10.3 Ownership of Know-How.

(a) A Party shall solely own title to all Know-How made by only its employees and those of its Affiliates and Sublicensees during the course of, and as part of, any of the Programs (“Sole Program Know-How”), so that BN shall solely own all Program Know-How made by only its employees and those of its Affiliates and Crucell shall solely own all Program Know-How made by only its employees and/or its Affiliates and/or Sublicensees. For the sake of clarity, Program Know-How concerning solely a Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector shall be Sole Program Know-How of BN and Program Know-How concerning solely either a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector shall be Sole Program Know-How of Crucell and each Party hereby does and shall assign any Patent Rights or other intellectual property rights in such Program Know-How to the Party entitled to such Program Know-How pursuant to this Section 10.3(a). Each Party shall cooperate in executing whatever documents are necessary to establish legal title in and ownership of Patent Rights disclosing or claiming such Program Know-How.

(b) The Parties shall jointly own title to all Know-How made by at least one employee of BN or its Affiliates or Sublicensees and at least one employee of Crucell or its Affiliates or Sublicensees during the course of, and as part of, any of the Programs (“Joint Program Know-How”), except that Program Know-How concerning solely the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector, which shall be Sole Program Know-How of BN and Program Know-How concerning solely either the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector, which shall be Sole Program Know-How of Crucell and each Party hereby does and shall assign any Patent Rights or other intellectual property rights in such Joint Program Know-How to the Party entitled to such Joint Program Know-How pursuant to this Section 10.3(b).Each Party shall cooperate in executing whatever documents are necessary to establish legal title in and ownership of Patent Rights disclosing or claiming such Joint Program Know-How.

10.4 Defense of Third Party Infringement Claims. If the production, sale or use of any Licensed Product developed pursuant to this Agreement results in a Claim, suit or proceeding alleging patent infringement against BN or Crucell (or their respective Affiliates or Sublicensees), such Party shall without undue delay Notify the other Party hereto in writing setting forth the facts of such Claim in reasonable detail. The Party subject to such Claim shall have the exclusive right to defend and control the defense of any such Claim, suit or proceeding, at its own expense, using counsel of its own choice, provided, however, it shall not enter into any settlement which admits or concedes that any aspect of the Patent Rights or Know-How of the other Party hereto is invalid or unenforceable without the prior written consent of such other Party. Such Party shall keep the other Party hereto reasonably informed of all material developments in connection with any such Claim, suit or proceeding.

10.5 Enforcement.

(a) Notification. In the event that a Party become aware that a Third Party is infringing one or more of the Program Patent Rights or any other Patent Right licensed hereunder, it shall without undue delay Notify the other Party of any such infringement setting forth the salient facts relating thereto.

(b) Control of Suit.

(1) Solely-Owned Crucell Patent Rights. As to the infringement of solely-owned Crucell Patent Rights, Crucell shall have the exclusive right and sole discretion to effect termination of such infringement, including bringing suit or other proceedings against the infringer in its own name and BN shall be kept informed at all times of all such proceedings taken by Crucell but only so as far as the Crucell Patent Rights in suit relates to a Licensed Product. If Crucell requests, BN may, at BN’s discretion, join with Crucell as a Party to the lawsuit or other proceeding at Crucell’ expense; however, Crucell shall retain control of the prosecution of such suit or proceedings, as the case may be.

(2) Solely-Owned BN Patent Rights. As to the infringement of solely-owned BN Patent Rights, BN shall have the exclusive right and sole discretion to effect termination of such infringement, including bringing suit or other proceedings against the infringer in its own name and Crucell shall be kept informed at all times of all such proceedings taken by BN only so as far as the BN Patent Rights in suit relates to a Licensed Product. If BN requests, Crucell may, at Crucell’s discretion, join with BN as a Party to the lawsuit or other proceeding at BN’s expense; however, BN shall retain control of the prosecution of such suit or proceedings, as the case may be.

(3) Joint Program Patent Rights and Joint Patent Rights. In the event that any Joint Program Patent Right or Joint Patent Right is infringed or misappropriated by a third party, BN and Crucell shall negotiate in good faith to mutually agree upon whether, and, if so, how, to enforce or defend said Patent Right in a declaratory judgment or similar proceeding. If the Parties cannot agree, then as joint and several owners of the Patent Right, each Party may exercise its legal rights without the consent of the other Party.

(4) Costs and Monetary Recovery. Unless the Parties agree otherwise and save as provided above, each Party shall bear all its costs incurred in connection with such lawsuit or other proceeding, and consequently shall be entitled to collect and retain for its own account any damages or profits as may be accrued as a result of such lawsuit or other proceeding.

(5) NIH License. The enforcement of those Patent Rights listed in Part 1 and Part 2 of Annex C shall be done at the sole discretion of Crucell. In this regard, BN recognizes that the licensor of the NIH License may participate in, or control, such enforcement.

10.6 Disclaimer. Nothing in this Agreement shall be construed as obligating either Party, or giving either Party the right, to proceed against a Third Party infringer.

10.7 Patent Term Extensions. BN hereby authorizes Crucell to provide in any BLA or its equivalent, a list of patents that include the Patent Rights of the other Party that relate to such Licensed Product and such other information, as the Party deems appropriate. In the event that any Applicable Law in any country provides for the extension of any term of any patent included among Patent Rights, at the request of Crucell or at it its own initiative, BN shall apply for and use its reasonable efforts to obtain such an

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

extension of the BN Patent Rights or Joint Program Patent Rights. BN shall further cooperate with Crucell in obtaining any such extensions. BN agrees to execute such documents, or to arrange to have such documents executed, and take such actions as Crucell may reasonably request in connection herewith at Crucell’s cost and expense.

10.8 Special Provisions. Both Parties, as well as their respective German Affiliates and German Sublicensees performing activities hereunder, shall:

(a) have in place a corporate policy that: (i) requires employees and contractors to assign their Inventions made during the course of their work, as well as the intellectual property rights (the Patent Rights and Know-How rights) concerning such Inventions, to their employers; and (ii) governs the compensation that such employees and contractors are to receive for such Inventions, Patent Rights and Know-How rights;

(b) agree with their German employees and German contractors acting on their behalf to assign their Inventions, as well as the intellectual property rights (the Patent Rights and the Know-How rights concerning those Inventions), made under the Development Program and/or while conducting Commercialization activities, to their employers; and

(c) agree with their German employees or any other German person acting on their behalf on any and all royalty or other compensation payable to their said employee or other person, or any invention conceived, reduced to practice, developed, made or created in the performance of, or as a result of, the Research Program by said employees or any other person acting on their behalf; and

(d) be responsible for paying to said German employees or any other person acting on their behalf any and all royalty or other compensation payable to the employee or other person, for any invention conceived, reduced to practice, developed, made or created in the performance of, or as a result of, the Research Program by said employees or any other person acting on their behalf; and

(e) compensate their German employees and German contractors for all such Inventions, as well as the intellectual property rights (the Patent Rights and the Know-How rights concerning those Inventions) made under the Development Program and/or while conducting Commercialization activities.

Article 11 Financial Provisions

11.1 Supply Price. In consideration for the supply of the Multivalent MVA-BN Vector hereunder and under the Commercialization Supply Agreement, Crucell shall pay BN for the supply of the Multivalent MVA-BN Vector in accordance with the Commercialization Supply Agreement at a price to be agreed but that does not exceed the cost charged under the Development Supply Agreement adjusted for inflation as per the Danish Consumer Price Index as published by Statistics Denmark with the first such adjustment being made in 1 January 2016.

11.2 Payments on Net Sales. In consideration for the rights granted hereunder, Crucell shall pay BN a royalty during the Royalty Term, at the following rates:

(a) [***] percent ([***]%) of Net Sales of Licensed Products by Crucell, its Affiliates and Sublicensees made to an other than those specified in Section 11.2(b); or

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(b) [***] percent ([***]%) of Net Sales of Licensed Products by Crucell, its Affiliates and Sublicensees for all sales (i) if the sale is at a price which is greater than or equal to Crucells cost of goods as calculated in accordance with Crucell’s usual procedures consistently applied to vaccine products plus [***] percent ([***]%), or (ii) in any of the US, the European Economic Area, Switzerland, Japan, Singapore or South Korea unless such sale in such country is made to an institute listed in Annex G at less than Crucells cost of goods as calculated in accordance with Crucell’s usual procedures consistently applied to similar products plus [***] percent ([***]%).

(c) Those royalties, if any, to be paid for Net Sales of Licensed Products by Crucell, its Affiliates and Sublicensees for sales for diagnostics applications shall be negotiated in good faith between the Parties upon one of the Parties delivering Notice to the other Party of the desire to have such negotiations. The Parties hereby agree that they shall not unreasonably delay or refuse to have such negotiations.

11.5 Other Royalty Provision. No royalties shall accrue on the disposition of a Licensed Product by either Party in reasonable quantities without direct or indirect consideration being received by the Parties such as samples (promotional or otherwise) or as donations at less than cost price (for example, to non-profit institutions or government agencies for a non-commercial purpose, or to patient assistance programs) or for use in Clinical Studies conducted by or on behalf of Crucell.

11.6 Third Party Royalties. To the extent that royalties, license fees, and milestone or other payments are due to Third Parties under licenses or similar agreements necessary to allow the Manufacture, importation, use or sale or offer for sale of the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector or any component thereof but not necessary for the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector such payments shall be made by Crucell provided always that Crucell shall be entitled to deduct [***] percent ([***]%) of such payments from the royalties payable to BN pursuant to Section 11.2(b) subject to such royalties not being reduced below [***] percent ([***]%) of Net Sales. For the sake of clarity, a component of the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector is not necessary for the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector if that same component is part of the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector.

11.7 Crucell Payment Obligations. Crucell shall be solely responsible for the payment of any royalties, license fees, and milestone or other payments due to Third Parties under licenses or similar agreements necessary to allow the Manufacture, importation, use or sale or offer for sale of the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector (or any component of the foregoing) but not necessary for the the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector. For the sake of clarity, a component of the Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector (or any component of the foregoing) is not necessary for a the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Vector merely because that same component is part of a the Multivalent MVA-BN Vector, Multivalent MVA Vector or a Monovalent MVA Vector as appropriate.

11.8 Further Payment Obligations. Crucell shall be responsible for the payment of and pay any royalties, license fees, and milestone or other payments due to Third Parties under licenses or similar agreements necessary to allow the Manufacture, importation, use or sale or offer for sale of the Licensed Product other than those set forth in Sections 11.6 and/or 11.7.

11.9 Payments and Milestones.

(a) Upfront Fee. Within [***] of the Effective Date, Crucell shall pay BN an upfront fee of twenty-five million United States dollars (25,000,000 USD).

(b) Milestone Payments. Crucell shall pay BN the following one time milestone payments:

(1) [***] for which a royalty is due under Section 11.2(b) in the Territory.

(2) [***].

11.10 If, under a US government funding arrangement pursuant to Section 4.8, any of the payments under this Agreement or the Development Supply Agreement are reduced or reclaimed by the US government, Crucell shall pay to BN an amount equal to the amount of the reduction or reclaim.

Article 12 Payments, Books and Records

12.1 Royalty Reports and Payments. After the supply of the first Licensed Product to a Third Party by Crucell, its Affiliates or Sublicensees of a Licensed Product on which royalties are payable, Crucell will submit to BN a written Sales and Royalty Report for each Licensed Product, in the form as set forth in Annex E, within [***] after the end of each Calendar Quarter, setting out in respect of each country in which Licensed Product’ is supplied to a Third Party, by Licensed Product, the quantity and Net Sales value of Licensed Products sold or supplied free of charge during the Calendar Quarter to which the royalty payment relates. The report shall show the total Net Sales value for each country expressed both in local currency and in the payment currency as defined in Section 12.3 below, showing the conversion rate used; and showing for each Licensed Product the applicable royalty rate and the calculation of the royalties payable pursuant to Section 11.2. Concurrently with the submission of such reports, the selling Party shall pay such royalties to the other Party within [***] after the end of the respective Calendar Quarter. In addition, a final report shall be submitted by BN to Crucell within [***] of termination or expiration of this Agreement.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

12.2 Payments for Costs Incurred by either Party. Following the Effective Date, within [***] after the end of each respective Calendar Quarter during the term of this Agreement (and up to 2 Calendar Quarters after the term of this Agreement), BN will provide Crucell with a report detailing the actual costs incurred during such Calendar Quarter as part of the Development Program (as described in section 4.8 above) in such reasonable detail and format to enable Crucell to reimburse BN for such costs. BN will provide and send to Crucell an invoice for such amount which shall be payable within [***] after the receipt thereof in the currency described in section 12.3 below. The Parties shall use Commercially Reasonable Efforts to provide all reports hereunder in sufficient time to permit the Parties to comply with their reporting obligations under applicable securities laws, rules and regulations.

12.3 Method of Payment. The payment to be made under Section 11.9(a) shall be paid in USD. Save in respect of the payment to be made under Section 11.9(a) all other payments due hereunder to BN shall be made in Euros and paid by bank wire transfer in immediately available funds to a bank account designated in writing by BN.

12.4 Interest. If any payment under this Agreement is not made by the date on which the same becomes due and payable and in case the delay is not occasioned by Force Majeure, the late Party shall owe the other Party interest at [***] percent ([***] %) on any outstanding amount assessed from the date the late Party receives notice from the other Party of such unpaid amount that is overdue, until payment is made in full.

12.5 No Refunds. Payments referred to herein shall not be refundable under any circumstances, including but not limited to the termination of this Agreement for whatever reason.

12.6 Currency Conversion. If any currency conversion shall be required in connection with the calculation of royalties or payments hereunder, such conversion shall be made using the following method: for the upcoming calendar year, Crucell shall provide BN: (a) a Currency Hedge Rate(s) to be used for the local currency of each country of the Territory; and (b) the details of such Currency Hedge Rate(s) in writing. This shall be provided not later than [***] after the Currency Hedge Rate(s) are available from Crucell, which is customarily in December. Such Currency Hedge Rate(s) will remain constant throughout the upcoming calendar year. The Parties shall use the Currency Hedge Rate(s) to convert Net Sales to Euro for the purpose of calculating royalties and payments between the Parties.

12.7 Taxes.

(a) Withholding. The paying Party will make each payment to the other Party under this Agreement without deduction or withholding for Taxes except to the extent that any such deduction or withholding is required by law in effect at the time of payment. Any Tax required to be withheld on amounts payable under this Agreement will be paid by the paying Party on behalf of the other Party to the appropriate governmental authority, and the paying Party will furnish the other Party with proof of payment of such Tax. Any such Tax required to be withheld will be an expense of and borne by the other Party. Prior to any first payment by the paying Party to the other Party in one Calendar Year, the said other Party shall provide the paying Party with any relevant form required by the Tax authorities in order for the said other Party to:

(1) attest to the other Party’s fiscal residence; and

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(2) obtain the application of the reduced withholding tax rate or the exemption of the withholding tax, according to the relevant bilateral agreement against double taxation.

The paying Party will forward to the said other Party such relevant application forms for fulfillment at least [***] prior to any payment. In the event the said other Party fails to return such forms duly filled and signed before a payment date, the paying Party will declare and pay withholding tax at the local common law rate applicable to the payments, and the paying Party will deduct such tax from the corresponding payment to the said other Party. The paying Party shall remit the withholding tax to the proper Tax authority and proof of payment of such tax shall be secured and sent to the said other Party as evidence of such payment.

(b) V.A.T. All amounts in this Agreement are stated to be exclusive of VAT and other sales or indirect taxes, which may be due on any invoice. If any such taxes are payable on the payments under this Agreement, then the payor shall be responsible for the payment of such taxes to the payee following receipt of a valid tax invoice from the payee.

12.8 Records and Inspections. Each Party and its Affiliates shall keep complete, true, and accurate books of account and financial records for the purpose of determining the payment amounts (including royalty payments (including the amount of royalties due under the NIH License), payments for Development costs incurred and payments based on the Cost of Goods) payable under this Agreement and payable under the NIH License. Such books and records shall be kept at the principal place of business of such Party or its Affiliate, as the case may be, for at least [***] following the end of the Calendar Quarter to which they pertain. Upon the written request of the representative or agent of the Party conducting the audit (the “Auditing Party”) but not more often than once each Calendar year, at the Auditing Party’s expense, the party being audited (the “Audited Party”) shall permit an independent certified accountant selected by the Auditing Party and reasonably acceptable to the Audited Party to have access during normal business hours to those financial records of the Audited Party (and its Sublicensees where relevant) as may be reasonably necessary for the sole purpose of verifying the accuracy of the quarterly royalty calculations and invoices for Development costs incurred. Such examination shall be limited to a period of time no more than [***] immediately preceding the request for examination.

The report of the independent certified accountant shall be shared with the Audited Party prior to distribution to the Auditing Party such that the Audited Party can provide the independent certified accountant with justifying remarks for inclusion in the report prior to sharing the conclusions of such independent public audit with the Auditing Party. The final audit report will be shared with the Audited and Auditing Parties at the same time and specify whether the amounts audited were correct or, if incorrect, the amount of any underpayment or overpayment. In the event that there has been an underpayment by Crucell or an overstatement of costs by BN of more than [***] percent ([***]%) then the Audited Party shall reimburse the Auditing Party’s costs of such audit.

The party to whom such payment is due will issue an invoice for the corresponding amount, payable within [***] of its receipt of the invoice.

12.9 Audit Under NIH License. BN recognizes and agrees that, pursuant to Sections 8.01 and 8.02 of the NIH License (and as is set out in Annex I), the licensor of the NIH License shall have the right to

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

inspect the books and records set forth in Section 12.8 of BN and, in the event of an underreporting or underpayment, then BN shall insure that any monies owed therefor is paid to Crucell within [***] of BN being informed that such monies are owed.

Article 13 Publications and Press Releases

13.1 Review of Publication. As soon as is practicable, and prior to any disclosure (in whatever form or format, whether in writing or orally), or submission to any Third Party for publication of a manuscript, describing or containing scientific data resulting from any work accomplished as part of the Development Program (a “Publication”), BN and its Affiliates or Crucell and its Affiliates, as the case may be, shall disclose to each Party the intended Publication, and shall allow each Party at least [***] to determine whether such Publication contains subject matter for which patent protection should be sought prior to publication or which the other believes should be modified to avoid necessary regulatory or commercial difficulties or disclosure of that Party’s confidential information. With respect to publications by investigators or other Third Parties, such publications shall be subject to review by the Operations Committee under this Section.

13.2 Publication Rights. After the expiration of [***] from the date of receipt of such Publication by the members of the Operations Committee under Section 13.1, unless BN or Crucell or their Affiliates has received the written Notice specified in 13.3, the authoring Party shall be free to submit or disclose such Publication in any manner consistent with academic standards.

13.3 Delay of Publication. Prior to the expiration of the [***] period specified in Section 13.1, the Operations Committee may Notify the submitting Party of its determination that such Publication contains objectionable material, material that negatively impacts a Party’s business interest, discloses confidential information of that Party, or material that consists of patentable subject matter for which patent protection should be sought. The notified Party shall withhold its proposed Publication and confer with the Operations Committee to determine the best course of action to take in order to modify or delay the Publication. After resolution of the regulatory or commercial issues, or either the filing of a patent application or removal from the proposed publication of the patentable subject matter or confidential information, the submitting Party shall be free to submit or disclose the Publication. The submitting Party shall not be obliged to delay publication by more than [***] from the date of request by the non-publishing Party.

13.4 Publicity and Press Releases. If either Party wishes to issue a press release with respect to this Agreement, it will provide a draft of such press release, which shall be brief and factual, to the other Party prior to its release and allow a reasonable time for the other Party’s review and consent. Either Party may make subsequent public disclosure of the same contents of such press release. Each Party agrees not to issue any other press release or other public statement, whether oral or written, disclosing the terms hereof or any information relation to this Agreement without the prior written consent of the other Party. Notwithstanding the above, each Party acknowledges that the other Party is listed on a public stock exchange, and each Party therefore accepts and agrees that the other Party shall be free to release any such company announcements as reasonably necessary to ensure compliance with Applicable Law and

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

stock exchange regulation without such prior written consent but, in such an event, the Party making such disclosure will use reasonable efforts to minimalize such disclosure .

13.5 Use of Name. Neither Party shall use the name of the other Party or its Affiliates or any of their employees in any publications, publicity, promotional materials or advertising, without the prior specific written permission of the other Party.

Article 14 Confidentiality

14.1 Confidentiality Obligations. During the Term of this Agreement and for a period of [***] thereafter, each Party and its Affiliates shall maintain in confidence all Confidential Information disclosed by the other Party (the “Discloser”) which is identified as confidential including without limitations information relating to the Discloser’s Know-How, and shall not, except as permitted by this Agreement, use such Confidential Information or disclose the same to anyone other than those of its agents, direct employees, consultants and investigators for the execution of the Development Program, Commercialization or as otherwise is necessary in connection with such receiving Party’s (the “Recipient”) activities as contemplated, responsibilities and obligations as set forth in this Agreement, provided, however, that, except for disclosures to governmental health regulatory authorities, any disclosure by the Party’s direct employees, consultants and investigators or agents for the execution of the Development Program or Commercialization, shall require prior review and approval for disclosure. Each Party shall obtain a written agreement prior to disclosure to such agents, direct employees, consultants or investigators containing obligations to hold in confidence and not make use of such Confidential Information Confidential Information for any purposes other than as permitted by this Agreement, which obligations will not be less stringent than the obligations in this Section.

14.2 Diligence. Each Recipient shall use similar efforts to that which it uses to protect its own trade secrets or proprietary information, but, in any event, not less than Commercially Reasonable Efforts to ensure that its agents, direct employees, consultants and investigators for the execution of the Development Program and Commercialization or otherwise do not disclose or make any unauthorized use of such Confidential Information. Each Party shall notify the other without undue delay of its knowledge of any unauthorized use or disclosure of the other’s Confidential Information.

14.3 Exceptions to Confidentiality. The confidentiality obligations under this Agreement shall not apply to the extent that:

(a) the Recipient is required to disclose information by order or regulation of a governmental agency or court of competent jurisdiction or by applicable stock exchange rules and regulations, or Recipient can demonstrate that;

(b) the disclosed Confidential Information was at the time of such disclosure by Recipient already in the public domain other than as a result of actions of Recipient, its Affiliates and its agents, direct employees, consultants or investigators, in violation hereof;

(c) the disclosed Confidential Information was rightly known by Recipient (as shown by its written records) and not subject to obligations of confidentiality to the Discloser prior to the date of disclosure to Recipient in connection with the Agreement;

(d) the disclosed Confidential Information was independently developed without regard to the Confidential Information (as shown by its written records); or

(e) The disclosed Confidential Information was received by Recipient (as shown by its written records) on an unrestricted basis from a source unrelated to any Party to this Agreement and not under a duty of confidentiality to the other Party.

14.4 Permitted Disclosures. Each Party hereto may disclose another’s Confidential Information to the extent such disclosure is necessary in complying with applicable governmental regulations or otherwise submitting information to either Tax or other governmental authorities, provided that if a Party is required to make any such disclosure of another Party’s confidential information, other than under the terms of an appropriate confidentiality agreement, it will give reasonable advance Notice to the latter Party of such disclosure. Notwithstanding the foregoing, neither Party shall disclose to Third Parties, clinical data or Regulatory Filings received from the other Party.

14.5 Disclosures under NIH License. The Parties agree that Crucell will send a fully-executed copy of this Agreement to the licensor of the NIH License.

14.6 Neither Party shall include Confidential Information belonging to the other Party in any proposal to the US government to which FAR clause 52.227-23 will apply without the prior written consent of the other Party.

Article 15 Representations and Warranties

15.1 Mutual Representations and Warranties. Each Party represents and warrants to the other that: (a) it has the full right and authority to enter into this Agreement and grant the rights and licenses granted herein; (b) it has not previously granted and will not grant any rights in conflict with the rights and licenses granted herein; (c) there are no existing or threatened actions, suits or Claims pending against it with respect to their respective Patent Rights, Know-How and Program Materials or their right to enter into and perform its obligations under this Agreement; and (d) it has not previously granted, and will not grant during the term of this Agreement, any right, license or interest in or to its Patent Rights, Know-How and Program Materials licensed hereunder, or any portion thereof, to manufacture, sell or use a product that is in conflict with the rights or licenses granted under this Agreement.

15.2 Disclaimer of Warranties. Each Party specifically disclaims any guarantee that the Development Program or Commercialization will be successful, in whole or in part. To the extent that BN and Crucell have complied with their obligations under this Agreement, the failure of the Parties to successfully develop a Licensed Product will not constitute a breach of any representation or warranty or other obligation under this Agreement. Neither BN nor Crucell makes any representation or warranty or guaranty that the Development Program will be successful. BN AND CRUCELL EXPRESSLY DISCLAIM ANY WARRANTIES OR CONDITIONS, EXPRESS, IMPLIED, STATUTORY OR OTHERWISE, WITH RESPECT TO THE DEVELOPMENT PROGRAM AND THE CRUCELL INTELLECTUAL PROPERTY AND THE BN INTELLECTUAL PROPERTY AND THE CRUCELL MATERIALS AND BN MATERIALS, INCLUDING, WITHOUT LIMITATION, ANY WARRANTY OF MERCHANTABILITY, NONINFRINGEMENT, OR FITNESS FOR A PARTICULAR PURPOSE,

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

VALIDITY OF INTELLECTUAL PROPERTY, PATENTED OR UNPATENTED, AND NONINFRINGEMENT OF THE INTELLECTUAL PROPERTY RIGHTS OF THIRD PARTIES.

15.3 Effect of Representations and Warranties. It is understood that if the representations and warranties under this Section are not true and accurate and BN or Crucell incurs liabilities, costs or other expenses as a result of such falsity, BN or Crucell, as the case may be, shall indemnify, defend and hold the other Party harmless from and against any such liabilities, costs or expenses incurred, provided that the indemnifying Party receives Notice without undue delay of any Claim against BN or Crucell, as the case maybe, resulting from or related to such falsity, the cooperation of the indemnified Party, as requested in connection with any such Claim, and the sole right to control the defense or settlement thereof

15.4 Representations and Warranties of Crucell. Crucell represents and warrants that:

(a) it shall not use BN Technology or BN Patent Rights, directly or indirectly, otherwise than is provided for in the terms of the Supply Agreement and in this Agreement;

(b) to its knowledge, prior to the Effective Date, Crucell has not received any written notification that the Crucell Technology transferred hereunder infringes any rights of any Third Parties; and

(c) that it Controls the right to grant all the rights that it is granting herein.

15.5 Representations and Warranties of BN. BN represents and warrants that:

(a) it shall not use Crucell Technology or Crucell Patent Rights, directly or indirectly, otherwise than is provided for in the terms of this Agreement and the Supply Agreement;

(b) to its knowledge, prior to the Effective Date, BN has not received any written notification that the BN Technology infringes any rights of any Third Parties; and

(c) that it Controls the right to grant all the rights that it is granting herein.

Article 16 Indemnification, Liability and Insurance

16.1 By BN. Except for the willful misconduct or negligence of Crucell, Crucell shall not be liable for and BN shall indemnify and hold Crucell, its officers, directors, employees and agents (“Crucell Indemnitee”) [***], arising in [***].

16.2 By Crucell. BN shall not be liable for and Crucell shall indemnify and hold BN, its officers, directors, employees and agents (“BN Indemnitee”) [***], arising in [***] provided however that [***]

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

[***].

16.3 Procedure. A Party (the “Indemnitee”) that intends to claim indemnification under this Section shall without undue delay Notify the other Party (the “Indemnitor”) in writing of any loss, Claim, damage, liability or action in respect of which the Indemnitee or any of its Affiliates (in the case of BN, its Registered Affiliates), Sublicensees or their directors, officers, employees or agents intend to claim such indemnification, and the Indemnitor shall have the right to participate in, and, to the extent the Indemnitor so desires, to assume the defense thereof with counsel mutually satisfactory to the Parties; provided, however, that Indemnitee shall have the right to retain its own counsel, with the fees and expenses to be paid by the Indemnitor, if representation of such Indemnitee by the counsel retained by the Indemnitor would be inappropriate due to actual or potential differing interests between such Indemnitee and any other Party represented by such counsel in such proceeding. The indemnity agreement in this Section shall not apply to amounts paid in settlement of any loss, Claim, damage, liability, or action if such settlement is effected without the consent of the Indemnitor, which consent shall not be withheld unreasonably. The failure to deliver written Notice to the Indemnitor within a reasonable time after the commencement of any such action, if prejudicial to its ability to defend such action, shall relieve such Indemnitor of any liability to the Indemnitee under this Section but the omission so to deliver written Notice to the Indemnitor shall not relieve it of any liability that it may have to any Indemnitee otherwise than under this Section. The Indemnitee under this Section, its employees and agents, shall cooperate fully with the Indemnitor and its legal representatives in the investigation of any action, Claim or liability covered by this indemnification.

16.4 Insurance. Each Party shall, at its own cost and expense, obtain and maintain in full force and effect during the Term the following: (i) Commercial General Liability Insurance (including any self-insured arrangements) with a limit of not less than $[***] per occurrence and $[***] annual aggregate; (ii) Products Liability Insurance (including any self-insured arrangements) with a per-occurrence limit of not less than $[***] and $[***] annual aggregate; and (iii) where required by law, each Party responsible for sponsoring clinical trials shall obtain and maintain Clinical Trial Insurance (including any self-insured arrangements) in full compliance with the legal requirements of the jurisdiction in which the clinical trial will be conducted. If any of the required policies of insurance are written on a Claims made basis, such policies shall be maintained throughout the Term and for a period of at least 3 years thereafter. Upon the other Party’s written request from time to time, each Party shall without undue delay furnish to the other Party a certificate of insurance or other evidence of the required insurance.

16.5 Special, Indirect and Other Losses. NEITHER PARTY NOR ANY OF ITS AFFILIATES SHALL BE LIABLE IN CONTRACT, TORT, NEGLIGENCE, BREACH OF STATUTORY DUTY OR OTHERWISE FOR ANY CONSEQUENTIAL, SPECIAL OR PUNITIVE DAMAGES OR FOR LOSS OF PROFITS SUFFERED BY THE OTHER PARTY, EXCEPT TO THE EXTENT ANY SUCH DAMAGES ARE REQUIRED TO BE PAID TO A THIRD PARTY AS PART OF A CLAIM FOR WHICH A PARTY PROVIDES INDEMNIFICATION UNDER THIS ARTICLE 16.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Article 17 Term and Termination

17.1 Term. The term of this Agreement shall be that period starting on the Effective Date and shall expire on the expiry of the Royalty Term for the last of the Licensed Products (the “Term”), unless this Agreement is otherwise terminated early as provided for herein.

17.2 Termination for Cause. Either Party to this Agreement may terminate this Agreement in the event the other Party shall have materially breached or defaulted in the performance of any of its material obligations hereunder, and such default shall have continued for [***] after written Notice thereof was provided to the breaching Party by the non-breaching Party (the “Cure Period”). Any termination shall become effective at the end of such [***] Cure Period unless the breaching Party (or any other Party on its behalf) has cured any such breach or default prior to the expiration of the [***] Cure Period.

17.3 Termination for Convenience. During Development and Commercialization, Crucell shall have the right to terminate this Agreement at any time with a [***] written Notice. Such Notice period commences upon BN’s receipt of the written Notice of termination.

17.4 Termination Upon Insolvency or Bankruptcy. If either Party is going to file for insolvency or is served notice that a Third Party is intending to or has filed for insolvency the affected Party shall promptly Notify the other Party. It is intended by the Parties that, subject to this Section 17.4, the licenses granted herein shall survive any insolvency of the Parties. Notwithstanding the foregoing, on the insolvency of a Party, the non-insolvent Party shall have the option by written Notice to immediately terminate this Agreement.

17.5 In the event of a Change of Control of BN prior to the first anniversary of the Effective Date or at any time if the acquirer is a Competitor then, at the election of Crucell, this Agreement shall terminate. In the event that Crucell does not elect to terminate this Agreement, then Crucell may elect (CoC Option) to terminate all Sections of this Agreement other than 5.5, 9.2, 9.3, 11.2, 11.5, 11.6, 11.7, 11.8, 11.9, 12, 14, 16 and 18 and the licenses granted in Section 9.2 shall be extended to include the right for Crucell to Manufacture a Multivalent MVA Vector, the Multivalent MVA-BN Vector and a Monovalent MVA Vector.

17.6 Rights and Obligations on Termination.

(a) Termination by either Party pursuant to this Article shall not prejudice any other remedy that a Party might have. Termination of this Agreement for any reason shall not release any Party hereto from any liability which, at the time of such termination, has already accrued to the other Party or which is attributable to a period prior to such termination nor preclude either Party from pursuing all rights and remedies it may have hereunder or at law or in equity with respect to any breach of this Agreement.

(b) Upon termination or expiration of this Agreement or by Crucell exercising either of its rights under Section 17.5 by either Party for any reason, at Crucell’s written request and option, BN and its Affiliates shall either: (i) destroy all Crucell Materials they have (Derivatives thereof) and destroy all documents containing Crucell Know How; or (ii) deliver and/or return to Crucell such Crucell Materials and Crucell Know How.

(c) Upon termination of this Agreement by either Party for any reason, at BN’s written request and option, Crucell and its Affiliates shall either: (i) destroy all BN Materials they have (Derivatives thereof) and destroy all documents containing BN Know How; or (ii) deliver and/or return to BN such BN Materials and BN Know How.

(d) In the event that this Agreement is terminated for any reason other than expiration of the Royalty Term, then all licenses granted by either Party hereunder shall immediately terminate with the sole exception of the license granted under Section 9.3, and then BN will be free to conclude licenses with any other entity concerning a Multivalent MVA Vector, the Multivalent MVA-BN Vector and a Monovalent MVA Vector. The foregoing shall not apply to licenses granted to Crucell (which licenses to Crucell shall continue pursuant to the continuing provisions of this Agreement under Section 17.5) if Crucell exercises its CoC Option pursuant to Section 17.5.

(e) Upon any termination of this Agreement by one or both Parties for any reason, both Parties shall without undue delay return to the other all Confidential Information including Technology received from the other (except one copy of which may be retained for archival purposes), except that a Party shall not be required to return Confidential Information including Technology to the other for which it has been granted rights under this Agreement that continues after termination . The foregoing shall not apply to the Confidential Information received from BN (which Crucell is entitled to retain pursuant to the continuing provisions of this Agreement under Section 17.5) if Crucell exercises its CoC Option pursuant to Section 17.5.

(f) On the expiry of this Agreement pursuant to Section 17.1, all of the licenses granted hereunder become non-exclusive and royalty free and the Parties shall not be required to return Confidential Information to each other if this Agreement has expired in accordance with Article 17.1 and such information is required to continue the development of, or marketing of, Licensed Products.

(g) Termination for Convenience. Upon termination of this Agreement for convenience pursuant to Section 17.3, and in the absence of an uncured material breach by BN, then no further payments from Crucell, other than outstanding amounts due to BN, shall be due and all licenses granted by either Party hereunder shall immediately terminate and this Agreement shall terminate without penalty to either Party.

(h) For the sake of clarity, in the event of a termination or expiry of the licenses granted to Crucell under this Agreement for any reason, then BN will be free to conclude licenses with any other entity concerning a Multivalent MVA Vector, the Multivalent MVA-BN Vector and a Monovalent MVA Vector. For the sake of clarity, in the event of a termination or expiry of the licenses granted to Crucell under this Agreement for any reason, then Crucell will be free to conclude licenses with any other entity concerning a Monovalent Ad26 ZEBOV Vector, a Monovalent Adenovirus Vector, a Multivalent Adenovirus Vector and/or any Multivalent Ad26 Vector

(i) Stock on Hand. In the event this Agreement is terminated for any reason, the terminated Party and, in the case of Crucell, its Affiliates and Sublicensees shall have the right to sell or otherwise dispose of the stock of any Licensed Product subject to this Agreement then on hand, subject to the payment of royalties as provided herein.

17.6 Termination of NIH License.

(a) Basis for Termination. BN understands and agrees that the NIH License may be terminated by either Crucell or by the licensor of the NIH License for a variety of reasons as set forth therein and in particular in Article 13, such reasons including breach, for convenience, insolvency and those reasons set forth in Sections 13.06-13.08 of Annex I.

(b) Consequences. In the event that the NIH License is terminated (pursuant to Article 13 of the NIH License), then the licenses granted hereunder to the Patent Rights listed in Part 1 and Part 2 of Annex C shall, at the option of BN, either:

(1) terminate; or

(2) be converted into a license directly between BN and the licensor of the NIH License. Such conversion is subject to the approval of the licensor of the NIH License, which shall not be unreasonably withheld and is contingent upon acceptance by BN of the remaining provisions of the NIH License.

17.7 Survival. In addition to any clause expressed to survive expiration or termination, insofar as applicable, Sections 10.1through 10.6, 10.8(c), 12, 13, 14, 15.2, 17 and 18 of this Agreement shall survive expiration or termination of this Agreement for any reason.

Article 18 Miscellaneous

18.1 Entire Agreement. This Agreement contains the entire agreement of the Parties regarding the subject matter hereof and supersedes all prior agreements, understandings, and negotiations regarding the same. This Agreement may not be changed, modified, amended, or supplemented except by a written instrument signed by both Parties hereto.

18.2 Assignment. Neither Crucell nor BN may assign this Agreement to another party. Notwithstanding the foregoing, Crucell may without BN’s consent assign any or all of its rights and obligations hereunder to any Affiliate, and BN may without consent from Crucell assign this Agreement to any Affiliate. Both Parties may assign this Agreement to a successor in title or to a Third Party company acquiring direct or indirect control of substantially all of its business related to this Agreement and such assignment shall then be binding upon, and inure to the benefit of, both Parties. The foregoing notwithstanding, the Parties understand and agree that all such assignments on the part of Crucell will be subject to approval of the licensor of the NIH License.

18.3 Severability. If any part of this Agreement shall be held invalid and/or unenforceable, the remainder of the Agreement shall nevertheless remain in full force and effect.

18.4 Further Assurances. Each Party hereto agrees to execute, acknowledge and/or deliver such further instruments, and to do all other acts, as may be necessary or appropriate in order to carry out the purposes and intent of this Agreement.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

18.5 Force Majeure. Neither BN nor Crucell shall be liable for any failure or delay in performance under this Agreement which is due in whole or in part directly or indirectly to any cause of any nature beyond the reasonable control of such Party. In the event that any such force majeure cause/situation has lasted in total for more than [***], the Party not affected by such force majeure shall have the right to terminate this Agreement.

18.6 Notices and Reports. All notices and reports required by this Agreement shall be in writing and in the English language (“Notices”). All notices and reports shall be sent by fax followed by registered airmail to the Parties at the following addresses or such other addresses as may be designated in writing by the respective Parties:

To Crucell: Crucell Holland B.V.

Archimedesweg 4,

2333 CN Leiden

The Netherlands

Attn. Business Development

With a copy to: Office of the General Counsel
Johnson & Johnson
One Johnson & Johnson Plaza
New Brunswick, NJ 08933
United States of America
Attn: General Counsel

To BN: Bavarian Nordic AS
Hejreskovvej 10A
3490 Kvistgaard
Denmark
Attn. President and CEO

Any notices shall be deemed given when received by the other Party.

18.7 Expenses. Each Party shall bear its own expenses, if not expressly agreed otherwise in this Agreement.

18.8 Relationships of the Parties. Both Parties are independent contractors under this Agreement. Nothing contained in this Agreement is intended nor is to be construed so as to constitute Crucell and BN as partners or joint ventures with respect to this Agreement. Neither Party hereto shall have any express or implied right or authority to assume or create any obligations on behalf of or in the name of the other Party or to bind the other Party to any other contract, agreement, or undertaking with any Third Party.

18.9 Export Laws. Notwithstanding anything to the contrary contained herein, all obligations of BN and Crucell are, to the extent applicable, subject to compliance with United States export regulations and such other United States laws and regulations as may be applicable, and to obtaining all necessary approvals required by the applicable agencies of the government of the United States. BN and Crucell

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

shall cooperate with each other and shall provide assistance to the other as reasonably necessary to obtain any required approvals.

18.10 Waiver. The waiver by either Party of a breach of any provisions contained herein shall be in writing and shall in no way be construed as a waiver of any succeeding breach of such provision or the waiver of the provision itself.

18.11 Choice of Law. This Agreement shall be construed and interpreted according to the laws of Denmark without reference to conflicts of laws principles and to the exclusion of any rule that would refer the subject matter to another forum. The English version of this Agreement shall, in case of conflicts between translations, govern.

18.12 Dispute Resolution. The Parties shall, in good faith, attempt to amicably resolve any disputes arising under this agreement first via mediation according to the ADR rules of the International Chamber of Commerce (ICC), and, failing mediation within four (4) weeks of a request for mediation has been made, via binding arbitration according to the rules of the ICC. The arbitral tribunal shall consist of three (3) arbitrators. If a Party does not appoint its arbitrator within [***] following the expiry of the allotted period, then such arbitrator shall be selected in accordance with the ICC Rules. The arbitrators may permit limited discovery as they deem appropriate in the circumstances of the dispute. The arbitration shall be conducted in the Hague, the Netherlands, and all documents submitted to the arbitrators shall be, in English. The arbitrators shall have no power to award punitive, special, incidental or consequential damages. The arbitrator’s decision and award shall be final and binding upon all Parties. Unless otherwise determined by the arbitrators, each Party shall bear its own costs for its counsel and other expenses, and the Parties shall equally share the costs of the arbitration. Judgment upon the award rendered by arbitration may be issued and enforced by any court having competent jurisdiction. This Section 18.13 shall not prevent the Parties, in order to protect its rights, from unilaterally seeking interim injunction or other forms of preliminary relief before the competent courts of a concerned jurisdiction and in accordance with the laws of said court.

Disputes concerning the NIH License and/or payments due thereunder shall be subject to the Section 14.12 of the NIH License if one of the parties to the dispute is the licensor of the NIH License or if the issue concerns an obligation or duty owned to the licensor of the NIH License.

18.13 Anti-Corruption Laws. Neither party shall perform any actions that are prohibited by local and other anti-corruption laws (collectively “Anti-Corruption Laws”) that may be applicable to one or both Parties to the Agreement. Without limiting the foregoing, neither party shall make any payments, or offer or transfer anything of value, to any government official or government employee, to any political party official or candidate for political office or to any other Third Party related to the transaction in a manner that would violate Anti-Corruption Laws.

18.14 Captions. Paragraph captions are inserted for convenience only and in no way are to be construed to define, limit or affect the construction or interpretation hereof.

IN WITNESS WHEREOF, the Parties intending to be bound have caused this Agreement to be executed by their duly authorized representatives, as follows:

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

In witness whereof, the Parties have executed this subscription agreement in counterparts on 22 October 2014.

For and on behalf of
Bavarian Nordic A/S

By:			By:	[***]

Name:		[***]	Name:		[***]
Title:		Chairman of the Board of Directors	Title:		President, CEO

By:	[***]

Name:		[***]
Title:		Executive Vice President, CFO


For and on behalf of
Johnson & Johnson Development Corporation

By:

Name:		[***]
Title:		Vice President

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

On 22 October 2014,

For Bavarian Nordic A/S:


[***]				[***]
Name:	[***]			Name:	[***]
Capacity:		Chairman of the Board of Directors		Capacity:		President, CEO


[***]

Name:	[***]
Capacity:			Executive Vice President, CFO


For Crucell Holland B.V.:


Name:				Name:
Capacity:				Capacity:

AMENDMENT NO. 1 TO COLLABORATION
AND LICENSE AGREEMENT

This Amendment No. 1 to the Collaboration and License Agreement is made and effective as of February 12, 2015 by and between Crucell Holland B.V. (“Crucell”) and Bavarian Nordic A/S (“BN”).

Recitals

Whereas Crucell and BN entered into that certain Collaboration and License Agreement effective as of October 22, 2014 (the “Agreement”); and

Whereas Crucell and BN desire to further amend the Agreement on the terms and conditions set forth below in accordance with Section 18.1 of the Agreement

NOW THEREFORE, for and in consideration of the mutual covenants contained herein, Crucell and BN hereby agree as follows:

1. Definitions and Cross References. Unless otherwise specified herein, each capitalized term shall have the meaning assigned to it in the Agreement and each reference to a Section or Article shall refer to the corresponding Section or Article in the Agreement.

2. Section 3.1 (c) under (3). Section 3.1 (c) under (3) shall be amended to read as follows: “if the matter involves Development activities funded unilaterally by Crucell, or involves Development activities funded either directly or indirectly (e.g. through an “in-kind matching” funding structure) by funding bodies or mechanisms of the European Union (such as IMI) or of the US Government (including NIH and BARDA), or the matter involves Commercialization, then subject to 3.1 (d) below, Crucell shall have the final decision-making authority relative thereto. For the avoidance of doubt, this right shall not reduce Crucell’s obligations to use Commercially Reasonable Efforts to Develop and Commercialize Licensed Products. For clarity, this clause derogates from Section 3.1 (c) under (1); if the matter involves Development activities funded by a party other than Crucell, which party is not a funding body or mechanism of the European Union or the US Government, Section 3.1 (c) under (1) shall apply, unless the Parties agree otherwise by amendment of this Agreement”.

3. Section 4.8 (d). The following shall be added to the end of section 4.8(d):

“In case of a conflict between this Agreement and the grant agreement and/or consortium agreement for the EBOVAC, EBOMAN and EBODAC projects within the Ebola+ IMI program (an “IMI Agreement”) for matters related to intellectual property access rights (to the extent that the intellectual property access rights for EBOVAC and EBODAC provide no further access rights than those provided in EBOMAN), governance of (pre-) clinical trials (provided Crucell shares the relevant development plan or clinical trial protocol with Bavarian Nordic within a reasonable timeframe), such IMI Agreement will prevail.”

Exhibit 10.10

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

OPTION AND LICENSE AGREEMENT

THIS OPTION AND LICENSE AGREEMENT (the “Agreement”) is made and entered into effective as of 03 March, 2015 (the “Effective Date”) by and among BAVARIAN NORDIC A/S, a Danish corporation having its principal place of business at Hejreskovvej 10A, DK-3490 Kvistgaard, Denmark (“BN”) and BAVARIAN NORDIC INC., BN’s wholly owned subsidiary, which is a Delaware corporation having its principal place of business at 2425 Garcia Avenue, Mountain View, CA 94043, USA (“BNInc”), on the one hand, and BRISTOL-MYERS SQUIBB COMPANY, a Delaware corporation headquartered at 345 Park Avenue, New York, New York 10154 USA (“BMS”), on the other hand. BN and BMS are sometimes referred to herein individually as a “Party” and collectively as the “Parties”. BNInc shall be considered a “Party” and one of the “Parties”, in each case jointly with BN, only with respect to the BNInc Provisions and shall have no other rights, obligations or liabilities under this Agreement other than as set out in the BNInc Provisions.

RECITALS

Whereas, BMS is a biopharmaceutical company engaged in the research, development, manufacture and commercialization of human therapeutic products.

Whereas, BN is a biotechnology company engaged in the development and manufacture of novel cancer immunotherapies. BN owns a subsidiary, BNInc, which develops novel cancer immunotherapies.

Whereas, BN is conducting a Phase 3 human clinical trial with respect to its proprietary targeted immunotherapy candidate, PROSTVAC®, for the treatment of prostate cancer.

Whereas, BMS and BN desire to enter into an agreement regarding the continued development of PROSTVAC and granting BMS an option to obtain exclusive rights to PROSTVAC, all in accordance with the terms and conditions set forth herein below.

Now Therefore, in consideration of the foregoing premises and the mutual promises, covenants and conditions contained in this Agreement, the Parties agree as follows.

1. DEFINITIONS

As used in this Agreement, the terms with initial letters capitalized, whether used in the singular or plural form, shall have the meanings set forth in this Article 1 or, if not listed below, the meaning designated in places throughout this Agreement.

1.1 “Accounting Standards” means, with respect to BMS, GAAP, and, with respect to BN, IFRS, in each case, as generally and consistently applied for accounting and financial reporting purposes throughout the Party’s organization. Each Party may change the accounting standards that it uses throughout such Party’s organization, in which case such Party shall promptly notify the other Party in writing of such change and “Accounting Standards” shall be modified as to such Party accordingly, it being understood that each Party may only use internationally recognized accounting principles (e.g., GAAP, IFRS, or successor standards thereto).

1.2 “Acquirer” is defined in Section 16.8.

1.3 “Adverse Event” means any untoward medical occurrence in a patient or human clinical investigation subject that is administered any Product, including occurrences which do not necessarily have a causal relationship with any Product.

1.4 “Affiliate” means, with respect to a particular Party, a person, corporation, partnership, or other entity that controls, is controlled by or is under common control with such Party. For the purposes of this definition, the word “control” (including, with correlative meaning, the terms “controlled by” or “under the common control with”) means the actual power, either directly or indirectly through one or more intermediaries, to direct or cause the direction of the management and policies of such entity, whether by the ownership of more than fifty percent (50%) of the voting stock of such entity, or by contract or otherwise.

1.5 “Alliance Manager” is defined in Section 3.2.

1.6 “Applicable Law” means any applicable federal, state, local or foreign law, statute, ordinance, principle of common law, or any rule, regulation, standard, judgment, order, writ, injunction, decree, arbitration award, agency requirement, license (other than a license granted under an Existing Product Agreement) or permit of any Governmental Authority.

1.7 “Approval in the European Union” means MAA approval by EMA and receipt of pricing and reimbursement approvals acceptable to BMS with respect to a Product in at least Germany, France and one of the other Major European Countries.

1.8 “Bankruptcy Event” is defined in Section 16.3(a).

1.9 “Biosimilar Product” means, with respect to a particular Product in a country, a biopharmaceutical product that: (a) contains clinically comparable or interchangeable active ingredients as such Product; (b) is approved for use in such country pursuant to a regulatory approval process governing approval of generic, interchangeable or biosimilar biologics, where such approval is obtained using an approval process (i) undertaken without the consent or assistance of BMS (excluding rights granted with BN’s consent in connection with settlement or resolution of patent infringement or other challenges pursuant to Article 9) and (ii) based upon clinical data generated by or on behalf of BMS or BN or any of their respective Affiliates and consent to use such data was not given by BMS; and (c) is sold in the same country as such Product by any Third Party that is not a Sublicensee of BMS or its Affiliates.

1.10 “BLA” means a Biologics License Application, for which Regulatory Approval by the FDA is required to market a Product in the U.S.

1.11 “BLA Approval” means, with respect to a Product, receipt of Regulatory Approval of a BLA by the FDA for such Product in the U.S.

1.12 “BMS Claims” is defined in Section 14.1.

1.13 “BMS Damages” is defined in Section 14.1.

1.14 “BMS Indemnitees” is defined in Section 14.1.

1.15 “BN Claims” is defined in Section 14.2.

1.16 “BN Damages” is defined in Section 14.2.

1.17 “BN Diagnostic Technology” means all Know-How, tangible materials (including documents) and Patents, each to the extent it is (a) Controlled as of the Effective Date or thereafter during the Term by BN and/or its Affiliate(s) and (b) is necessary or reasonably useful for the Development, manufacture, use and/or Commercialization of Companion Diagnostics.

1.18 “BN Indemnitees” is defined in Section 14.2.

1.19 “BNInc Agreement” means the License Agreement, dated as of December 31, 2011, by and between BN and BNInc, as may be amended from time to time as permitted by this Agreement.

1.20 “BNInc Provisions” means Section 13.8 and, solely as they relate to Section 13.8, Article 1 and Sections 16.1, 16.3, 16.5, 16.6, 16.9, 16.12, 16.14, 16.15, 16.16 and 16.17.

1.21 “BN Know-How” means all Know-How to the extent that it is Controlled as of the Effective Date or thereafter during the Term by BN and/or its Affiliate(s) and that is necessary or reasonably useful for the Development, manufacture, use and/or Commercialization of Products in the Field and that is Confidential Information at the time of its use. BN Know-How includes, to the extent that the same is Controlled by BN, all chemical, structural, biological, pharmacological, toxicological, clinical, assay, structure activity relationship information or other information that relates to any Product (including its composition, formulation, or method of use, manufacture, preparation or administration). BN Know-How shall exclude rights under any BN Patents and BN’s interest in any Joint Patents and any inventions claimed therein. For clarity, subject to and to the extent as provided in Section 16.8, the use of “Affiliate” in this definition shall exclude any Acquirer of BN.

1.22 “BN Materials” means all tangible materials (including documents) in the possession of and to the extent that they are Controlled by BN and/or its Affiliate(s) as of the Effective Date or thereafter during the Term that are necessary or reasonably useful for the Development, manufacture, use and/or Commercialization of Products in the Field. For clarity, subject to and to the extent as provided in Section 16.8, the use of “Affiliate” in this definition shall exclude any Acquirer of BN.

1.23 “BN Patents” means all Patents to the extent that they are Controlled as of the Effective Date or thereafter during the Term by BN and/or its Affiliate(s) and that Cover any Product (including in each case its composition, formulation, combination, product by process, or method of use, manufacture, preparation or administration) or that would be necessary or reasonably useful for the Development, manufacture, use and/or Commercialization of Products in the Field. BN Patents shall include BN’s interest in Joint Patents, Product Specific Patents and Other BN Patents. For clarity, subject to and to the extent as provided in Section 16.8, the

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

use of “Affiliate” in this definition shall exclude any Acquirer of BN. As of the Effective Date, the BN Patents include the Product Specific Patents listed in Exhibit A1, and the Other BN Patents listed in Exhibit A2.

1.24 “BN Technology” means the BN Patents, BN Know-How and BN Materials.

1.25 “Business Day” means a day that is not a Saturday, Sunday or a day on which banking institutions in New York, New York and/or in Copenhagen, Denmark are required by Applicable Law to remain closed.

1.26 “Calendar Quarter” means each of the three (3) consecutive month periods ending on March 31, June 30, September 30 and December 31 of any Calendar Year; provided, that the first Calendar Quarter during the Term shall be the period of less than three (3) months commencing on the Effective Date and the last Calendar Quarter during the Term shall be the period of less than three (3) months ending on the termination date of this Agreement. “Quarterly” shall have the correlative meaning.

1.27 “Calendar Year” means each one (1) year period beginning on January 1 and ending on December 31.

1.28 “Claim” is defined in Section 14.4.

1.29 “Clinical Trial” means any human clinical trial of a Product.

1.30 “Combination Product” means a Product that includes at least one additional active ingredient (whether co-formulated or co-packaged) that is not PROSTVAC (and not GM-CSF where the Regulatory Approval of the Product includes the use of GM-CSF). Biopharmaceutical dosage form vehicles, adjuvants, and excipients shall not be deemed to be “active ingredients”, except in the case where such vehicle, adjuvant, or excipient is recognized by the FDA as an active ingredient in accordance with 21 C.F.R. 210.3(b)(7). For the avoidance of doubt, any GM-CSF which is sold by BMS for use with PROSTVAC shall be included as part of the Product for the purpose of calculating Net Sales and not as a component in a Combination Product.

1.31 “Commercialization and Development Plan” means the plan for the commercialization and further Development of the Product in the Major Markets by BMS after the License Effective Date in the format set out in Exhibit J, in any case in a manner consistent with BMS then-current practice, setting forth the anticipated Commercialization activities (including launch plans, product positioning, target prescribers, and detailing activities) and timelines for such activities. The Commercialization and Development Plan shall cover the activities that BMS plans to undertake in respect of the Commercialization and Development of Products pursuant to this Agreement over the [***] following issuance thereof.

1.32 “Commercialization Wind-Down Period” is defined in Section 12.7(b).

1.33 “Commercialize” or “Commercialization” means the marketing, promotion, sale (and offer for sale or contract to sell), distribution, importation or other commercial

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

exploitation of, including pricing and reimbursement activities for, a Product or Companion Diagnostic in the Territory. Commercialization shall include commercial activities conducted in preparation for Product or Companion Diagnostic launch.

1.34 “Companion Diagnostic” means a product (a) for the identification of a patient’s suitability for treatment with a Product; (b) for uses connected with the prognosis of a patient with prostatic disease who is treated with a Product; or (c) to monitor the biologic effect or response of the patient to the Product.

1.35 “Competing Product” is defined in Section 10.1.

1.36 “Confidential Information” means, with respect to a Party, all non-public Information of such Party or its Affiliates that is disclosed to the other Party under this Agreement, which may include unpublished patent applications, whether disclosed in oral, written, graphic, or electronic form. All Information disclosed by a Party pursuant to the Prior CDA shall be deemed to be the Confidential Information of such Party pursuant to this Agreement (with the mutual understanding and agreement that any use or disclosure thereof that is authorized under Article 11 shall not be restricted by, or be deemed a violation of, such Prior CDA).

1.37 “Control” means, with respect to any material, Information, or intellectual property right, that a Party (a) owns such material, Information, or intellectual property right, or (b) has a license or right to use to such material, Information, or intellectual property right, in each case (a) or (b) with the ability to grant to the other Party access, a right to use, or a license, or a sublicense (as applicable) to such material, Information, or intellectual property right on the terms and conditions set forth herein, without (i) violating the terms of any agreement or other arrangement with any Third Party in existence as of the time such Party or its Affiliates would first be required hereunder to grant the other Party such access, right to use or (sub)license or (ii) paying any sums of money to any Third Party that assigned or licensed such Information and/or intellectual property right to such Party that become payable in connection with the other Party’s exploitation thereof hereunder unless (A) the other Party agrees in writing to pay any such sums, subject to Section 8.5(b)(ii), or (B) such sums are payable under any agreement in effect as of the Effective Date.

1.38 “Cover”, “Covered” or “Covering” means, with respect to a Product or invention and a Patent, that, in the absence of a (sub)license under, or ownership of, such Patent, the making, using, offering for sale, selling or importing of such Product, or the using of such invention, would infringe a Valid Claim of such Patent.

1.39 “CRO” means PPD Development, LP, the contract research organization that is conducting the PROSPECT Trial.

1.40 “CRO Agreement” means, collectively, (a) the Master Services Agreement by and between BNInc and CRO, dated as of [***], as amended as of the Effective Date and (b) the Project Addendum under the foregoing, dated as of [***], as amended as of the Effective Date.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.41 “Develop” or “Development” means all activities that relate to obtaining, maintaining or expanding Regulatory Approval of a Product or Companion Diagnostic and to supporting appropriate usage for such product, for one or more indications in the Field. This includes: (a) preclinical/nonclinical research and testing, toxicology, and Clinical Trials; and (b) preparation, submission, review, and development of data or Information and Regulatory Materials for the purpose of submission to a Governmental Authority to obtain, maintain and/or expand Regulatory Approval of a Product or Companion Diagnostic (including contacts with Regulatory Authorities), and outside counsel regulatory legal services related thereto; provided, however, that Development shall exclude Commercialization and manufacturing activities (including manufacturing activities related to Development).

1.42 “Diligent Efforts” means (a) with respect to BMS’s obligations under this Agreement to Develop or Commercialize a Product, the carrying out of such obligations or tasks with a level of effort and resources consistent with the commercially reasonable practices [***] for the research, development, manufacture or commercialization of a similar biopharmaceutical product owned by it (or to which it has exclusive rights) at a similar stage of development or commercialization and of similar market potential, profit potential and strategic value, based on conditions then prevailing, including issues of safety and efficacy, Regulatory Authority-approved labeling, product profile, the competitiveness of alternative products in the marketplace, pricing/reimbursement for the product in a country relative to other markets, the likely timing of the product’s entry into the relevant market in a country, the patent and other proprietary position, the likelihood of regulatory approval and other relevant scientific, technical and commercial factors and (b) with respect to BN’s obligations under this Agreement, the carrying out of such obligations or tasks with a level of effort and resources consistent with commercially reasonable practices normally [***] at such time.

1.43 “Disclosing Party” is defined in Section 11.1.

1.44 “DOJ” means the United States Department of Justice.

1.45 “Dollar” or “$” means the lawful currency of the United States.

1.46 “Effective Date” means the date specified in the initial paragraph of this Agreement.

1.47 “EMA” means the European Medicines Agency and any successor agency thereto.

1.48 “EU” or “European Union” means the European Union, as its membership may be constituted from time to time, and any successor thereto, and which, as of the Effective Date, consists of Austria, Belgium, Bulgaria, Czech Republic, Denmark, Estonia, Finland, France, Germany, Greece, Hungary, Ireland, Italy, Latvia, Lithuania, Luxembourg, Malta, The Netherlands, Poland, Portugal, Romania, Slovakia, Slovenia, Spain, Sweden and the United Kingdom, and that certain portion of Cyprus included in such organization.

1.49 “Exclusivity Period” is defined in Section 10.1.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.50 “Executive Officer” means (i) in the case of BMS, any senior executive who reports directly to the Chief Executive Officer of BMS, or who reports directly to a senior executive who reports directly to the Chief Executive Officer of BMS and (ii) in the case of BN, BN’s Chief Executive Officer.

1.51 “Existing Combination Product Patent” means, subject to Section 9.2(d)(i), the Product Specific Patent listed in section (I) of Exhibit A2 as of the Effective Date.

1.52 “Existing Product Agreement Licensor” means a Person granting rights to BN or any of its Affiliates with respect to BN Technology under an Existing Product Agreement.

1.53 “Existing Product Agreements” means the PHS License Agreement, the NIH CRADA, the BNInc Agreement and the CRO Agreement.

1.54 “Expert” means a mutually acceptable, disinterested, conflict-of-interest-free individual not affiliated with either Party or its Affiliates who, with respect to a dispute concerning a financial, legal, commercial, scientific or regulatory matter possesses appropriate expertise to resolve such dispute. The Expert (or any of the Expert’s former employers) shall not be or have been at any time during the previous [***] an Affiliate, employee, consultant, officer or director of either Party or any of its Affiliates or employed by a law firm engaged by either Party or its Affiliates.

1.55 “FD&C Act” or “Act” means the United States Federal Food, Drug and Cosmetic Act, as amended.

1.56 “FDA” means the United States Food and Drug Administration and any successor agency thereto.

1.57 “Field” means any and all indications and uses for the treatment and prevention of prostatic diseases (which includes prostate cancer), subject to the PHS License Agreement.

1.58 “First Commercial Sale” means, with respect to a Product in a country, the first sale to a Third Party of such Product in such country after Regulatory Approval has been obtained in such country.

1.59 “FTC” means the United States Federal Trade Commission.

1.60 “FTE” means the equivalent of the work of one appropriately qualified individual working on a full-time basis in performing work in connection with this Agreement for a [***] period (consisting of at least a total of [***] hours per year of dedicated effort). FTE efforts shall not include the work of general corporate or administrative personnel.

1.61 “FTE Rate” means, for the period from the Effective Date to 31 December 2015, [***] US dollars (US$[***]). Thereafter, the FTE Rate shall be increased or decreased on 1 January of each year by the annual percentage increase or decrease in the [***].

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.62 “GAAP” means U.S. generally accepted accounting principles.

1.63 “GM-CSF” means a granulocyte macrophage colony-stimulating factor.

1.64 “Governmental Authority” means any multi-national, federal, state, local, municipal or other government authority of any nature (including any governmental division, subdivision, department, agency, bureau, branch, office, commission, council, court, tribunal or other entity).

1.65 “Gross Negligence” means a Party’s act or omission committed with a reckless disregard of or indifference to an obvious risk to the rights and safety of others and is more fundamental than failure to exercise proper skill and/or care constituting simple negligence that results in damage to the other Party.

1.66 “HSR Act” means the Hart-Scott-Rodino Antitrust Improvements Act of 1976, as amended (15 U.S.C. Sec. 18a), and the rules and regulations promulgated thereunder.

1.67 “HSR Clearance” means either (a) early termination of the applicable waiting period under the HSR Act with respect to the HSR Filings or (b) expiration of the applicable waiting period under the HSR Act with respect to the HSR Filings.

1.68 “HSR Filings” means the filings by BN and BMS with the FTC and the Antitrust Division of the DOJ of a Notification and Report Form for Certain Mergers and Acquisitions (as that term is defined in the HSR Act) with respect to the matters set forth in this Agreement, together with all required documentary attachments thereto.

1.69 “ICH” means International Conference on Harmonization of Technical Requirements for Registration of Pharmaceuticals for Human Use.

1.70 “[***]” is defined in Section 6.3.

1.71 “IFRS” means International Financial Reporting Standards.

1.72 “IND” means (a) an Investigational New Drug Application as defined in the FD&C Act and applicable regulations promulgated thereunder by the FDA, or (b) the equivalent application to the applicable Regulatory Authority in any other regulatory jurisdiction, the filing of which is necessary to initiate or conduct clinical testing of a biopharmaceutical product in humans in such jurisdiction.

1.73 “Indemnified Party” is defined in Section 14.4.

1.74 “Indemnifying Party” is defined in Section 14.4.

1.75 “Indirect Damages” is defined in Section 14.5(a).

1.76 “Information” means any data, results, and information of any type whatsoever, in any tangible or intangible form, including know-how, trade secrets, practices, techniques, methods, processes, inventions, developments, specifications, formulations, formulae, materials

or compositions of matter of any type or kind (patentable or otherwise), software, algorithms, marketing reports, expertise, stability, technology, test data including pharmacological, biological, chemical, biochemical, toxicological, and clinical test data, analytical and quality control data, stability data, studies and procedures.

1.77 “Infringement” is defined in Section 9.6(a).

1.78 “Infringement Action” is defined in Section 9.6(b).

1.79 “Initial TC Term” is defined in Section 8.5(d).

1.80 “Insolvency Event” is defined in Section 12.4.

1.81 “JNDA” means a new drug application filed with the MHLW required for marketing approval for the applicable Product in Japan.

1.82 “JNDA Approval” means, with respect to a Product, receipt of Regulatory Approval of a JNDA by the MHLW and receipt of pricing and reimbursement approvals, for such Product in Japan.

1.83 “Joint Committee” or “JC” means the committee formed by the Parties as described in Section 3.1(a).

1.84 “Joint Invention” is defined in Section 9.1.

1.85 “Joint Patent” means a Patent with a claim Covering a Joint Invention.

1.86 “Know-How” means any Information and any other intellectual property (other than Product Marks or Patents) of any type whatsoever, in any tangible or intangible form or medium, and all rights associated therewith in any jurisdiction, including all inventions (whether or not patentable or reduced to practice), improvements, works of authorship (whether or not copyrightable) and copyrights.

1.87 “License” means the rights and licenses set forth in Article 4.

1.88 “License Effective Date” means the date determined pursuant to Section 2.5(a) or 2.5(b), as applicable.

1.89 “Liens” means any lien, pledge, encumbrance, mortgage, security interest, purchase option, call or similar right, conditional and installment sale agreements, charges or claims of any kind.

1.90 “MAA” or “Marketing Authorization Application” means an application for Regulatory Approval for a Product in the EU.

1.91 “Major European Countries” means France, Germany, Italy, Spain and the United Kingdom.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

include any BN Patents arising after the Effective Date that the Parties agree are not Product Specific Patents.

1.106 “Other Infringement Action” is defined in Section 9.6(e).

1.107 “Patent” means (a) all patents and patent applications, including provisional patent applications, (b) all patent applications filed either from such patents, patent applications or provisional applications or from an application claiming priority directly or indirectly from any of these, including divisionals, continuations, continuations-in-part, non-provisionals, converted provisionals, and continued prosecution applications, (c) any and all patents that have issued or in the future issue from the foregoing patent applications in (a) and (b), including utility models, petty patents and design patents and certificates of invention, (d) any and all extensions or restorations by existing or future extension or restoration mechanisms, including adjustments, revalidations, reissues, re-examinations and extensions (including any supplementary protection certificates and the like) of the foregoing patents or patent applications in (a), (b) and (c), and (e) any similar rights, including so-called pipeline protection, or any importation, revalidation, confirmation or introduction patent or registration patent or patents of addition to any of such foregoing patent applications and patents.

1.108 “Patent Challenge” is defined in Section 9.8.

1.109 “Patent Contact” is defined in Section 9.11.

1.110 “Patent Prosecution Costs” means the direct out-of-pocket costs (including the reasonable fees and expenses incurred to outside counsel and other Third Parties, including filing, prosecution and maintenance fees incurred to Governmental Authorities) recorded as an expense by a Party or any of its Affiliates (in accordance with Accounting Standards and its customary accounting practices) after the Effective Date and during the Term and pursuant to this Agreement, in connection with the preparation, filing, prosecution, maintenance and extension of Patents, including costs of Patent interference, appeal, opposition, reissue, reexamination, revocation, petitions or other administrative proceedings with respect to Patents and filing and registration fees.

1.111 “Patent Term Extension Patent” means [***] and all foreign counterparts.

1.112 “Person” means any individual, firm, corporation, partnership, limited liability company, trust, business trust, joint venture company, governmental authority, association or other entity.

1.113 “Phase 3 Clinical Trial” means a Clinical Trial of a product on sufficient numbers of patients that is designed to establish that such product is safe and efficacious for its intended use, and to define warnings, precautions and adverse reactions that are associated with such product in the dosage range to be prescribed, and to support regulatory approval of such product or label expansion of such product.

1.114 “Phase 3 Completion Milestone” is defined in Section 8.2.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.115 “PHS” means the United States Public Health Service within the United States Department of Health and Human Services.

1.116 “PHS License Agreement” means the Exclusive Patent License Agreement (NIH Reference #L-149-2008/0), dated as of August 12, 2008, by and between BNInc and PHS, as amended on [***], and as may be amended from time to time as permitted by this Agreement.

1.117 “PHS Royalty Term” means the period during which BNInc is required pursuant to the PHS License Agreement to pay PHS an earned royalty of [***] percent ([***]%) of “Net Sales” (as defined therein).

1.118 “Prior CDA” means the Confidential Disclosure Agreement entered into by BMS and BNAS, dated as of January 13, 2014.

1.119 “Product” means any biopharmaceutical product candidate or product containing PROSTVAC (alone or as a Combination Product), in all forms, presentations, formulations and dosage forms.

1.120 “Product Liability Claim” means any claim, suit, proceeding or cause of action arising out of illness, injury or bodily or mental harm (including death) to any person that is alleged to have been caused by the administration or use of PROSTVAC. A Product Liability Claim may be based on the existence of a design defect, strict tort liability, a manufacturing defect, a failure to warn or any other cause of action.

1.121 “Product Liability Losses” is defined in Section 14.3.

1.122 “Product Marks” means all logos, slogans, trade dress, domain names, trademarks (excluding the PROSTVAC Mark), trade names and service marks and other proprietary names for a product filed with a Regulatory Authority that a Party has used or plans to use specifically in relation to a Product; provided, that the Product Marks shall not use or incorporate any corporate names or corporate logo owned or Controlled by a Party or any of its respective Affiliates.

1.123 “Product Specific Patent” means a Patent Controlled as of the Effective Date or thereafter during the Term by BN (or any BN Affiliate) that Covers the composition, formulation, method of use and/or method of manufacture of any Product, excluding the Other BN Patents. For clarity, subject to and to the extent as provided in Section 16.8, the use of “Affiliate” in this definition shall exclude any Acquirer of BN. The Product Specific Patents existing at the Effective Date are listed in Exhibit A1. Exhibit A1 shall be updated by BN following BMS’s reasonable request from time to time.

1.124 “Product Specific Infringement Action” is defined in Section 9.6(b).

1.125 “Prosecute” or “Prosecution” is defined in Section 9.2.

1.126 “Prosecuting Party” is defined in Section 9.5(a).

1.127 “PROSPECT Clinical Supplies” is defined in Section 5.1(e).

1.128 “PROSPECT Final Data” means efficacy and safety data following realization of the required events for both comparisons and locking of the database relative to the established final data cutoff date of the PROSPECT Trial.

1.129 “PROSPECT Interim Data” means the database associated with a specific statistical analysis plan-defined interim analysis that meets all the following criteria: (a) has a cutoff date associated with the projected realization of the required events for that interim analysis, (b) has met the statistical criterion specified for that interim analysis together with an accepted recommendation from the data monitoring committee that the trial be opened to the sponsor, (c) contains the locked data used to perform that interim analysis, and (d) is supplemented with data associated with other events prior to the cutoff date but not collected prior to performing the interim analysis (e.g., additional safety data, resolution of outstanding queries not associated with deaths, etc.).

1.130 “PROSPECT Trial” means the ongoing Phase 3 Clinical Trial of PROSTVAC that is being conducted by BN as of the Effective Date, the protocol for which is set forth on Exhibit B attached hereto (the “Protocol”).

1.131 “PROSTVAC” means the product that is the subject of the PROSPECT Trial, which comprises a product that is a sequentially dosed combination of two different poxviruses, each of which encodes prostate specific antigen (PSA) plus three immune enhancing co-stimulatory molecules, B7.1, ICAM-1, and Lfa-3 (TRICOM). The first poxvirus is Vaccinia-PSA-TRICOM, and the second poxvirus is Fowlpox-PSA-TRICOM.

1.132 “PROSTVAC Mark” means the trademark PROSTVAC®, to the extent Controlled by BN as of the Effective Date or at any time during the Term and existing in any country or jurisdiction in the Territory, together with any other trademarks containing the term “PROSTVAC” used by BMS or its Affiliates or Sublicensees during the Term.

1.133 “Protocol” is defined in Section 1.130.

1.134 “Publication” is defined in Section 11.4.

1.135 “Receiving Party” is defined in Section 11.1.

1.136 “Region” is defined in Exhibit F, Part B.

1.137 “Regulatory Approval” means with respect to any country, extra-national territory, province, state, or other regulatory jurisdiction, any and all approvals, licenses, registrations or authorizations of any Regulatory Authority necessary in order to commercially distribute, sell, manufacture, import, export or market a product in such country, state, province, or some or all of such extra-national territory or regulatory jurisdiction, but which shall exclude any pricing and reimbursement approvals.

1.138 “Regulatory Authority” means, with respect to a particular country, extra-national territory, province, state, or other regulatory jurisdiction, any applicable Governmental Authority involved in granting Regulatory Approval and/or, to the extent required for such country, extra-national territory, province, state, or other or regulatory jurisdiction, pricing or reimbursement approval of a Product in such country or regulatory jurisdiction, including the FDA, the EMA, the European Commission and MHLW, and in each case including any successor thereto.

1.139 “Regulatory Materials” means regulatory applications, submissions, dossiers, notifications, registrations, Regulatory Approvals and/or other filings made to or with, or other approvals granted by, a Regulatory Authority that are necessary or reasonably desirable in order to Develop, manufacture or Commercialize a Product in a particular country or regulatory jurisdiction. Regulatory Materials include INDs, MAAs, BLAs and JNDAs. Save in respect of any copyright, Regulatory Materials shall not include the intellectual property rights contained or disclosed therein.

1.140 “Related Party” shall mean BMS and its Affiliates and their respective Sublicensees (and such Sublicensees’ Affiliates) of one or more Products. For clarity, Related Party shall not include any distributors, wholesalers or the like unless such entity is an Affiliate of BMS.

1.141 “Restricted Product” is defined in Section 10.2.

1.142 “Safety Reason” means that BMS has formed the reasonable belief that, based upon additional information that becomes available or an analysis of the existing information at any time using sound scientific principles, the medical risk/benefit of such Product is sufficiently unfavorable as to be incompatible with the welfare of patients to Develop or Commercialize or to continue to Develop or Commercialize it.

1.143 “SEC” means the U.S. Securities and Exchange Commission.

1.144 “Sole Inventions” is defined in Section 9.1.

1.145 “Sublicensee” means any Third Party granted a sublicense by BMS under Section 4.2 to the rights licensed to BMS hereunder, but shall not include any wholesaler or distributor that is a party to a wholesaler or distributor arrangement for the sale of Product (even if such wholesaler or distributor is granted a right or license to sell a Product).

1.146 “Supply Agreement” means the supply agreement to be entered into by the Parties on the License Effective Date, in the form attached hereto as Exhibit G, and with only those changes contemplated by Exhibit I hereto. “Supply Agreement” also includes any additional supply agreement entered into between BN and any Affiliate of BMS having terms substantially equivalent to those in Exhibit G.

1.147 “TC Term” is defined in Section 8.5(d).

1.148 “Term” is defined in Section 12.1.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

1.149 “Termination Notice” is defined in Section 12.3(a).

1.150 “Territory” means all countries of the world.

1.151 “Third Party” means any Person other than BN or BMS or an Affiliate of either of BN or BMS.

1.152 “Title 11” is defined in Section 16.3(a).

1.153 “Topline” means, with respect to data from a Clinical Trial, all tables, listings and figures specified in the statistical analysis plan for such Clinical Trial.

1.154 “Total Compensation” is defined in Section 8.5(a).

1.155 “U.S.” means the United States of America and its territories, districts and possessions.

1.156 “U.S. Bankruptcy Code” is defined in Section 16.3(a).

1.157 “Valid Claim” means either (a) a claim of an issued and unexpired patent which has not been held permanently revoked, unenforceable or invalid by a decision of a court or other governmental agency of competent jurisdiction, unappealable or unappealed within the time allowed for appeal and that is not admitted to be invalid or unenforceable through reissue, post-grant proceeding, disclaimer or otherwise (i.e., only to the extent the subject matter is disclaimed or is sought to be deleted or amended through reissue), or (b) a claim of a pending patent application being diligently prosecuted in good faith and that has not been abandoned, finally rejected or expired without the possibility of appeal or refiling, provided, however, that Valid Claim will exclude any such pending claim in an application that has not been granted within [***] in the case of pending claims licensed under the PHS License Agreement) following the first date of examination for such application, unless and until such claim is granted.

1.158 “Virtual Data Room” means all the documents available prior to 17.00 PST on the date that is [***] before the Effective Date in the virtual data room hosted via Merrill Datasite® at https://datasite.merrillcorp.com set up by BN for the purposes of this transaction and to which representatives of BMS have had access. An electronic copy on a disk or a memory stick of all of the documents in the Virtual Data Room has been provided to BMS on the Effective Date; provided that, such electronic copy shall represent a true and complete copy of such Virtual Data Room as of the date [***] prior to the Effective Date, without any additions, deletions or changes thereto.

2. OPTION

2.1 Grant. BN hereby grants to BMS the exclusive option, exercisable at BMS’s sole discretion, to obtain the licenses set forth in Section 4.1 (the “Option”), subject to Sections 2.2, 2.3, 2.4 and 2.5.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

2.2 Option Exercise. BMS shall have the right to exercise the Option at any time after the Effective Date in accordance with the following by providing BN written notice of such Option exercise (the “Option Exercise Notice”) and within the time periods set forth below (the “Option Term”):

(a) BMS may exercise the Option at any time prior to the date that is [***] after all of the following have occurred: (i) BMS or its designated Affiliate has received clear feedback directly from the FDA, or by BN providing BMS with a copy of a written communication from the FDA, indicating that the overall survival results based on PROSPECT Interim Data support BLA filing for the Product based on such PROSPECT Interim Data, where such feedback is provided by FDA either in writing or following a meeting with FDA (with BN to give BMS reasonable advance notice of such meeting, which BMS or its designated Affiliate may attend); (ii) BN has provided BMS with all Topline PROSPECT results (and other reports and data required by Sections 5.1(g) and 5.1(h)) prior to the FDA meeting referred to in (i) above; (iii) BN has notified BMS that BN intends to submit a BLA based on the PROSPECT Interim Data; and (iv) BN has delivered to BMS the certificate set forth in Section 2.2(e) dated no earlier than the date of the notice set forth in clause (iii).

(b) If BMS does not exercise the Option pursuant to Section 2.2(a), and BN subsequently submits a BLA in the United States for the Product based on the PROSPECT Interim Data, then the Option Term shall end and BMS’s right to exercise the Option shall expire; provided, however, that, if BN subsequently withdraws the BLA or receives a refusal to file or a complete response letter for the BLA and, as of the date of such withdrawal or letter, no Third Party has rights to PROSTVAC that are inconsistent with BMS’s Option, then the Option Term shall be reinstated and BMS shall have the right to exercise the Option as described in Section 2.2(d) below, or, if another interim analysis point as defined in the Protocol occurs subsequently where the right to exercise is triggered, under Section 2.2(a) above.

(c) If BN notified BMS in accordance with Section 2.2(a) that BN planned to submit a BLA in the United States using such PROSPECT Interim Data, BMS does not exercise the Option pursuant to Section 2.2(a), and BN does not subsequently submit a BLA in the United States for the Product based on such PROSPECT Interim Data prior to the PROSPECT Interim Data from the next subsequent analysis point as defined in the Protocol at the relevant time (or based on the PROSPECT Final Data if there is no next interim analysis point, as the case may be), then the Option Term shall be reinstated and BMS shall have the right to exercise the Option as described in Section 2.2(d) below, or, if another interim analysis point as defined in the Protocol occurs subsequently where the right to exercise is triggered, under Section 2.2(a) above.

(d) If the Option Term has not terminated pursuant to Section 2.2(b) or has been reinstated pursuant to either Section 2.2(b) or Section 2.2(c), then BMS may exercise the Option at any time until [***] after all of the following have occurred: (i) BMS or its designated Affiliate has received clear feedback directly from the FDA, or by BN providing BMS with a copy of a written communication from the FDA, indicating that the overall survival results based on PROSPECT Final Data support BLA filing for the Product based on such PROSPECT Final Data, where such feedback is provided by FDA either in writing or following a meeting with FDA (with BN to give BMS reasonable advance notice of such meeting, which BMS or its designated Affiliate may attend; (ii) BN has provided BMS with all Topline

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

PROSPECT Final Data (and other reports and data required by Sections 5.1(g) and 5.1(h)) prior to the FDA meeting referred to in (i) above; (iii) BN has delivered to BMS the certificate set forth in Section 2.2(e) dated no earlier than the date on which the FDA has provided clear feedback pursuant to clause (i).

(e) As set forth in Sections 2.2(a) and 2.2(d), BN shall provide BMS with a certificate signed by a senior officer of BN certifying that (i) the representations and warranties of BN under Article 13 are true and correct in all respects as of the date of such certificate, subject to any matter disclosed by BN in a disclosure schedule attached to such certificate, and (ii) BN and its Affiliates have performed and complied with each covenant to be performed by it under this Agreement during the Option Term. BN shall promptly provide to BMS all information reasonably requested by BMS in order to allow BMS to make a detailed assessment of the impact of any matter disclosed in the disclosure schedule and the Parties shall discuss in good faith possible adjustments to this Agreement to account for such impact (without any obligation on either Party to agree to make any such adjustment), and the [***] period for BMS to exercise the Option shall not commence until the earlier of (A) any such discussions and/or the negotiation of any such adjustments having been completed and (B) [***] from the date on which the certificate was provided to BMS.

2.3 Expiration of Option. If BMS does not exercise the Option within the Option Term, then (a) the Option shall terminate and be of no further force or effect as of the expiration of the Option Term, and (b) this Agreement shall expire pursuant to Section 12.1.

2.4 HSR. If BMS reasonably determines in good faith prior to the expiration of the Option Term that the exercise of the Option is required to be filed with the FTC under the HSR Act, and/or any other clearance is needed from any other Governmental Authority in connection with the exercise of the Option, BMS shall provide written notice of exercise of the Option to BN prior to the end of the Option Term, and the Parties shall file the relevant documents with the FTC and/or any other Governmental Authority as required within [***] after BMS’s written notice of the exercise of the Option. The Parties shall cooperate in good faith with respect to such filings with the objective of obtaining prompt HSR Clearance and/or all other such clearances. Where BMS has made its filings within the aforementioned time limit, the Option Term shall automatically be extended until the earlier of (i) HSR Clearance (and/or all other such clearances) are granted; (ii) BMS withdraws its request for HSR Clearance (and/or all other such clearances); or [***] after the later to occur of (A) provision of written notice of the exercise of the Option by BMS to BN and (B) the date on which BN has made all of its filings under this Section 2.4. Nothing in this Section 2.4 or otherwise in this Agreement shall require either Party to divest any assets, or to take action (beyond cooperation with the other Party) to respond to any “Second Request” from the FTC or similar request from any other Governmental Authority (unless BMS elects to respond to a Second Request or similar request from any other Governmental Authority in which case both Parties will do so), in connection with any clearance filing. Each Party shall be responsible for all costs and expenses, including filing fees and attorneys’ fees, incurred by such Party in connection with the preparation and filing of submissions to the FTC under the HSR Act and in responding to any “Second Request” and/or other action by the FTC under the HSR Act, and/or in connection with any other such clearance needed from any other Governmental Authority;

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

provided, that BMS will bear all filing fees required by FTC for submission. If HSR Filings and/or any other such clearance from any other Governmental Authority are required, each Party shall use Diligent Efforts to prepare and file its respective filings as promptly as is practicable, and BMS shall use commercially reasonable efforts to request early termination of all applicable waiting periods. In the event that clearance has not been granted within [***] after the provision of written notice of the exercise of the Option by BMS to BN then BN or BMS may terminate this Agreement with no further liability to the other and the provisions of Section 12.6 shall apply.

2.5 License Effective Date.

(a) If the exercise by BMS of the Option does not require the making of HSR Filings under Section 2.4, the License shall become effective on the date that BMS provides the Option Exercise Notice.

(b) If the exercise by BMS of the Option requires the making of HSR Filings under Section 2.4, the License shall become effective on the date of HSR Clearance.

(c) If the exercise by BMS of the Option requires the making of any filings (other than HSR Filings) under Section 2.4, BMS shall not acquire any license hereunder with respect to the portion of the Territory under any reviewing Governmental Authority’s jurisdiction until the date on which: (i) all applicable waiting periods have expired or terminated and (ii) all applicable approvals and/or clearances from such Governmental Authority have been received. For the avoidance of doubt the delay in BMS’s acquisition of its license rights hereunder pursuant to this Section 2.5(c) shall not delay the License Effective Date beyond that set out in Sections 2.5(a) and 2.5(b).

3. GOVERNANCE

3.1 Joint Committee.

(a) Establishment and Membership of JC. Within [***] after the Effective Date, the Parties will establish a joint committee responsible for overseeing the activities of the Parties in the Development of Products (the “Joint Committee” or “JC”). Each Party will initially appoint two (2) representatives to the JC. The JC may change its size from time to time by mutual consent of its members, provided that the JC will consist at all times of an equal number of representatives of each of BN and BMS. The JC membership and procedures are further described in this Section 3.1. Each Party may at any time appoint different JC representatives by written notice to the other Party. Each of BN and BMS will designate representatives with appropriate expertise to serve as members of the JC. Each of BN and BMS will select from their representatives a co-chairperson for the JC, and each Party may change its designated co-chairperson from time to time upon written notice to the other Party. The co-chairpersons of the JC, with assistance and guidance from the Alliance Managers, will be responsible for calling meetings and preparing and circulating an agenda in advance of each meeting, provided that the co-chairpersons will call a meeting of the JC promptly upon the reasonable written request of either co-chairperson to convene such a meeting.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(b) Role of JC. The JC shall be limited to (i) overseeing the activities of the Parties in the Development of Products, including monitoring the progress of performance of the PROSPECT Trial by BN, reviewing changes to the Protocol, and coordinating and managing the interactions of the Parties prior to the Option being exercised by BMS, and (ii) reviewing information regarding BMS’s Commercialization and Development of Products, including the Commercialization and Development Plan. The JC may establish subcommittees and working groups to perform work within the JC’s purview and that will report to the JC to further the objectives of the JC.

(c) JC Meetings. The JC will hold meetings at such times and places as the co-chairpersons may determine. The JC will meet at least once every Calendar Quarter during which BN is conducting the PROSPECT Trial and semi-annually thereafter unless the Parties agree otherwise. The meetings shall be quorate so long as at least one member from each Party can hear and be heard at the relevant meeting. The meetings of the JC need not be in person and may be by telephone or any other method determined by the JC. Each Party will bear its own costs associated with attending such meetings.

(d) Discontinuation of JC. The JC shall exist until the earlier of (i) [***], (ii) the date on which it is dissolved pursuant to Section 10.4, (iii) the date on which the Parties agree in writing that it should be dissolved. All subcommittees and working groups established by the JC will dissolve when they have fulfilled their purpose. BMS shall perform all functions of the JC following its dissolution.

(e) Decision-Making and Limitations on Authority of the JC. Decisions of the JC shall be by consensus (with each Party having one vote); provided that if the JC is unable to reach consensus on any matter, the matter shall be referred to the Executive Officers of the Parties for resolution. In the event such Executive Officers cannot reach agreement on such matter within [***] after such referral, then, (i) prior to License Effective Date, except as otherwise set forth in this Agreement, BN’s Executive Officer shall have the final decision-making authority for all decisions relating to the Products in the Field in the Territory, and (ii) from and after the License Effective Date, BMS’s Executive Officer shall have the final decision-making authority for all decisions relating to future Development and/or Commercialization (including pricing and reimbursement of Products in the Field in the Territory) but excluding manufacturing matters pursuant to the Supply Agreement where BN’s Executive Officer shall have the final decision-making authority subject to the terms and conditions of the Supply Agreement. The JC will have solely the roles and responsibilities assigned to it in this Article 3. The JC will have no authority to amend, modify or waive compliance with this Agreement. The JC (whether through consensus or a Party exercising its final decision-making authority) shall not have the authority to alter a Party’s rights or obligations, or to waive a Party’s compliance with its obligations, under this Agreement.

3.2 Alliance Managers. Each of the Parties will appoint one representative who possesses a general understanding of Development issues to act as its alliance manager (each, an “Alliance Manager”). The role of the Alliance Manager is to act as a primary point of contact between the Parties to assure a successful relationship between the Parties. The Alliance Managers will attend all meetings of the JC and support the co-chairpersons of the JC in the

discharge of their responsibilities. An Alliance Manager may bring any matter to the attention of the JC if such Alliance Manager reasonably believes that such matter warrants such attention. Each Party may change its designated Alliance Manager from time to time upon written notice to the other Party. Any Alliance Manager may designate a substitute to temporarily perform the functions of such Alliance Manager upon written notice to the other Party’s Alliance Manager. Each Alliance Manager will be charged with creating and maintaining a collaborative work environment within the JC. Each Alliance Manager also will:

(a) be the point of first referral in all matters of conflict resolution;

(b) provide a single point of communication both internally within the Parties’ respective organizations and between the Parties, including during such time as the JC is no longer constituted provided that the JC may agree that other people be nominated for specific subject matter (such as the clinical or regulatory functions);

(c) plan and coordinate any cooperative efforts under this Agreement, if any, and internal and external communications; and

(d) take responsibility for ensuring that JC activities, such as the conduct of required JC meetings, occur as set forth in this Agreement and that relevant action items, if any, resulting from such meetings are appropriately carried out or otherwise addressed.

4. GRANT OF RIGHTS AND LICENSES

4.1 Licenses to BMS.

(a) The licenses granted by BN to BMS under this Section 4.1, and the other rights and licenses under this Article 4, shall only become effective upon the License Effective Date.

(b) Subject to the terms and conditions of this Agreement and the applicable terms of the Existing Product Agreements, BN hereby grants to BMS an exclusive (even as to BN and its Affiliates) license, with the right to grant sublicenses as provided in Section 4.2, under BN’s and its Affiliates’ rights in BN Technology, to research, Develop, have Developed, use, sell, offer for sale, import, export and otherwise exploit (including the exclusive right to Commercialize and have Commercialized), and transfer physical possession of or title in, Products in the Field in the Territory; provided that such license shall not include rights to practice any claim of any of the BN Patents to the extent such claim is directed to the composition or formulation of any active ingredient other than PROSTVAC or methods of use of any active ingredient other than in combination with PROSTVAC. For the avoidance of doubt, such license shall include rights under Patent claims Covering PROSTVAC in combination with one or more other active ingredients (whether such claims Cover compositions of matter, methods of use or methods of manufacturing said combinations) but such license shall not include the right to manufacture, use, sell or dispose of any such other active ingredients separately from such combination. For clarity, if BN Controls only non-exclusive rights to any BN Technology, BMS shall have an exclusive license as to Products in the Field in the Territory under BN’s non-exclusive rights to such BN Technology.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(c) Subject to the terms and conditions of this Agreement, BN hereby grants to BMS a non-exclusive license, with the right to grant sublicenses as provided in Section 4.2, under BN Diagnostic Technology to research, Develop, have Developed, manufacture, use, sell, offer for sale, import, export and otherwise exploit (including the right to Commercialize and have Commercialized) Companion Diagnostics in the Territory. This license shall not be exercised for the Commercialization of Companion Diagnostics by BMS itself unless and until the Parties have agreed on the financial terms thereof in accordance with Section 10.5, but it shall be entitled to grant sublicenses to Third Parties for such Commercialization (in addition to the other rights pursuant to this Section 4.1(c)) subject to Section 4.2.

(d) Subject to the terms and conditions of this Agreement and the applicable terms of the Existing Product Agreements, BN hereby grants to BMS a non-exclusive license, with the right to grant sublicenses (to its Affiliates and, subject to BN’s prior written consent, not to be unreasonably withheld or delayed, to any Third Party), under BN Technology to manufacture Products in the Field in the Territory in accordance with the Supply Agreement.

(e) All the rights granted in this Agreement shall be subject to the rights of PHS and the NIH under the provisions of the PHS License Agreement and the NIH CRADA, respectively, and such rights of PHS and the NIH shall be binding upon BMS and each Sublicensee of rights arising under the PHS License Agreement and the NIH CRADA.

(f) The obligations of BN to PHS and the NIH under the provisions of the PHS License Agreement, and, if applicable, under any license granted in accordance with the NIH CRADA, that are set forth on Exhibit C shall, to the extent applicable, be binding upon BMS and each Sublicensee of rights arising under the PHS License Agreement and any license granted in accordance with the NIH CRADA as if BMS or such Sublicensee were a party to the PHS License Agreement and the applicable license granted in accordance with the NIH CRADA, in each case as such obligations may be modified by amendments to such agreements as to which BMS provided its written consent and in each case subject to BN performing all such obligations to PHS and NIH that are applicable to BN (for example, and without limitation, such obligations relating to supply). BMS agrees to cause copies of such provisions to be attached to all agreements entered into by BMS that grant a sublicense of any rights arising under the PHS License Agreement and, if applicable, any license granted in accordance with the NIH CRADA. Following the execution of any license granted in accordance with the NIH CRADA, the Parties shall amend Exhibit C to reflect the provisions of such license that BN is obligated to attach hereto to the extent such provisions differ from those set forth on Exhibit C as of the Effective Date.

4.2 Sublicensing by BMS. BMS shall have the right to sublicense any or all of the rights granted hereunder [***]. BMS shall provide BN with a copy of a near final draft of any agreement requiring BN’s consent at least [***] prior to its execution and, without prejudice to BMS’s obligation to obtain BN’s consent to such license, shall give good faith consideration to all of BN’s reasonable comments. Subject to the foregoing, any sublicense entered into by BMS that requires BN’s consent shall not differ in any material respect from the draft provided to BN. In connection with any such sublicensing, BMS may disclose and provide to such permitted

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Sublicensees any applicable BN Know-How and BN Materials in connection therewith. BMS shall ensure that each of its Sublicensees is bound by a written agreement that is consistent with, and subject to the terms and conditions of, this Agreement (including Section 4.1(e)). In addition, BMS shall be responsible for the performance of any of its Sublicensees that are exercising rights under a sublicense of the rights granted by BN to BMS under this Agreement, and the grant of any such sublicense shall not relieve BMS of its obligations under this Agreement, except to the extent they are satisfactorily performed by any such Sublicensee(s). Promptly following the execution of each sublicense with a Third Party as provided in this Section 4.2, BMS shall provide BN with a copy of such sublicense agreement; provided that any financial or commercial terms may be redacted unless they are required to be provided by this Agreement or Section 4.1(f), and BMS shall not be obligated to provide BN with notice or copies of sublicenses executed by BMS with its Affiliates.

4.3 Transfer of Materials. BN shall only be required to transfer to BMS the BN Materials identified in Exhibit D. Such transfer shall be at BMS’s reasonable request, such request to be made prior to the first anniversary of the License Effective Date. To the extent that BN transfers to BMS any BN Materials, such materials shall be used solely for the purposes of this Agreement and for no other purpose whatsoever. BMS shall keep such materials secure and shall not provide the same to any Third Party other than as required for the purpose of carrying out its obligations under this Agreement. In particular BMS shall not incorporate any part of the BN Materials in any other materials or products. BMS shall, at BN’s option, return, or destroy such BN Materials on termination or expiry of this Agreement. BMS acknowledges that, except for any Products supplied and paid for under the Supply Agreement, all BN Materials provided under this Agreement are, unless otherwise agreed in writing, provided as is and are experimental in nature and are provided without any warranty of merchantability, fitness for any purpose or any other warranty.

4.4 No Other Rights. Except for the rights expressly granted under this Agreement, no right, title, or interest of any nature whatsoever is granted whether by implication, estoppel, reliance, or otherwise, by a Party to the other Party. All rights with respect to Information, Patent or other intellectual property rights that are not specifically granted herein are reserved to the owner thereof.

4.5 Public Domain Information. Nothing in this Agreement shall prevent BMS and its Affiliates from using for any purpose any Know-How or other Information that is in the public domain.

4.6 Technology and Data Transfer; Transition. Promptly following BMS’s request on or after the License Effective Date:

(a) BN shall perform the activities and provide to BMS the BN Technology set forth on Exhibit D attached hereto as soon as practicable and in any event within [***] after the License Effective Date.

(b) BN shall transfer to BMS the safety database for the Products, in the form in which it is held by BN, as soon as practicable and in any event within [***] after the License Effective Date.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(c) BN shall perform the activities with respect to transitioning responsibility for Product Development and regulatory matters set forth on Exhibit E attached hereto within the time limits set out in Exhibit E.

(d) BN shall provide FTEs up to [***] hours over a period of [***] commencing on the License Effective Date to perform its obligations pursuant to this Section 4.6. BMS shall pay (at the FTE Rate) for any FTEs provided by BN that exceed [***] hours over a period of up to [***] commencing on the License Effective Date; provided, however, that BN shall not be obligated to provide more than [***] hours of FTEs over the [***] period and, if BN decides not to provide same, the Parties shall meet and confer for the purpose of determining an appropriate solution regarding the number of hours and which FTEs are to be provided. Following the provision of such efforts, any further technology transfer shall be provided by prior agreement with BN, which shall not be unreasonably withheld, as to the amount of work, the timing and the effort to be applied and at BMS’s cost, subject to BMS meeting BN’s internal costs (at the FTE Rate) and out-of-pocket costs for doing so pursuant to a mutually agreed plan and budget.

5. DEVELOPMENT; REGULATORY MATTERS

5.1 Development of Product Before Option Exercise. Prior to the License Effective Date, except as otherwise set forth in this Section 5.1, and subject to JC oversight, BN shall have sole responsibility, including sole responsibility for all funding, resourcing and decision-making, for Development of the Products, including the conduct of the PROSPECT Trial and the preparation, content and submission of all Regulatory Materials. Where BN is required to inform BMS of, or discuss (including seek the advice or recommendations of) with BMS a matter under this Section 5, providing that information to the JC or having such discussion within the JC shall be deemed to be compliance with that obligation. Notwithstanding the foregoing, prior to the License Effective Date, BN shall inform BMS of any additional activity proposed to be conducted under the NIH CRADA that is specifically related to PROSTVAC in sufficient time to allow BMS a reasonable opportunity to comment thereon, and, unless BMS otherwise agrees in writing, BN shall be solely responsible for, and bear all costs of, all activities conducted under the NIH CRADA, whether conducted before or after the License Effective Date.

(a) BN (i) shall conduct, and use Diligent Efforts to complete, and be solely responsible for the PROSPECT Trial and (ii) shall conduct, and shall ensure that its Affiliates and/or Third Party independent contractors shall conduct, the PROSPECT Trial in good scientific manner and in compliance with all applicable good clinical practices, cGMP and all other Applicable Laws, and, without limiting the generality of the foregoing, in accordance with the Protocol and all other terms and conditions of this Agreement. BN shall conduct the PROSPECT Trial, and allocate and ensure there are sufficient resources, as needed, and use Diligent Efforts to complete the PROSPECT Trial and submit a meeting request with the FDA [***]. BN agrees that it will not change the CRO responsible for the PROSPECT Trial without prior consultation with JC subject to the provisions of Section 3.1(e). BN shall keep the JC informed of any major changes to the CRO Agreement through the JC meetings, and shall not change the CRO Agreement in any manner that may materially and

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

adversely affect the timing and/or conduct of the PROSPECT Trial without BMS’s prior written approval, with such approval not to be unreasonably withheld or delayed.

(b) BN shall be responsible for all costs and expenses incurred by BN or on BN’s behalf in the performance of the PROSPECT Trial and all other activities undertaken by or on behalf of BN in connection with the Development of Products prior to the License Effective Date with the exception of any clinical studies to be carried out under the Clinical Collaboration Agreement entered into by the Parties on the Effective Date. For the avoidance of doubt, BN shall not be responsible for any of BMS’s costs incurred in relation to any time prior to or after the License Effective Date, except as provided under this Agreement or any other agreement to which the Parties are parties.

(c) No later than [***] before BN’s blinded estimate of the potential occurrence of the first interim analysis for the PROSPECT Trial, BN shall submit to the FDA an amendment to the statistical analysis plan for the PROSPECT Trial so that, subject to the FDA’s affirmation in writing that the Special Protocol Assessment (as so revised or as reissued with the amendment included) remains in effect and is not compromised by the change, interim analyses will be performed only on the PROSTVAC-only arm plus placebo arm (not the PROSTVAC plus GM-CSF arm), which amendment shall be subject to BMS’s prior written approval, not to be unreasonably withheld or delayed. For clarity, analysis of the PROSTVAC plus GM-CSF arm data will occur after completion (after approximately [***]% of the required number of events specified in the Protocol and statistical analysis plan) of the PROSPECT Trial, or, in the case of early termination of the PROSPECT Trial, after such early termination. BN shall promptly notify BMS of any change to its blinded estimate of the potential occurrence of the first interim analysis for the PROSPECT Trial.

(d) Except as set forth in Section 5.1(c), BN shall not make any substantive change to (i) the Protocol for the PROSPECT Trial, and/or (ii) the target number of patients to be enrolled in the PROSPECT Trial without the prior written approval of BMS, with such approval not to be unreasonably withheld or delayed and, if BMS does not respond in any manner to BN’s written request (provided in accordance with Section 16.5) containing the details (including, as applicable, the text) of the proposed change within [***] after receipt, BMS shall be deemed to have approved such change. Any dispute in relation to the conduct and implementation of the PROSPECT Trial shall be subject to Section 5.1(f).

(e) BN shall, at its own expense, have and maintain such offices, laboratories, manufacturing and other facilities and all other assets and resources as may be necessary to perform and fully support the PROSPECT Trial and ensure that such facilities, and, as applicable, such other assets and resources, meet all requirements under Applicable Laws. Without limiting the generality of the foregoing, BN hereby acknowledges and agrees that BN shall be solely responsible and liable for all manufacturing activities, including supply of all clinical supplies required to conduct and fully support the PROSPECT Trial, including the manufacture of the Product and the handling, packaging, storage and shipment thereof for the purposes of the PROSPECT Trial (collectively, “PROSPECT Clinical Supplies”).

(f) BN shall have final decision-making authority regarding its conduct and implementation of the PROSPECT Trial in accordance with, and subject to, the Protocol and all

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

other terms and conditions of this Agreement, but shall duly consider, without being bound by, the recommendations and advice of BMS in connection therewith.

(g) Reasonable high level information regarding the conduct of the PROSPECT Trial shall be promptly disclosed to the JC. Within [***] following the end of each Calendar Quarter, BN shall provide to the JC a written report summarizing at high level detail the work performed by it under the PROSPECT Trial and any other Development and/or manufacturing activities achieved by BN with respect to the Product during the preceding Calendar Quarter. If reasonably requested by BMS, BN shall, subject to Section 5.1(k), make presentations to the JC of the work done in the performance of the PROSPECT Trial (including blinded event data, regulatory interactions and activities, audit plans, summaries of site audit reports, summaries of health authority site inspection reports, and summaries of manufacturing/supply chain activities). BMS shall have the right to visit and conduct audits of the Manufacturing Facilities for the Product on reasonable advanced notice (not being less than [***]) at reasonable times during business hours. As may be reasonably requested by BMS on no more than [***] occasions between each meeting of the JC, each request to be received at least [***] prior to the FDA meeting referred to in Section 2.2(d)(ii), BN shall promptly provide BMS, directly or through the JC, with additional detail regarding the conduct of the PROSPECT Trial (including summaries of work performed by the CRO or any other Person on behalf of BN) and manufacturing of the Product, subject to Section 5.1(k). Any reports required under this Section 5.1(g) may take the form of and be recorded in minutes of the JC’s meetings, which shall contain copies of any slides relating to the results presented to the JC at its meetings for which such minutes are prepared. All Information generated in connection with the PROSPECT Trial solely by or on behalf of BN shall be owned by BN and treated as Confidential Information of BN; except that during the Term following the License Effective Date, notwithstanding that it is owned by and confidential to BN, such Information shall also be kept confidential by BN subject to the same rights (including the right to publish) and obligations that BN has under Article 11 in respect of Confidential Information of BMS.

(h) Without limiting the generality of Section 5.1(g), BN shall promptly notify BMS (and in any event not later than [***] thereafter) of any recommendation from the data monitoring committee that the PROSPECT Trial be opened to the sponsor and, within one hundred and [***] after the unblinding of the PROSPECT Interim Data or PROSPECT Final Data, BN shall provide BMS with the Topline results of the PROSPECT Trial. Upon BMS’s reasonable request, BN shall, subject to Section 5.1(k), perform up to [***] within a reasonable time limit, being not less than [***] after each such request. Any such request must be made within [***] after the receipt by BMS of the Topline analyses from the statistical analysis plan of the PROSPECT Trial referred to above.

(i) Promptly following BMS’s preparation of such plans in accordance with its normal business practices, but in no event earlier than [***] before BMS’s expected First Commercial Sale of a Product in the Territory, BMS shall, subject to Section 10.4, provide to the JC the Commercialization and Development Plan for the Product which is subject of the PROSPECT Study.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(j) The Parties agree that the PROSTVAC Mark will not be used as the proprietary name to commercialize the Product. Notwithstanding BN’s sole responsibilities set out in Section 5.1 above, as of the Effective Date, BMS shall have the right to conduct activities, at BMS’s expense, relating to the identification, selection and registration of new suitable Product Marks for the Product, and, as between the Parties, BMS shall own all rights to and goodwill in any new Product Marks so selected by BMS. BMS will give consideration to any reasonable comments BN may provide with respect to BMS’s activities and the Parties will seek to avoid duplicative activities. BN will provide promptly to BMS after the Effective Date any search opinions/agency assessment in its possession relating to potential Product Marks for PROSTVAC, and BMS will be free to use and pursue registration for any such names. If BMS does not exercise the Option and BN wishes to obtain ownership of a given Product Mark, then, to the extent that BMS has any ownership right to such Product Mark, BMS shall assign the same to BN following BN’s reimbursement of all out-of-pocket costs incurred by BMS and its Affiliates in connection with identifying, selecting and registering such Product Mark.

(k) BN’s obligation to comply with BMS’s reasonable requests for information as set forth in Sections 5.1(g) and 5.1(h) (but not to provide any information otherwise required by such Sections) shall be subject to the JC’s agreement as to the scientific soundness of such requests and BMS’s prior written agreement to reimburse BN for BN’s internal costs (at the FTE Rate) and external costs incurred in complying with such requests pursuant to a mutually agreed budget.

5.2 Development of Product Following Option Exercise.

(a) From and after the License Effective Date, subject to BN’s continuing obligations under the NIH CRADA as of the License Effective Date, BMS (by itself or through its Affiliates) shall have sole responsibility, including sole responsibility for all funding (subject to Section 5.2(b)), resourcing and decision-making, for all further research and Development with respect to the Products, subject to JC oversight; provided that BN shall continue to complete the conduct and statistical analysis of the PROSPECT Trial, and contribute to the Regulatory Materials for the submission of a BLA, subject to Section 5.3, and BN shall, unless expressly assumed by BMS in writing, perform all close-down/close-out activities with respect to the PROSPECT Trial. BMS shall Develop the Products in compliance with all Applicable Laws. BMS (by itself or through its Affiliates, Sublicensees, contractors or agents, as applicable) shall use Diligent Efforts to Develop (including at a minimum, for PROSTVAC, to meet the diligence benchmarks in Appendix E of the PHS License Agreement as modified by the latest amendment to that agreement as to which BMS provided its written consent) a Product for the purpose of obtaining a Regulatory Approval in each Major Market.

(b) BMS shall use Diligent Efforts to Develop and obtain Regulatory Approval for a Product for each of the Major Markets. In particular, and subject to BN’s compliance with its obligations hereunder, BMS shall use Diligent Efforts to file for Regulatory Approval for the PROSTVAC Product in at least the U.S. and the European Union within [***] after the License Effective Date and thereafter to obtain such Regulatory Approvals.

(c) BN shall remain responsible for all expenses related to the conduct of the PROSPECT Trial.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(d) Following the dissolution of the JC, for each Calendar Year following the License Effective Date and continuing until such time as Regulatory Approval of all Products under Development has been obtained in the Major Markets, BMS shall provide to BN at least annually (and more often as BN may reasonably request) within [***] after the end of such Calendar Year a written report of the status of its efforts to Develop Products hereunder. BMS will provide such Development report to BN’s Alliance Manager.

5.3 Regulatory Matters for Product.

(a) From and after the License Effective Date, BMS (by itself or through its Affiliates) shall have primary responsibility for preparing and submitting all Regulatory Materials for Products in the Field in the Territory, including preparing, submitting and holding all applications for Regulatory Approval for Products. In accordance with Exhibit E, BN shall prepare portions of the dossier to support U.S. and EU applications for Regulatory Approval as a Common Technical Document (CTD) including: financial disclosures, FDA correspondence, and other appropriate sections of Module 1 that pertain to BN; quality and nonclinical overviews/summaries for Module 2; all documentation and reports for Modules 3 and 4; and final study reports and/or publications that are held by and reasonably available to BN for all completed studies in Module 5 other than the PROSPECT Trial. BN will prepare, write and finalize a Clinical Study Report for the completed PROSPECT Trial, with review and input by BMS. Subject to agreement between the Parties as to which Party shall be responsible for filing the BLA pursuant to Section 5.3(b), BMS working with BN may prepare, write and finalize Clinical Summary documents to complete the regulatory dossier for Modules 2 and 5. BMS will provide administrative documents, product labeling and REMs information to complete Module 1. BN shall cooperate fully with BMS in finalizing the dossiers for submissions to Regulatory Authorities. If BMS exercises the Option, BMS shall reimburse BN’s out-of-pocket and internal costs (at the FTE Rate) incurred in undertaking the activities set out in this Section 5.3(a) whether undertaken before or after the License Effective Date pursuant to a mutually agreed budget on a quarterly basis within [***] after receipt of an invoice from BN.

(b) After the Effective Date the Parties, through the JC (with BMS having final decision-making authority), shall discuss whether there are advantages to BN filing the BLA notwithstanding that BMS has exercised the Option. If the Parties agree that BN will file the BLA then the Parties shall agree detailed provisions that will govern this activity including: (i) the responsibilities of each Party for the compiling of various sections of the BLA, taking into account BN’s responsibilities set out in Section 5.2(a); (ii) without prejudice to BMS’s obligations to pay BN’s costs pursuant to Section 5.2(a), [***]; (iii) the content of the BLA shall be agreed by the JC; (iv) all correspondence from the FDA shall be copied to BMS; (v) no response shall be sent to the FDA without BMS’s prior review and approval; and (vi) BN shall otherwise comply with BMS’s directions other than any such direction that is not supported by sound scientific principles. On the grant of the BLA, BN shall assign the same to BMS for no additional consideration other than reimbursement of its costs as provided for herein.

(c) Within [***] after the License Effective Date, BN shall transfer and assign to BMS (or one or more Affiliates designated by BMS) all of BN’s right, title and

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

interest to any Regulatory Materials identified in Exhibit E, including IND(s), for Products in the Field that have been submitted as of the License Effective Date, in accordance with Exhibit E. BN shall notify the applicable Regulatory Authorities in writing that it is transferring such Regulatory Materials to BMS. BN shall cooperate fully with BMS and provide to BMS all Information Controlled by BN, in each case as may be reasonably requested by BMS, in order to support any Regulatory Materials for Products in the Field in the Territory and interactions with any Regulatory Authority in connection with Development and/or Regulatory Approval of Products. From and after the License Effective Date, BMS will own all Regulatory Materials created by BMS for Products in the Territory and all such Regulatory Materials shall be submitted in the name of BMS (or its Affiliate or Sublicensee, as applicable). Notwithstanding the foregoing, the Information contained in such Regulatory Materials shall be owned in accordance with Section 9.1 provided always that where BN owns such data and it has relevance to products or processes other than PROSTVAC, BN shall not be restricted in its use of such Information for products and processes other than Products. Except as otherwise provided under the Supply Agreement, BMS (by itself or through its Affiliates) shall, subject to compliance with the Existing Product Agreements and the provisions of Section 5.2(b), have sole decision-making authority with respect to regulatory matters with respect to Products (including the content of any regulatory filing or dossier, pharmacovigilance reporting, labeling, safety, and the decision to file or withdraw any BLA, MAA, JNDA or to commence, cease or suspend any Clinical Trial). For clarity, the CRO Agreement will not be assigned to BMS and BN will remain responsible for all obligations, including making payments, thereunder.

5.4 Adverse Event Reporting. From and after the date that safety data has been transferred to BMS pursuant to Section 4.6(b), BMS shall be responsible for the reporting to the appropriate Regulatory Authorities of all Adverse Events and any other information concerning the safety of Products, in each case, in accordance with Applicable Law of the relevant countries. Unless the Parties otherwise agree, the Parties will enter into a mutually agreed pharmacovigilance agreement with respect to the Products within [***] after the License Effective Date.

6. MANUFACTURING

6.1 Manufacturing. The Parties shall enter into the Supply Agreement on the License Effective Date. Subject to the provisions of the Supply Agreement, BN shall have responsibility for the manufacture of Products for the Territory.

6.2 PROSPECT Clinical Supplies. BN shall ensure that all PROSPECT Clinical Supplies are manufactured in accordance with cGMP, applicable regulatory requirements and all other Applicable Laws and the established specifications therefor and the quality standards agreed to by the Parties, including all Applicable Laws (a) where any PROSPECT Clinical Supplies are being used, and (b) in the applicable country of manufacture with respect to environment, health, safety and hazardous transportation (EHS). Without limiting the generality of BN’s obligations hereunder, BN shall keep BMS regularly updated, through the JC (and as may be reasonably requested by BMS), with respect to all such manufacturing activities that relate to the PROSPECT Trial or with regard to the manufacture of the PROSPECT Clinical Supplies.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

6.3 [***] Manufacturing. BMS acknowledges that BN has contracted with [***] in respect of the manufacture of the PROSTVAC Product for the PROSPECT Trial and agrees that in the event that BMS, itself or through any sublicensee, decides at any time within a period of [***] subsequent to the date of completion of the Product deliverables under BN’s manufacturing contract with [***] to have any Product manufactured in commercial quantities by any party other than BN, BMS shall commence good faith negotiations with [***] for said manufacture to be undertaken [***] percent ([***]%) exclusively by [***] pursuant to the terms and conditions of a manufacturing agreement to be mutually agreed and entered into by said parties for such purpose. BMS agrees to insert in any sublicense agreement a provision binding each sublicensee, and its sublicensees, to the obligations above set forth. At the time that BMS makes the aforesaid decision, BMS shall request from BN, and BN shall promptly provide to BMS, the date of said completion of the Product deliverables under BN’s manufacturing contract with [***] in order that BMS may calculate the aforesaid [***] time period. For avoidance of doubt, nothing in this Agreement shall be construed as imposing any legal obligation of any kind whatsoever to enter into such manufacturing agreement in the event that BMS and [***], acting in good faith, are not able to agree upon the terms and conditions of a manufacturing agreement as contemplated in this Section 6.3. No agreement providing for any such possible collaboration and/or transaction shall be deemed to exist between the Parties or BMS and [***] unless and until a definitive manufacturing agreement has been executed and delivered.

6.4 Manufacturing Inspection. At any time prior to BMS’s exercise of the Option, BMS shall have the right, but not the obligation, at BMS’s reasonable cost and expense, to conduct due diligence with respect to BN’s and its Affiliates’ manufacturing and supply capability of clinical and/or commercial quantities of the Product if and as may be requested by BMS. Without limiting the generality of the foregoing, BMS shall have the right to inspect and audit, itself and/or with or through any of its Affiliates, independent contractors and/or representatives reasonably acceptable to BN and subject to confidentiality obligations in a form reasonably acceptable to both Parties, all facilities used or proposed to be used by BN and/or its Affiliates for any Product manufacturing or related activities (each, a “Manufacturing Facility”) (including with respect to technical, quality, environmental, health and safety (EHS), compliance and capacity) and the right to observe generally BN’s and its Affiliates’ ordinary manufacturing processes (including any manufacturing activities conducted in connection with the PROSPECT Trial). BN shall assist and cooperate with BMS in connection with such diligence process as may be requested by BMS, and BN shall provide access to the Manufacturing Facilities to BMS and its Affiliates, independent contractors and representatives during normal business hours and upon reasonable notice, and BN shall ensure that its Affiliates and any Third Party contractors shall, make available to BMS (and its designees), its employees and independent contractors, and all permits, licenses, inspection reports, records and all other Information related to such Manufacturing Facilities and/or, more generally, to the manufacture of any Product.

7. COMMERCIALIZATION

7.1 Commercialization of Products. From and after the License Effective Date, BMS (by itself or through its Affiliates, Sublicensees, contractors or agents, as applicable) shall

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

use Diligent Efforts to have a First Commercial Sale of a Product in each Major Market within [***] after BMS receives both Regulatory Approval and pricing and reimbursement approvals acceptable to BMS necessary for the sale of the Product in such Major Market, and thereafter Commercialize such Product in such Major Market. Without prejudice to the foregoing, (i) BMS shall use its Diligent Efforts to Commercialize the Product in accordance with the portion of the then-current Commercialization and Development Plan covering the then-current Calendar Year and (ii) BMS (by itself or through its Affiliates) shall have sole right, including sole responsibility for all funding, resourcing and decision-making, for all Commercialization activities with respect to the Products. BMS shall perform such Commercialization activities in compliance with all Applicable Laws.

7.2 Commercialization and Development Plan. Subject to Section 10.4, the Commercialization and Development Plan shall be updated by BMS and presented to the JC at least once per Calendar Year no later than 30 November in each year. At each JC meeting BMS shall present its progress against the Commercialization and Development Plan. Subject to Section 10.4, BMS shall be required to provide an updated Commercialization and Development Plan directly to BN following dissolution of the JC.

7.3 Commercialization Report. Following dissolution of the JC, subject to Section 10.4, BMS shall provide to BN annually in November of each Calendar Year following Regulatory Approval for a Product in a Major Market a written report that summarizes the Commercialization activities performed by BMS, and its Affiliates and Sublicensees, with respect to Products in the Major Markets since the prior such report.

8. PAYMENTS

8.1 Option Grant and Option Exercise Payments.

(a) Upfront Option Grant Payment. In consideration of the grant by BN to BMS of the Option and of the performance by BN of its obligations during the Option Term, BMS shall pay to BN a one-time option grant payment of sixty million Dollars ($60,000,000) within [***] after the Effective Date.

(b) Option Exercise and License Payment. If BMS elects to exercise the Option and the License becomes effective pursuant to Section 2.5, BMS shall pay to BN a one-time Option exercise and license fee payment of eighty million Dollars ($80,000,000) (the “Option Exercise and License Fee”) within [***] after the License Effective Date.

8.2 Phase 3 Completion Milestone Payments. If BMS elects to exercise the Option and the License becomes effective pursuant to Section 2.5, then BMS shall pay to BN the following amounts, each of which shall be payable only once, following the earlier of BMS’s or its designated Affiliate’s [***] that the [***] or BMS’s or its designated Affiliate’s [***] that the [***] (the earlier of such receipts, the [***]). For the avoidance of doubt, in the event that there is a dispute as to whether the [***] has

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

8.3 Regulatory Milestone Payments. BMS shall pay to BN the following one-time non-refundable milestone payments set forth in Table 1 within [***] after the first achievement of the specified milestone event for the first indication by BMS, its Affiliates or its Sublicensees for the first Product to achieve such milestone event. In no event shall milestone payments to be made pursuant to this Section 8.3 exceed $110 million in the aggregate. For clarity, such milestone payments shall not be paid on any other Products that might achieve the same milestone event. BMS shall provide written notice to BN within [***] after the first achievement of the specified milestone event by BMS or its Affiliates and within [***] after the first achievement of the specified milestone event by its Sublicensees.

Table 1

Milestone Event for Product	Milestone Payment
[***]	$	[***]
[***]	$	[***]
[***]	$	[***]
Total	$	110,000,000

8.4 Sales Milestone Payment. The following one-time non-refundable sales milestone payments shall be payable by BMS to BN when [***] set forth below.

Milestone Event	Milestone Payment
[*] first exceed $[*]	$	[***]
[*] first exceed $[*]	$	[***]
[*] first exceed $[*]	$	[***]
[*] first exceed $[*]	$	[***]
Total	$	495,000,000

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

BMS shall pay to BN the above one-time sales milestone payments within [***] after the end of [***] during which the specified milestone event if first achieved by BMS, its Affiliates or its Sublicensees, but in any event shall not exceed $495 million in the aggregate. For clarity, [***] of a [***] (as determined in the definition of [***]) shall be taken into account for purposes of [***] with respect to the above milestone events and the [***] in [***] below.

8.5 Total Compensation Payments to BN.

(a) Generally. Subject to the other provisions of this Article 8 and other provisions of this Agreement, in consideration of the licenses granted by BN to BMS hereunder to the BN Technology and in consideration of the supply of finished Product by BN (or its applicable Affiliate) to BMS (or Related Parties), BMS shall pay to BN (or its Affiliates) total compensation (“Total Compensation”), with respect to such Product (including Product purchase price and a portion of Net Sales) equal to the [***] paid or payable to [***] during the [***] for a [***] for a [***], the applicable [***] of [***] in a [***] by [***] in the [***] as follows [***] subject to any [***] set forth in [***]

Portion of total annual Net Sales in a Calendar Year for all Products sold during the applicable [***]:	Percentage of Net Sales Rate
less than or equal to $[***]	[***]	%
greater than $[*] and less than or equal to $[*]	[***]	%
greater than $[*] and less than or equal to $[*]	[***]	%
greater than $[***]	[***]	%

By way of example, if the total [***] of [***] in the [***] in a particular [***] during the applicable [***], the amount of [***] payable hereunder (prior to any applicable offsets or reductions) [***], as follows:

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

A: (([***]% x $[***]) + ([***] x $[***]) + ([***]% x $[***]) + ([***]% x $[***]) = $[***])

B: The [***] of [***] or [***] in such [***].

(b) Third Party Payments.

(i) [***] shall bear all [***] with respect to a [***] as of the Effective Date.

(ii) Subject to Section 8.5(b)(i), if BMS reasonably determines that it is advisable to obtain a license from any Third Party under any Third Party Patent that Covers the relevant Product as such Product is formulated by BN at such time (or as formulated by BN prior to any assumption of formulation responsibility by BMS or a Third Party pursuant to the Supply Agreement), and BMS or BN obtains a license under such Third Party Patent, including for the import, manufacture, use and/or sale thereof, then BMS’s Net Sales Compensation obligations to BN under this Agreement shall be reduced by [***] percent ([***]%) of the amount of the payments made by BMS to such Third Party (or to [***] on account of such license, provided that: (x) the Total Compensation payable to BN during the Initial TC Term shall not be reduced pursuant to this Section 8.5(b)(ii) below (i) [***] percent ([***]%) of Net Sales plus (ii) the Manufacturing Cost-Based Component of Supply Price paid or payable to BN for same; provided further that BMS may carry forward to subsequent payment periods any reduction it would have been entitled to take under this Section 8.5(b)(ii) but for the floor in the preceding proviso; and (y) BMS shall not be entitled to make any deduction under this Section 8.5(b)(ii) in respect of any Product in any country after the expiry of the Initial TC Term for that Product in that country.

(iii) For the avoidance of doubt this Section 8.5(b) shall not apply to any Third Party Patent that Covers an active ingredient in a Combination Product that is not PROSTVAC.

(c) Biosimilar Competition. During the portion of the applicable Initial TC Term in a particular country where one or more Biosimilar Products with respect to a Product are sold in that country, BMS’s Net Sales Compensation obligations with respect to such Product in such country shall be reduced by reducing the percentages set forth in the table in Section 8.5(a) above by [***] percent ([***]%), in respect of any Calendar Quarter in which the sales of such Biosimilar Product(s), by unit equivalent volume in such country, exceed a [***] percent ([***]%) share of the market in that country; provided that the Total Compensation payable to BN during the Initial TC Term shall not be reduced pursuant to this Section 8.5(c) below the sum of (A) [***] percent ([***]%) of Net Sales, plus (B) the [***]. For purposes of this Section 8.5(c), “market” refers to the aggregate of the sales of the Biosimilar Product(s) and the applicable Product in a country.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(d) TC Term. BMS’s obligation to pay Net Sales Compensation on Net Sales at the rates set out in Section 8.5(a) on a Product-by-Product and country-by-country basis shall continue until the latest of: (i) the 12th anniversary of the First Commercial Sale of such Product in such country, (ii) the expiration in such country of the last Valid Claim of the last-to-expire Product Specific Patent that would be infringed by the sale of such Product in such country absent a license with respect to such Product Specific Patent and (iii) the expiration of applicable regulatory exclusivity as to such Product in such country (the “Initial TC Term”), provided however, that following the Initial TC Term for a given country, BMS shall continue to pay BN Total Compensation equal to [***] of [***] percent ([***]%) of Net Sales for Products that BN supplies to BMS (or a Related Party) pursuant to the Supply Agreement, plus (y) the [***]. “TC Term” means the Initial TC Term plus any applicable extension as described in the preceding sentence. Upon the expiration of the TC Term with respect to a Product in a given country, BMS shall have a fully paid-up perpetual license under Section 4.1 for the making, using, selling, offering for sale and importing of such Product in such country.

(e) Application of Offset. Any offsets to be applied pursuant to Sections 8.5(b)(ii) and/or 8.5(c) shall be applied first to the highest tier of Net Sales Compensation being paid, and thereafter to successively lower tiers as needed to implement same. Under no circumstances shall the Net Sales Compensation payable to BN pursuant to this Section 8.5 be reduced below [***] percent ([***]%) during the Initial TC Term; provided that BMS may carry forward to subsequent payment periods any reduction it would have been entitled to take under but for such floor.

8.6 Total Compensation Payments and Reports. All amounts payable to BN pursuant to Section 8.5 shall be paid within [***] after the end of the [***] in which the applicable Net Sales were recorded. BMS will deduct from payment of Total Compensation under this Section 8.6 any amounts paid or payable by BMS or any Related Party to BN for commercial supply of Product under the Supply Agreement with respect to such supply of Product. Each quarterly payment shall be accompanied by a Total Compensation report providing a statement, on a Product-by-Product and country-by-country basis, of: (a) the amount of Net Sales of Products in the Territory during the applicable Calendar Quarter, (b) a calculation of the amount of Total Compensation in Dollars for the Product included in Net Sales for such Calendar Quarter ([***]), (c) the amount of withholding taxes, if any, required by Applicable Law to be deducted with respect to such Total Compensation, and (d) the amount of Net Sales Compensation, if any, payable hereunder.

8.7 Payment Method. All payments due under this Agreement to BN shall be made by bank wire transfer in immediately available funds to an account designated by BN. All payments hereunder shall be made in Dollars.

8.8 Taxes. All sums payable by BMS hereunder are exclusive of any sales and value added taxes, which where applicable shall be payable by BMS in addition to the amounts specified. If laws or regulations require that taxes be withheld with respect to any Total Compensation payments by BMS to BN under this Agreement, BMS will: (x) deduct those taxes from the remittable payment, (y) pay the taxes to the proper taxing authority, and (z) send

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

evidence of the obligation together with proof of tax payment to BN on a timely basis following that tax payment. Each Party agrees to reasonably cooperate with the other Party in claiming refunds or exemptions from such deductions or withholdings under any relevant agreement or treaty which is in effect. The Parties shall discuss applicable mechanisms for minimizing such taxes to the extent possible in compliance with Applicable Law. In addition, the Parties shall reasonably cooperate in accordance with Applicable Law to minimize indirect taxes (such as value added tax, sales tax, consumption tax and other similar taxes) in connection with this Agreement. Further:

(a) [***].

(b) [***].

8.9 Foreign Exchange. Conversion of sales recorded in local currencies to Dollars shall be performed in a manner consistent with BMS’s normal practices used to prepare its audited financial statements for internal and external reporting purposes.

8.10 Offsetting. BMS may offset any damages awarded to BMS under the Supply Agreement against any amounts payable to BN under this Agreement.

8.11 Records. Each Party shall keep, and shall require its Affiliates and Sublicensees (in the case of BMS) to keep, complete, true and accurate books of accounts and records sufficient to determine and establish the amounts payable incurred under this Agreement and compliance with the other terms and conditions of this Agreement. Such books and records shall be kept reasonably accessible and shall be made available for inspection for at least three (3) full Calendar Years in accordance with Section 8.12 below (or, in the case of an audit under 8.12(b)(ii) for such period of time until the credit or withholding can no longer be used).

8.12 Audits.

(a) Of BMS Records. Upon reasonable prior notice, BMS shall permit an independent nationally recognized certified public accounting firm (subject to obligations of confidentiality to BMS), appointed by BN and reasonably acceptable to BMS, to audit the financial records of BMS to the extent relating to payments to BN under this Article 8; provided that such audit shall not occur more often than once per Calendar Year, unless a material error is

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

discovered in such audit, in which case BN shall have the right to conduct a more thorough audit. Any inspection conducted under this Section 8.12(a) shall be at the expense of BN, unless such inspection reveals any underpayment of the Total Compensation due hereunder for a given Calendar Year by at least [***] percent ([***]%), in which case the reasonable costs of such inspection for such period shall be borne by BMS. Any underpayment shall be paid by BMS to BN within [***] with interest on the underpayment at the rate specified in Section 8.13 from the date such payment was originally due, and any overpayment shall be credited against future amounts due by BMS to BN.

(b) Of BN Records. Upon reasonable prior notice, BN shall permit an independent nationally recognized certified public accounting firm (subject to obligations of confidentiality to BN), appointed by BMS and reasonably acceptable to BN, to audit the financial and tax records of BN to the extent relating to the application of and use of any tax credits and/or withholdings related to amounts paid by BMS to BN or that may be payable by BN to BMS pursuant to Section 8.8(a); provided that such audit shall not occur more often than once per Calendar Year, unless a material error is discovered in such audit, in which case BMS shall have the right to conduct a more thorough audit. Any inspection conducted under this Section 8.12(b) shall be at the expense of BMS, unless such inspection reveals any overpayment by BMS pursuant to Section 8.8(a) in connection with the amount being audited for the audited period by at least [***] percent ([***]%), in which case the reasonable costs of such inspection for such period shall be borne by BN. Any overpayment shall be paid by BN to BMS within [***] with interest on the underpayment at the rate specified in Section 8.13 from the date such payment was originally due, and any underpayment shall be credited against future amounts due by BMS to BN.

8.13 Late Payments. Any payments or portions thereof due hereunder that are not paid on the date such payments are due under this Agreement shall bear interest at a rate equal to the lesser of: (a) [***] percentage points above the [***] as published by Citibank, N.A., New York, New York, USA, or any successor thereto, at 12:01 a.m. on the first day of each Calendar Quarter in which such payments are overdue or (b) the maximum rate permitted by Applicable Law; in each case calculated on the number of days such payment is delinquent, compounded monthly.

8.14 Payments to or Reports by Affiliates. Any payment required under any provision of this Agreement to be made to either Party or any report required to be made by any Party shall be made to or by an Affiliate of that Party if designated in writing by that Party as the appropriate recipient or reporting entity.

9. INTELLECTUAL PROPERTY

9.1 Ownership of Information and Inventions. Each Party will own all inventions (and Patents that claim such inventions) solely invented by or on behalf of it and/or its Affiliates and/or their respective employees, agents and independent contractors in the course of conducting its activities under this Agreement (collectively, “Sole Inventions”). All inventions invented jointly by employees, Affiliates, agents, or independent contractors of each Party in the course of conducting its activities under this Agreement (collectively, “Joint Inventions”) and Joint Patents will be owned jointly by the Parties; provided that each Party may designate or one

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

or more of its Affiliates to own such Party’s share of any Joint Patents provided always that such Affiliate shall be bound by the terms of this Agreement applicable to the Party making the designation as though it is a party to it. Subject to a Party’s obligations under applicable terms of this Agreement (e.g., licenses granted hereunder, confidentiality obligations, etc.) with respect to same, any Information generated during or resulting from a Party’s activities under this Agreement may be used by such Party for any purpose. Following the License Effective Date, this Agreement will be understood to be a joint research agreement under applicable U.S. patent law entered into for the purpose of developing Products under the terms set forth herein.

9.2 Prosecution of Product Specific Patents.

(a) In relation to the Patents licensed under the Existing Product Agreements, the provisions of those agreements shall prevail over the provisions below and BN and/or the Existing Product Agreement Licensor shall continue to Prosecute the relevant Patents in the manner that they have been Prosecuted prior to the Effective Date; provided always that BN shall use its Diligent Efforts to provide BMS with copies of correspondence it receives from or provides to PHS or NIH or their patent attorneys in respect of such prosecution. After the License Effective Date, BMS (or its applicable Affiliate) shall bear one hundred percent (100%) of the Patent Prosecution Costs for the Non-Combination Product Specific Patents included in those licensed pursuant to the Existing Product Agreements.

(b) Prior to the License Effective Date and subject to the PHS License Agreement, BN shall draft, file, prosecute and maintain (including any oppositions, interferences, reissue proceedings, reexaminations and post-grant proceedings) in all jurisdictions in the Territory the Product Specific Patents (such activities with respect to Patents being the “Prosecution”, with the term “Prosecute” having the corresponding meaning). BN shall, prior to the License Effective Date, bear one hundred percent (100%) of the Patent Prosecution Costs for the Product Specific Patents and have lead responsibility and decision-making control for such Prosecution of the Product Specific Patents; provided that BN shall not allow any Product Specific Patent to be abandoned without BMS’s prior written consent.

(c) Non-Combination Product Specific Patents.

(i) From and after the License Effective Date, subject to the PHS License Agreement, BMS (by itself or through its Affiliates) will, as between BN and BMS, have the first right, but not the obligation, to Prosecute in all jurisdictions in the Territory the Non-Combination Product Specific Patents in BN’s or the Existing Product Agreement Licensor’s name as appropriate. Subject to Section 9.2(c)(ii), BMS (or its applicable Affiliate) shall bear one hundred percent (100%) of the Patent Prosecution Costs for the Non-Combination Product Specific Patents, and shall have lead responsibility and decision-making control for such Prosecution of the Non-Combination Product Specific Patents. For clarity, each Party will bear its own internal costs (i.e., those costs that are not Patent Prosecution Costs) with respect to its Prosecution activities for the Non-Combination Product Specific Patents.

(ii) If BMS elects not to Prosecute in any country any Patent within the Non-Combination Product Specific Patents pursuant to Section 9.2(c)(i), BMS will give BN at least [***] notice before any relevant deadline and provide to BN information it

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

reasonably requests relating to the Non-Combination Product Specific Patent. BN will then have the right to assume responsibility, using patent counsel of its choice, for the Prosecution of such Non-Combination Product Specific Patent. If BN assumes responsibility for the Prosecution for any such Non-Combination Product Specific Patents as set forth above, then the Patent Prosecution Costs incurred by BN in the course of such Prosecution will thereafter be borne by BN, provided, however, that BMS shall reimburse BN for its out-of-pocket Patent Prosecution Costs for those Non-Combination Product Specific Patents and in those countries set forth in Exhibit F (Part A) attached hereto.

(iii) The Parties will cooperate in Prosecution of the Non-Combination Product Specific Patents in all respects. Each Party will provide the other Party all reasonable assistance and cooperation in such Prosecution efforts as the other Party may reasonably request from time to time, including providing any necessary powers of attorney and executing any other required documents or instruments for such Prosecution, all at the requesting Party’s sole expense, and including, in the case of BN, using Diligent Efforts to obtain the assistance and cooperation of the Product Agreement Licensors as necessary to allow for BMS to Prosecute the Non-Combination Product Specific Patents as contemplated in Section 9.2(c) or, if that is not achievable, exercising BN’s rights regarding Prosecution under the Existing Product Agreements in a manner consistent with BMS’s decisions and decision-making authority under Section 9.2(c). Each Party will provide the other Party with copies of any documents it receives or prepares in connection with such Prosecution and will inform the other Party of the progress of it. Before filing in connection with such Prosecution any document with a patent office, each Party will provide a copy of the document to the other Party sufficiently in advance to enable the other Party to comment on it, and the first Party will give due consideration to such comments.

(d) Existing Combination Product Patent.

(i) From and after the License Effective Date, BN will continue to have the first right, but not the obligation, to Prosecute in all jurisdictions in the Territory the Existing Combination Product Patent in BN’s name. Subject to Section 9.2(d)(iii), BN shall bear one hundred percent (100%) of the Patent Prosecution Costs for the Existing Combination Product Patent, and, subject to Section 9.2(d)(iv), shall have lead responsibility and decision-making control for such Prosecution of the Existing Combination Product Patent.

(ii) Whenever permitted by Applicable Law, and subject to the mutual written consent of both Parties (not to be unreasonably withheld), BN shall divide the Existing Combination Product Patent claims into separate patent applications such that patent application(s) Covering PROSTVAC combinations can be prosecuted independently of claims that Cover molecules or products other than in combination with PROSTVAC in all countries in the Territory where such patent applications have been filed. Any patent applications that Cover PROSTVAC combinations shall thereafter be excluded from the definition of Existing Combination Product Patent and included in the definition of Non-Combination Product Specific Patents, and, for clarity, any such patent applications that do not Cover PROSTVAC shall thereafter no longer be considered a BN Patent or Existing Combination Product Patent.

(iii) If BN elects not to Prosecute in any country the Existing Combination Product Patent pursuant to Section 9.2(d)(i), BN will give BMS at least [***]

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

[***] notice before any relevant deadline and provide to BMS information it reasonably requests relating to the Existing Combination Product Patent. BMS will then have the right to assume responsibility, using patent counsel of its choice, for the Prosecution of the Existing Combination Product Patent. If BMS assumes responsibility for the Prosecution for the Existing Combination Product Patent as set forth above, then the Patent Prosecution Costs incurred by BMS in the course of such Prosecution will thereafter be borne by BMS.

(iv) The Parties will cooperate in Prosecution of the Existing Combination Product Patent in all respects, to the extent the same relates to or could reasonably be expected to impact claims Covering PROSTVAC. Each Party will provide the other Party all reasonable assistance and cooperation in such Prosecution efforts as the other Party may reasonably request from time to time, including providing any necessary powers of attorney and executing any other required documents or instruments for such Prosecution, all at the requesting Party’s sole expense. Each Party will provide the other Party with copies of any documents it receives, files or submits in connection with such Prosecution and will inform the other Party of the progress of it. Before filing in connection with such Prosecution any document with a patent office, each Party will provide a copy of the document to the other Party sufficiently in advance to enable the other Party to comment on it, and the first Party will give due consideration to such comments. For clarity, each Party will bear its own internal costs (i.e., those costs that are not Patent Prosecution Costs) with respect to its Prosecution activities for the Existing Combination Product Patent.

9.3 Patent Term Adjustments or Extensions. As of the Effective Date, the Parties have agreed to seek a patent term adjustment, patent term extension, supplementary patent protection and/or related extension of rights with respect to the Patent Term Extension Patent, and agree not to seek any such adjustment, extension or protection for any other Patent Covering the Product unless they mutually agree. As between the Parties and subject to the PHS License Agreement, BMS (by itself or through its Affiliates) shall have the sole right to apply for any such adjustment, extension or protection for any Product Specific Patent in respect of the Product. BN covenants that neither it nor its Affiliates will seek, and neither it nor its Affiliates will consent to any Existing Product Agreement Licensor seeking, patent term extensions, supplementary protection certificates, or similar rights or extensions in respect of the Product for the Product Specific Patents other than the Patent Term Extension Patent without the prior written consent of BMS. Each Party will cooperate fully with and provide all reasonable assistance to the other Party and use all commercially reasonable efforts consistent with its obligations under Applicable Law (including any applicable consent order or decree) in connection with obtaining any such adjustments or extensions for the Product Specific Patents consistent with such strategy. To the extent reasonably and legally required in order to obtain any such adjustment or extension in a particular country, each Party will make available to the other a copy of the necessary documentation to enable such other Party to use the same for the purpose of obtaining the adjustment or extension in such country.

9.4 Data Exclusivity. As applicable, BMS (by itself or through its Affiliates) will, after the License Effective Date, have the sole right and authority for securing, maintaining and enforcing exclusivity rights with respect to a Product in the Field that may be available under Applicable Law in a country, such as any data, market, pediatric, orphan drug or other regulatory

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

exclusivity periods. BMS shall not consent, during the Initial TC Term, to the use of or any cross reference to PROSTVAC-related data generated by BN or BMS or held by any Regulatory Authority for the purpose of a Third Party gaining Regulatory Approval for a product (other than PROSTVAC or a Companion Diagnostic) that encodes PSA in any country in the Territory without BN’s prior written consent, not to be unreasonably withheld or conditioned; except that BMS may, without BN’s prior written consent, consent to a Third Party’s use of or cross reference to such data solely for the development, Regulatory Approval and Commercialization of such Third Party’s product in combination use with PROSTVAC (but not as a fixed dose combination product). BN will cooperate fully with and provide all reasonable assistance to BMS and use all commercially reasonable efforts consistent with its obligations under Applicable Law (including any applicable consent order or decree) to seek, maintain and enforce all data exclusivity periods available for the Products.

9.5 Prosecution of Certain Other Patents.

(a) Joint Patents That Are Not BN Patents. This Section 9.5(a) will apply only to Joint Patents that are not BN Patents. BMS (by itself or through its Affiliates) will have the first right, but not the obligation, to Prosecute in all jurisdictions all Joint Patents that are not BN Patents in the name of the Parties. If BMS determines in its sole discretion to abandon, cease prosecution of or otherwise not file or maintain any such Joint Patent in any jurisdiction, then BMS will provide BN written notice of such determination at least [***] before any deadline for taking action to avoid abandonment (or other loss of rights) and will provide BN with the opportunity to prepare, file, prosecute and maintain such Joint Patent in such jurisdiction. The Party that is responsible for Prosecuting a particular Joint Patent (the “Prosecuting Party”) will provide the other Party reasonable opportunity to review and comment on such prosecution efforts regarding such Joint Patent, and such other Party will provide the Prosecuting Party reasonable assistance in such efforts. The Prosecuting Party will provide the other Party with a copy of all material communications from any patent authority in the applicable jurisdictions regarding such Joint Patent being prosecuted by such Party, and will provide the other Party drafts of any material filings or responses to be made to such patent authorities a reasonable amount of time in advance of submitting such filings or responses so that such other Party may have an opportunity to review and comment thereon. In particular, each Party agrees to provide the other Party with all information necessary or desirable to enable the other Party to comply with the duty of candor/duty of disclosure requirements of any patent authority. Unless the Parties agree otherwise, each Party will bear its own internal costs and the Patent Prosecution Costs that it incurs with respect to the Prosecution of such Joint Patents that are not BN Patents.

(b) Other BN Patents. BN will have the first right and authority with respect to Prosecution of all Other BN Patents (including those set forth in Exhibit A2) in any jurisdiction. BN will be responsible for all costs incurred by it (including all Patent Prosecution Costs) in the course of Prosecuting and enforcing such Other BN Patents. If BN elects not to Prosecute in any country any Other BN Patent, BN will give BMS at least [***] notice before any relevant deadline and provide to BMS information it reasonably requests relating to the Other BN Patent. BMS (by itself or through its Affiliates) will then have the right to assume responsibility, using patent counsel of its choice, for the Prosecution of such Other BN

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Patent in BN’s or the Existing Product Agreement Licensor’s name as appropriate. If BMS assumes responsibility for the Prosecution for any such Other BN Patent as set forth above, then the Patent Prosecution Costs incurred by BMS in the course of such Prosecution will thereafter be borne by BMS. BN will provide all reasonable assistance and cooperation in such Prosecution efforts as BMS may reasonably request from time to time.

9.6 Infringement of BN Patents by Third Parties.

(a) Notification. The Parties will promptly notify each other of any actual, threatened, alleged or suspected infringement in the Field by a Third Party (an “Infringement”) of the BN Patents of which it becomes aware. A notice under 42 U.S.C. 262(l) (however such section may be amended from time to time during the Term) with respect to a Product will be deemed to describe an act of Infringement, regardless of its content. As permitted by Applicable Law, each Party will promptly notify the other Party in writing of any such Infringement of which it becomes aware, and will provide notice of the facts and circumstances that such Party believes support a claim of Infringement. In particular, each Party will notify and provide the other Party with copies of any written allegations of patent invalidity, unenforceability or non-infringement of any BN Patents Covering a Product (including methods of use or manufacture thereof). Such notification and copies will be provided by the Party receiving such allegations to the other Party as soon as practicable and, unless prohibited by Applicable Law, within no more than [***] after the receiving Party receives such allegations in writing. Such notification and copies will be sent by facsimile and overnight courier to BMS at the address set forth below, and to BN at the address specified in Section 16.5.

Bristol-Myers Squibb Company
P.O. Box 4000
Route 206 & Province Line Road
Princeton, New Jersey 08543-4000
Attention: Vice President and Chief Intellectual Property Counsel
Telephone: 609-252-4825
Facsimile: 609-252-4526

(b) From and after the License Effective Date, subject to the Existing Product Agreements and in particular the rights of PHS under the PHS License Agreement, BMS (by itself or through its Affiliates) will have the first right, but not the obligation, to bring and control, at its expense, an appropriate suit or other action before any government or private tribunal (an “Infringement Action”) against any person or entity allegedly engaged in any Infringement of any Non-Combination Product Specific Patent to remedy the Infringement (or to settle or otherwise secure the abatement of such Infringement) in the Field (a “Product Specific Infringement Action”). The foregoing right of BMS shall include the right to perform all actions of a reference product sponsor set forth in 42 USC 262(l). BN will have the right, at its own expense and by counsel of its choice, to be represented in any Product Specific Infringement Action. At BMS’s request, BN will join any Product Specific Infringement Action as a party and will use commercially reasonable efforts to cause any applicable Existing Third Party Licensor to join such Product Specific Infringement Action as a party if doing so is necessary for the purposes of establishing standing or is otherwise required by Applicable Law to pursue such action. BMS will have a period of [***] after its receipt or delivery of notice and

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

evidence pursuant to Section 9.6(a) to elect to so enforce such Product Specific Patents in the applicable jurisdiction (or to settle or otherwise secure the abatement of such Infringement), provided, however, that such period will be more than [***] to the extent Applicable Law prevents earlier enforcement of such Product Specific Patents (such as the enforcement process set forth in 42 USC 262(l)) and such period will be less than [***] to the extent that a delay in bringing an action to enforce the applicable Product Specific Patents against such alleged Third Party infringer would limit or compromise the remedies (including monetary and injunctive relief) available against such alleged Third Party infringer. In the event BMS does not so elect (or settle or otherwise secure the abatement of such Infringement) within the aforementioned period of time, it will so notify BN in writing and in the case where BN then desires to commence a suit or take action to enforce the applicable Product Specific Patents with respect to such Infringement in the applicable jurisdiction, the Parties will confer and upon BMS’s prior written consent (such consent not to be unreasonably withheld, conditioned or delayed), BN will have the right to commence a Product Specific Infringement Action to enforce the applicable Product Specific Patents, at BN’s expense. Each Party will provide to the Party enforcing any such rights under this Section 9.6(b) reasonable assistance in such enforcement, at such enforcing Party’s request and expense, including joining such action as a party plaintiff if doing so is necessary for the purposes of establishing standing or is otherwise required by Applicable Law to pursue such action. The enforcing Party will keep the other Party regularly informed of the status and progress of such enforcement efforts, and will reasonably consider the other Party’s comments on any such efforts.

(c) Settlement. Without the prior written consent of the other Party (not to be unreasonably withheld, conditioned or delayed), neither Party will settle any Product Specific Infringement Action in any manner that would adversely affect a Product Specific Patent or that would limit or restrict the ability of BMS (or its Affiliates or Sublicensees, as applicable) to sell Products anywhere in the Territory. Any settlement shall be subject to the provisions of the PHS License Agreement; provided, however that BN shall use Diligent Efforts to obtain PHS’s agreement that BMS shall have the first right to settle, subject to PHS’s consent to the terms of the settlement, any Product Specific Infringement Action that may occur for which BMS is the enforcing Party provided always that such efforts shall not require BN to pay any money to PHS unless the same is reimbursed by BMS.

(d) Expenses and Recoveries. A Party bringing a Product Specific Infringement Action under this Section 9.6 against any Third Party engaged in Infringement of the Product Specific Patents will be solely responsible for any expenses incurred by such Party as a result of such Product Specific Infringement Action. If such Party recovers monetary damages from such Third Party in such Product Specific Infringement Action, such recovery will first be applied to all out-of-pocket costs and expenses incurred by the Parties in connection therewith, including attorneys’ fees. [***].

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(e) Infringement of BN Patents Outside of Product Specific Infringement Actions. BN will have the first right, but not the obligation, to bring and control, at its expense, an Infringement Action against any person or entity allegedly engaged in any Infringement of any BN Patent (other than an Infringement of any Non-Combination Product Specific Patent in the Field) to remedy the Infringement (or to settle or otherwise secure the abatement of such Infringement) (an “Other Infringement Action”). BN will have a period of [***] after its receipt or delivery of notice and evidence pursuant to Section 9.6(a) to elect to so enforce such BN Patents in the applicable jurisdiction (or to settle or otherwise secure the abatement of such Infringement), provided, however, that such period will be more than [***] to the extent Applicable Law prevents earlier enforcement of such BN Patents (such as the enforcement process set forth in 42 U.S.C. 262(l)) and such period will be less than [***] to the extent that a delay in bringing an action to enforce the applicable BN Patents against such alleged Third Party infringer would limit or compromise the remedies (including monetary and injunctive relief) available against such alleged Third Party infringer. If BN brings an Other Infringement Action with respect to the Existing Combination Product Patent, BN will keep BMS regularly informed of the status and progress of, and will reasonably consider BMS’s comments on, such enforcement effort. In the event BN does not elect to bring an Other Infringement Action (or settle or otherwise secure the abatement of such Infringement) within the aforementioned period of time, it will so notify BMS in writing and in the case where BMS then desires to commence a suit or take action to enforce the applicable BN Patents with respect to such Infringement in the applicable jurisdiction, the Parties will confer and, upon BN’s prior written consent (such consent not to be unreasonably withheld, conditioned or delayed), BMS (itself or through its Affiliates) will have the right to commence an Other Infringement Action to enforce the applicable BN Patents, at BMS’s expense provided always that for the avoidance of doubt BMS shall have no right to bring any Infringement Action in respect of activities outside the Field without BN’s prior written consent. BN will provide to BMS reasonable assistance in such Other Infringement Action, at BMS’s request and expense, including joining such action as a party plaintiff if required by Applicable Law to pursue such action. BMS will not settle any Other Infringement Action in any manner that would adversely affect a BN Patent without the prior written consent of BN (not to be unreasonably withheld, conditioned or delayed). [***].

9.7 Infringement of Joint Patents that are not BN Patents.

(a) BMS (by itself or through its Affiliates) will have the right, but not the obligation, to bring at its expense an appropriate suit or other action against any Third Party allegedly engaged in any Infringement of Joint Patents that are not BN Patents. BMS will have a period of [***] after its receipt or delivery of notice of such Infringement to elect to so enforce such Joint Patent (or to settle or otherwise secure the abatement of such Infringement); provided, however, that such period will be more than [***] to the extent Applicable Law prevents earlier enforcement of such Joint Patents (such as the enforcement process set forth in 42 U.S.C. 262(l)) and such period will be less than [***] to the extent that a delay in bringing an action to

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

enforce the applicable Joint Patents against such alleged Third Party infringer would limit or compromise the remedies (including monetary and injunctive relief) available against such alleged Third Party infringer. In the event BMS does not so elect (or settle or otherwise secure the abatement of such Infringement), it will so notify BN in writing and in the case where BN then desires to commence a suit or take action to enforce the applicable Joint Patents with respect to such infringement, the Parties will confer and BN will have the right to commence such a suit or take such action to enforce the applicable Joint Patents, at BN’s expense, subject to BMS’s prior written consent, not to be unreasonably withheld, conditioned or delayed. Each Party will provide to the Party enforcing any such rights under this Section 9.7 reasonable assistance in such enforcement, at such enforcing Party’s request and expense, including joining such action as a party plaintiff if required by Applicable Law to pursue such action. The enforcing Party will keep the other Party regularly informed of the status and progress of such enforcement efforts, and will reasonably consider the other Party’s comments on any such efforts.

(b) Without the prior written consent of the other Party (not to be unreasonably withheld, conditioned or delayed), neither Party will settle any claim, suit or action that it may bring with respect to a Joint Patent that is not an BN Patent.

(c) A Party bringing a claim, suit or action under this Section 9.7 against any Third Party engaged in Infringement of any Joint Patent that is not a BN Patent will be solely responsible for any expenses incurred by such Party as a result of such claim, suit or action. If such Party recovers monetary damages from such Third Party in such suit or action, such recovery will first be applied to all out-of-pocket costs and expenses incurred by the Parties in connection therewith, including attorneys’ fees. [***].

9.8 Reexaminations, Oppositions and Related Actions.

(a) The Parties will promptly notify each other in the event that any Third Party files, or threatens to file, any paper in a court, patent office or other government entity, seeking to invalidate, reexamine, oppose or compel the licensing of any Product Specific Patent (any such Third Party action being a “Patent Challenge”).

(b) From and after the License Effective Date, subject to the PHS License Agreement and in particular the rights of PHS under the PHS License Agreement, BMS (by itself or through its Affiliates) will have the first right to bring and control, at its expense, any effort in defense of such a Patent Challenge against a Non-Combination Product Specific Patent, except in the case where such Patent Challenge is made in connection with an Infringement Action, in which case the enforcing Party in the Infringement Action will have the first right to bring and control the defense of such Patent Challenge and such Patent Challenge will be considered part of the Infringement Action under this Article 9. In the case where BMS controls the defense of such Patent Challenge, BN will have the right, at its own expense and by counsel of its choice, to

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

be represented in any such effort. If BMS fails to take action to defend such Patent Challenge within [***] prior to the time limit for bringing such defense (or within such shorter period to the extent that a delay in bringing such defense would limit or compromise the outcome of such defense of such Patent Challenge), then BN will have the right, but not the obligation, to bring and control any effort in defense of such Patent Challenge at its own expense.

(c) BN will have the first right to bring and control, at its expense, any effort in defense of such a Patent Challenge related to the Existing Combination Product Patent or any Other BN Patent, except in the case where such Patent Challenge is made in connection with an Infringement Action, in which case the enforcing Party in the Infringement Action will have the first right to bring and control the defense of such Patent Challenge and such Patent Challenge will be considered part of the Infringement Action under this Article 9. In the case where BN controls the defense of such Patent Challenge, BMS (by itself or through its Affiliates) will have the right, at its own expense and by counsel of its choice, to be represented in any such effort. If BN fails to take action to defend such Patent Challenge within [***] prior to the time limit for bringing such defense (or within such shorter period to the extent that a delay in bringing such defense would limit or compromise the outcome of such defense of such Patent Challenge), then BMS (by itself or through its Affiliates) will have the right, but not the obligation, to bring and control any effort in defense of such Patent Challenge at its own expense.

9.9 Third Party Rights.

(a) The Parties will promptly notify each other of any written allegation that any activity pursuant to this Agreement infringes the Patent rights of any Third Party.

(b) Subject to Sections 9.9(c), 9.9(d) and 9.9(e), with respect to any Third Party Patent under Section 9.9(a), BMS (by itself or through its Affiliates) will have the first right to control, at its expense subject to Section 8.5(b)(ii), obtaining a license with respect to such Third Party Patent that Covers the composition, formulation, method of use and/or method of manufacture of any Product. Subject to Sections 9.9(c), 9.9(d) and 9.9(e), in the case where BMS elects not to obtain such a license, BN shall have the right to pursue obtaining a license with respect to such Third Party Patent at its own expense and upon BMS’s written consent (not to be unreasonably withheld). For the avoidance of doubt, where the relevant Patent Covers any activity that BN is obliged to undertake under this Agreement or the Supply Agreement and BMS does not consent to the taking of a license or agree to indemnify BN against claims that such activities infringe such Patent, BN shall be relieved of such obligation until such time that BMS consents to a license and the license is granted or BMS agrees to indemnify BN against claims that such activities infringe such Patent.

(c) Notwithstanding the foregoing, in the case a claim of infringement of a Patent is brought against a Party in a suit or other action or proceeding with respect to any Third Party Patent under Section 9.9(a), such Party will have the right, at its own expense and by counsel of its own choice, to prosecute and defend any such claim in such suit or other action or proceeding. If both Parties are named, the Parties shall consult with one another and cooperate with respect to such suit or other action or proceeding.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(d) Without the prior written consent of the other Party (not to be unreasonably withheld, conditioned or delayed), neither Party will settle any claim under this Section 9.9 in any manner that would (i) limit or restrict the ability of BMS (or its Affiliates or Sublicensees, as applicable) to sell Products anywhere in the Territory or (ii) impose any obligation, restriction or limitation on the other Party.

(e) The Parties will cooperate in all respects with one another in prosecuting or defending any action pursuant to this Section 9.9.

9.10 Disclosure of Inventions. Each Party will promptly disclose to the other Party all invention disclosures submitted to such Party by its or its Affiliates’ employees describing Joint Inventions and Sole Inventions. Each Party will also respond promptly to reasonable requests from the other Party for more Information relating to such inventions.

9.11 Patent Contacts. Each Party will designate a patent counsel representative who will be responsible for coordinating the activities between the Parties in accordance with this Article 9 (each a “Patent Contact”). Each Party will designate its initial Patent Contact within [***] following the Effective Date and will promptly thereafter notify the other Party of such designation. If at any time a vacancy occurs for any reason, the Party that appointed the prior incumbent will as soon as reasonably practicable appoint a successor. Each Party will promptly notify the other Party of any substitution of another person as its Patent Contact. The Patent Contacts will, from time to time, coordinate the respective patent strategies of the Parties relating to this Agreement. In particular the Patent Contacts will review and update the list of BN Patents from time to time to ensure that all BN Patents are listed.

9.12 Employee Obligations. Prior to receiving any Confidential Information or beginning work under this Agreement relating to any research, Development or Commercialization of a Product, each employee of BMS or BN or of either Party’s respective Affiliates will be bound in writing by non-disclosure and invention assignment obligations which are consistent with the obligations of BMS or BN under this Agreement.

9.13 Agent and Independent Contractor Obligations. Each Party also will use Diligent Efforts to ensure that each of its authorized agents and independent contractors, before receiving any Confidential Information or performing work under this Agreement relating to any research, Development or Commercialization of a Product, is bound in writing by non-disclosure and invention assignment obligations which are consistent with the obligations of BMS or BN, as applicable, under this Agreement (provided that where necessary (a) such Party will use Diligent Efforts to obtain the authorized agent’s or independent contractor’s agreement to grant such Party an exclusive license with the right to grant sublicenses with respect to resulting inventions and Patents (or a nonexclusive, sublicensable license with an option to obtain such exclusive, sublicensable license) and (b) the period of time with respect to non-disclosure obligations may be shorter, but such Party will use Diligent Efforts to ensure it is no shorter than [***] from the effective date of the written obligation). Each Party shall be responsible for satisfying any obligation to compensate such Party’s employees, authorized agents and independent contractors for such invention assignments. For the avoidance of doubt, it is agreed that NIH and its employees and agents shall not be considered as the agents or contractors of BN for the purposes of this Section 9.13.

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

9.14 Patents Licensed from Third Parties. BMS has had the opportunity to perform due diligence on the Existing Product Agreements and it accepts that the rights granted under this Agreement are subject to those agreements.

9.15 Product Marks and Marking. Subject to the provisions of Section 5.1(j), BMS (by itself or through its Affiliates) shall be responsible for the selection, registration, maintenance, enforcement and defense of all Product Marks used in connection with the sale or marketing of Products in the Field in the Territory, as well as all expenses associated therewith incurred after the License Effective Date by BMS or by BN at BMS’s request. Following the License Effective Date, BN shall assign to BMS all of BN’s rights, title, interests and goodwill in any such Product Marks previously obtained by BN where BMS has requested the assignment of such Product Mark to it. For the avoidance of doubt, BMS is not responsible for the registration, maintenance, enforcement and/or defense of the PROSTVAC Mark. All uses of the Product Marks shall comply with all Applicable Law (including those laws and regulations particularly applying to the proper use and designation of trademarks in the applicable countries). BMS agrees to mark all Products or their packaging sold in the United States with all applicable U.S. patent numbers and similarly to indicate “Patent Pending” status where and to the extent required by Applicable Law or any Existing Product Agreement. All Products manufactured in, shipped to, or sold in other countries shall be marked in a manner to preserve BN’s and each of its Existing Product Agreement Licensor’s patent rights in those countries. Neither Party shall, without the other Party’s prior written consent, use any trademarks or other marks of the other Party (including the other Party’s corporate name), trademarks, advertising taglines or slogans confusingly similar thereto, for any purpose, except as may be expressly authorized in writing in connection with activities under this Agreement and except to the extent required to comply with Applicable Law.

9.16 Further Action. Each Party will, upon the reasonable request of the other Party, provide such assistance and execute such documents as are reasonably necessary for such Party to exercise its rights and perform its obligations pursuant to this Article 9; provided, however, that neither Party will be required to take any action pursuant to Article 9 that such Party reasonably determines in its sole judgment and discretion conflicts with or violates any applicable court or government order or decree or Applicable Law.

10. EXCLUSIVITY; OTHER PRODUCTS

10.1 Competing Products. Each Party covenants that, during the period commencing on the Effective Date and ending on the earlier of (a) the period [***] after the License Effective Date or (b) termination of this Agreement (the “Exclusivity Period”), neither it nor its Affiliates will, directly or indirectly, work independently of this Agreement for itself or any other Person (including by the grant of any license or option to any Third Party) to clinically develop (other than Phase 1 studies) or commercialize any product containing [***] (a “Competing Product”).

10.2 Additional Product Option. BN shall, or shall procure that BNInc shall, grant to BMS an exclusive first right to negotiate the inclusion of the product known as of the Effective

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Date as MVA-BN®PRO in the terms of this Agreement by licensing to BMS the rights to such vaccine, on the following basis:

(a) Prior to the completion of the first phase 1 study of MVA-BN®PRO to be commenced after the License Effective Date and for [***] after the delivery to BMS of the draft study report containing the outcome of such phase 1 study (collectively, the “FRON Period”), BN shall not and shall cause its Affiliates not to, engage in, solicit, initiate, encourage, seek, entertain or enter into any discussion, negotiation or agreement with any Third Party relating to the license or acquisition by any Third Party of any interest or right (including any ownership interest, option or license right) in MVA-BN®PRO.

(b) At any time during the FRON Period BMS may serve notice on BN that it would like to exercise the first right of negotiation for the inclusion of MVA-BN®PRO in the scope of this Agreement, subject to the agreement in writing of any amendments necessary to this Agreement to effect such inclusion. Such notice shall include a term sheet setting out BMS’s proposal on the following points:

(i) responsibility for future development activities of MVA-BN®PRO;

(ii) an outline development plan for MVA-BN®PRO; and

(iii) financial provisions for the inclusion of MVA-BN®PRO to include any proposed signature payment, percentage of Net Sales compensation, milestones and responsibility for development costs.

(c) On receipt of such notice the Parties shall enter into good faith negotiations for the basis on which MVA-BN®PRO shall be included in the terms of this Agreement and for a period of [***] after the date on which the FRON Period expired, BN shall not and shall cause its Affiliates not to, engage in, solicit, initiate, encourage, seek, entertain or enter into any discussion, negotiation or agreement with any Third Party relating to the license or acquisition by any Third Party of any interest or right (including any ownership interest, option or license right) in MVA-BN®PRO. In the event that the Parties have not agreed the basis on which MVA-BN®PRO shall be included in the terms of this Agreement by the date that is [***] after the expiration of the FRON Period, then BN shall be free to offer MVA-BN®PRO to and negotiate the terms on which it is to be licensed to any Third Party without further reference to BMS; provided, however, that BN and its Affiliates may not, for a period of [***] after expiration of the FRON Period, offer or license MVA-BN®PRO to any Third Party on terms that are financially materially more favorable to such Third Party (vis-à-vis BMS) than the last terms offered by BMS to BN.

10.3 Restricted Products. Notwithstanding Section 10.1, if BMS or any of its Affiliates, either through its own efforts or by acquisition, obtains ownership of or a license to, or is acquired by or otherwise merges with an entity that owns or has a license to, a Competing Product that is in clinical development, in all such cases that would result in a violation of Section 10.1 above with respect to a particular Region (each such Competing Product that would

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

lead to such a violation being a “Restricted Product”), then BMS or its Affiliate shall promptly notify BN in writing and elect one of the following actions:

(a) divest itself of such Restricted Product (if such Restricted Product is already being commercialized at the time of acquisition) in such Region and notify BN in writing of such divestiture, which divestiture may occur by an outright sale to a Third Party of all of BMS’s and its Affiliate’s rights to such Restricted Product or by an outlicense arrangement under which BMS has no continuing active involvement in the development or commercialization of such Restricted Product (for clarity, efforts in connection with (i) the receipt and audit of payments in respect of the Restricted Product, (ii) the maintenance, defense and enforcement of any applicable licensed patents, and (iii) the receipt of information to ensure compliance with the applicable agreement (including efforts to enforce or terminate same, or seek damages, for breach) shall not constitute continuing active involvement) (provided that such divestiture occurs within [***] after obtaining such ownership or license, or being acquired by or merging with an entity that has such ownership or license; provided further that BMS or its Affiliate shall have an additional [***] to effect such divestiture in the event that BMS or its Affiliate merged with an entity having such ownership or license and can demonstrate it has used commercially reasonable efforts, but has been unable, to effect such divestiture during the [***] after such merger);

(b) provide BN with notice of termination of this Agreement as to such Region pursuant to Section 12.2(a); or

(c) if the Parties can agree, within [***] after a product becomes a Restricted Product, on the terms (including compensation) for including the Restricted Product within this Agreement, agree that the Restricted Product shall be deemed a Product hereunder, including for purposes of Article 8 and BMS’s Diligent Efforts obligations under Sections 5.2(a) and 7.1.

10.4 Prostate Cancer Products. If BN or any of its Affiliates develops, either alone or in conjunction with any Third Party, or acquires any rights to any product (other than PROSTVAC) for the treatment of prostate cancer that is in phase III development or later, then (a) the JC shall be dissolved upon BMS’s written notice and (b) BMS shall have no obligation to provide any Commercialization and Development Plan, or any Commercialization report pursuant to Section 7.3.

10.5 Companion Diagnostics. BMS and its Affiliates may elect to Develop, either alone or in conjunction with any Third Party, one or more Companion Diagnostic. The Parties will discuss in good faith the role and responsibility that BN may have in connection with the Development of such Companion Diagnostics including whether BN will make available for BMS’s use in connection with same, subject to applicable privacy laws and the terms under which same were provided to BN, any patient samples and related clinical data and other materials possessed and Controlled by BN. BN agrees not to Develop or Commercialize any Companion Diagnostic unless the JC (or BMS, in the absence of the JC) has agreed for it to do so, including the basis, scientific rationale, and financial and other terms for BN’s Development and/or Commercialization of a Companion Diagnostic, in which case the decision of the JC shall govern BN’s Development and/or Commercialization of such Companion Diagnostic. BN shall

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

retain operational control of any such Development and Commercialization authorized by the JC subject to the decisions of the JC. BMS and its Affiliates will not, directly or indirectly, Commercialize any Companion Diagnostic (but may Develop though Regulatory Approval a Companion Diagnostic on its own or in collaboration with, or via a sublicense to, a Third Party), unless and until agreed by the JC (with neither Party having the final say). [***]. If BMS enters into an agreement with a Third Party granting such Third Party the right to Commercialize a Companion Diagnostic that was Developed using samples or data provided by BN, then BMS will pay BN [***] percent ([***]%) of any amounts BMS or its Affiliates receives from such Third Party in connection with sales of such Companion Diagnostics, once BMS has recovered any out-of-pocket expenses incurred in the development of such Companion Diagnostic; provided that BMS shall provide BN with reasonable documentation of any such expenses following BN’s request.

11. CONFIDENTIALITY

11.1 Confidentiality. Except to the extent expressly authorized by this Agreement or otherwise agreed in writing by the Parties, each Party (the “Receiving Party”) agrees that, for the Term and for [***] thereafter, it shall keep confidential and shall not publish or otherwise disclose and shall not use for any purpose other than as provided for in this Agreement (which includes the exercise of any rights or the performance of any obligations hereunder) any Confidential Information furnished to it by the other Party (the “Disclosing Party”) pursuant to this Agreement, provided that the foregoing shall not apply to that portion of such Information that the Receiving Party can demonstrate by competent written proof:

(a) was already known to the Receiving Party or any of its Affiliates, other than under an obligation of confidentiality to the Disclosing Party, at the time of disclosure by the other Party;

(b) was generally available to the public or otherwise part of the public domain at the time of its disclosure to the Receiving Party;

(c) became generally available to the public or otherwise part of the public domain after its disclosure and other than through any act or omission of the Receiving Party in breach of this Agreement;

(d) is subsequently disclosed to the Receiving Party or any of its Affiliates by a Third Party without obligations of confidentiality to the Disclosing Party with respect thereto; or

(e) is subsequently independently discovered or developed by the Receiving Party or its Affiliate without the aid, application, or use of Confidential Information of the Disclosing Party.

All Information generated by either Party in the Development of a Product after the Effective Date or licensed to BMS hereunder shall, notwithstanding that it is owned by and confidential to the creating Party, be kept confidential by the Parties subject to the same rights (including the right to publish) and obligations that it has under this Article 11 in respect of Confidential Information of that Party.

11.2 Authorized Disclosure. Notwithstanding Section 11.1, each Party may disclose Confidential Information belonging to the other Party to the extent such disclosure is reasonably necessary in the following situations:

(a) filing or prosecuting Patents in accordance with Article 9;

(b) subject to Section 11.3, regulatory filings and other filings with Governmental Authorities (including Regulatory Authorities), including filings with the FDA, as necessary for the Development or Commercialization of a Product, as required in connection with any filing, application or request for Regulatory Approval; provided, however, that reasonable measures will be taken to assure confidential treatment of such information;

(c) prosecuting or defending litigation;

(d) complying with Applicable Law, including regulations promulgated by securities exchanges;

(e) subject to Section 11.3, complying with Applicable Law, including regulations promulgated by securities exchanges;

(f) disclosure to its Affiliates, employees, agents, independent contractors, licensors and any Sublicensees of the BN Technology only on a need-to-know basis and solely in connection with the performance of this Agreement, provided that each disclosee must be bound by obligations of confidentiality and non-use at least as equivalent in scope as and no less restrictive than those set forth in this Article 11 prior to any such disclosure;

(g) disclosure of the material terms of this Agreement (or a redacted copy of this Agreement) to any bona fide potential or actual investor, stockholder, investment banker, acquirer, merger partner or other potential or actual financial partner or their agents; provided that each disclosee must be bound by obligations of confidentiality and non-use at least as equivalent in scope as and no less restrictive than those set forth in this Article 11 prior to any such disclosure;

(h) disclosure of the stage of Development of Products under this Agreement to any bona fide potential or actual investor, stockholder, investment banker, acquirer, merger partner or other potential or actual financial partner; provided that each disclosee must be bound by obligations of confidentiality and non-use at least as equivalent in scope as and no less restrictive than those set forth in this Article 11 prior to any such disclosure;

(i) disclosure of certain blinded data generated under this Agreement to any bona fide potential or actual investor, stockholder, investment banker, acquirer, merger partner or

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

other potential or actual financial partner; provided that each disclosee must be bound by obligations of confidentiality and non-use at least as equivalent in scope as and no less restrictive than those set forth in this Article 11 prior to any such disclosure; and

(j) disclosure pursuant to Section 11.4.

Notwithstanding the foregoing, in the event a Party is required to make a disclosure of the other Party’s Confidential Information pursuant to Sections 11.2(a), 11.2(c) or 11.2(d), it will, except where impracticable, give reasonable advance notice to the other Party of such disclosure and use reasonable efforts to secure confidential treatment of such information. In any event, the Parties agree to take all reasonable action to avoid disclosure of Confidential Information hereunder.

Nothing in Sections 11.1 or 11.2 shall limit either Party in any way from disclosing to any Third Party such Party’s U.S. or foreign income tax treatment and the U.S. or foreign income tax structure of the transactions relating to such Party that are based on or derived from this Agreement, as well as all materials of any kind (including opinions or other tax analyses) relating to such tax treatment or tax structure, except to the extent that nondisclosure of such matters is reasonably necessary in order to comply with applicable securities laws.

11.3 Publicity; Terms of Agreement.

(a) The Parties agree that the terms and contents of this Agreement (including the Exhibits hereto) shall be treated as Confidential Information of both Parties, subject to the special authorized disclosure provisions set forth in Section 11.2 and this Section 11.3. Subject to Sections 11.3(b) and 11.3(d), neither Party shall make any public announcement regarding the execution or terms of this Agreement without the consent of the other Party in accordance with Section 11.3(c).

(b) The Parties have agreed to make public announcements of the execution of this Agreement substantially in the form of the press releases attached as Exhibit H hereto on or after the Effective Date.

(c) Except as set forth in Section 11.3(b), neither Party shall make a public announcement concerning the existence, terms and/or contents of this Agreement, except in the case of a press release or governmental filing required by Applicable Law (where reasonably advised by the disclosing Party’s counsel), in which event the disclosing Party shall provide the other Party with such advance notice as it reasonably can and shall not be required to obtain approval therefor. A Party commenting on such a proposed press release shall provide its comments, if any, within [***] (or within [***] in the event that such shorter period is required to comply with Applicable Law) after receiving the press release for review and the other Party shall give good faith consideration to same. BN shall have the right to make a press release announcing the achievement of each milestone under this Agreement as it is achieved, and the achievements of Regulatory Approvals as they occur including where it is relevant to BN’s obligations to ensure that the guidance it provides is not or has not become misleading BN may disclose the amounts that it expects to receive consequent on such event, subject to the review procedure set forth in the preceding sentence and following

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

discussion with BMS. In relation to BMS’s review of such an announcement, BMS may make specific, reasonable comments on such proposed press release within the prescribed time for commentary, but shall not withhold its consent to disclosure of the information that the relevant milestone or Regulatory Approval has been achieved and triggered a payment hereunder. Neither Party shall be required to seek the permission of the other Party to repeat any information regarding the terms of this Agreement that have previously been publicly disclosed by such Party, or by the other Party, in accordance with this Section 11.3. For clarity, neither Party shall disclose the financial terms of this Agreement without the prior written approval of the other Party, except as and to the extent otherwise expressly permitted under this Agreement or required by Applicable Law.

(d) The Parties acknowledge that either or both Parties may be obligated to file under Applicable Law a copy of this Agreement with the SEC or other Government Authorities. Each Party shall be entitled to make such a required filing, provided that it requests confidential treatment of at least the financial terms and sensitive technical terms hereof and thereof to the extent such confidential treatment is reasonably available to such Party. In the event of any such filing, each Party will provide the other Party with a copy of this Agreement marked to show provisions for which such Party intends to seek confidential treatment not less than [***] prior to such filing (and any revisions to such portions of the proposed filing a reasonable time prior to the filing thereof), and shall reasonably consider the other Party’s comments thereon to the extent consistent with the legal requirements, with respect to the filing Party, governing disclosure of material agreements and material information that must be publicly filed, and shall only disclose Confidential Information which it is advised by counsel or the applicable Governmental Authority is legally required to be disclosed. No such notice shall be required under this Section 11.3(d) if the substance of the description of or reference to this Agreement contained in the proposed filing has been included in any previous filing made by either Party hereunder or otherwise approved by the other Party.

(e) Each Party shall require each of its Affiliates and private investors to which Confidential Information of the other Party is disclosed as permitted hereunder to comply with the covenants and restrictions set forth in Sections 11.1 through Section 11.3 as if each such Affiliate and each such investor were a Party to this Agreement and shall be fully responsible for any breach of such covenants and restrictions by any such Affiliate or investor.

11.4 Publications. Neither Party shall publicly present or publish results of studies carried out under this Agreement (each such presentation or publication a “Publication”) without the opportunity for prior review by the other Party and, in the case of publications by BN, approval (not to be unreasonably withheld) by BMS, except to the extent otherwise required by Applicable Law, in which case Section 11.3 shall apply with respect to disclosures required by the SEC and/or for regulatory filings. The submitting Party shall provide the other Party the opportunity to review any proposed Publication at least [***] prior to the earlier of its presentation or intended submission for publication. The submitting Party agrees, upon request by the other Party, not to submit or present any Publication until the other Party has had [***] to comment on any material in such Publication. The submitting Party shall consider the comments of the other Party in good faith, but will retain the sole authority to submit the manuscript for Publication; provided that the submitting Party agrees to delay such Publication

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

as necessary to enable the Parties to file a Patent if such Publication might adversely affect such Patent. The submitting Party shall provide the other Party a copy of the Publication at the time of the submission or presentation. Notwithstanding the foregoing, BMS shall not have the right to publish or present BN’s Confidential Information without BN’s prior written consent, and BN shall not have the right to publish or present BMS’s Confidential Information without BMS’s prior written consent. Each Party agrees to acknowledge the contributions of the other Party, and the employees of the other Party, in all publications as scientifically appropriate. This Section 11.4 shall not limit and shall be subject to Section 11.5.

Nothing contained in this Section 11.4 shall prohibit the inclusion of information in a patent application claiming, and in furtherance of, the manufacture, use, sale or formulation of PROSTVAC, provided that the non-filing Party is given a reasonable opportunity to review, comment upon and/or approve the information to be included prior to submission of such patent application, where and to the extent required by Article 9.

Notwithstanding the foregoing, the Parties recognize that independent investigators have been engaged, and may be engaged in the future, to conduct Clinical Trials of the Product. The Parties recognize that such investigators operate in an academic environment and may release information regarding such studies in a manner consistent with academic standards; provided, that each Party will use reasonable efforts to prevent publication prior to the filing of relevant patent applications and to ensure that no Confidential Information of either Party is disclosed.

11.5 Termination of Prior CDA. This Agreement terminates, as of the Effective Date, the Prior CDA. All Confidential Information (as defined in the Prior CDA) exchanged between the Parties under the Prior CDA shall be deemed Confidential Information of the corresponding Party under this Agreement and shall be subject to the terms of this Article 11.

12. TERM AND TERMINATION

12.1 Term. This Agreement shall become effective on the Effective Date and, unless earlier terminated pursuant to this Article 12, shall continue until either: (a) the Option Term expires without exercise by BMS of the Option and cannot be reinstated or (b) following exercise of the Option, on a Product-by-Product and country-by-country basis until expiration of the TC Term (the “Term”).

12.2 Termination by BMS at Will or for Safety Reasons.

(a) Termination by BMS at Will. BMS may terminate this Agreement as a whole (at any time) or on a Region-by-Region (where the Regions are defined in Exhibit F Part B) and/or Product-by-Product basis (from and after the License Effective Date), effective upon [***] prior written notice to BN if the notice is given prior to the License Effective Date, [***] prior written notice to BN if such notice is given after the License Effective Date but prior to the First Commercial Sale of a Product in the Territory and on [***] prior written notice in all other cases. Where such termination occurs prior to the License Effective Date, the effect of such termination shall be as set forth in Section 12.6. Notwithstanding any such notice of termination under this Section 12.2(a) on or after the License Effective Date, any milestone payments under Section 8.4 will be due, and no milestone

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

payments under Sections 8.2 and 8.3 will be due, on milestones achieved during the period between the notice of termination and the effective date of termination, and the terms of Section 12.7 shall apply. BN shall have the right to accelerate the effective date of termination by providing BMS with at least [***] prior notice specifying such date. BMS shall have no Diligent Efforts obligations with respect to the Development and Commercialization of the terminated Product(s) and terminated Region(s) during the period between providing notice of termination and the effective date of termination under this Section 12.2(a), provided that (i) BMS will generally (subject to normal course limitations, including responding to safety issues) act consistently with the product reversion clauses set forth in Section 12.7 (i.e., manage Product activities (e.g., required regulatory filings, trademark and patent prosecution and maintenance, fulfillment of Product contracts and orders on a timely basis, etc.) in the normal course so that reversion can be effected upon termination), and (ii) if BMS has filed an application for Regulatory Approval, it will continue to use Diligent Efforts manage the application process during the notice period.

(b) Termination by BMS for Safety Reasons. BMS may terminate this Agreement on a Product-by-Product basis for the Territory as a whole only upon written notice to BN based on Safety Reasons. Notwithstanding any such notice of termination under this Section 12.2(b), any milestone payments under Section 8.4 will be due, and no milestone payments under Sections 8.2 and 8.3 will be due, on milestones achieved during the period between the notice of termination and the effective date of termination.

12.3 Termination by Either Party for Breach.

(a) (i) Prior to exercise of the Option, either Party may terminate this Agreement in its entirety in the event the other Party materially breaches this Agreement, and (ii) following exercise of the Option, either Party may terminate this Agreement (A) with respect to any Product (on a Product-by-Product basis) as to the entire Territory (where such breach affects such Product in all Regions), (B) with respect to any Region (on a Region-by-Region basis) (where such breach affects such Region), or (C) in its entirety (if such breach affects all Products in all Regions), in each case ((i)-(ii)) if such breach shall have continued for [***] (or, if such default cannot be cured within such [***] period, if the alleged breaching Party has not commenced within such [***] and diligently continued good faith efforts to cure such breach and achieved such cure by the expiry of [***] after such written notice) after written notice shall have been provided to the breaching Party by the non-breaching Party specifying the alleged breach and requiring such breach to be remedied and stating an intention to terminate if not so cured (a “Termination Notice”). Except as set forth in Section 12.3(b), any such termination shall become effective at the end of such [***] period unless the breaching Party has cured any such breach prior to the expiration of the [***] period (or, if such default cannot be cured within such [***] period, if the alleged breaching Party has not cured the breach within [***] after such written notice).

(b) If the alleged breaching Party disputes the existence or materiality of a breach specified in a Termination Notice provided by the other Party in accordance with Section 12.3(a), and such alleged breaching Party provides the other Party notice of such dispute within said [***]period after receiving such Termination Notice, then the non-breaching Party

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

shall not have the right to terminate this Agreement under Section 12.3(a) with respect to the applicable Product(s) or Region(s) unless and until, in accordance with Exhibit M, it has been finally decided that the alleged breaching Party has materially breached this Agreement with respect to such Product(s) or Region(s), subject to the following sentence. If the alleged breaching Party initiated such dispute in good faith, then, following such final decision, such Party shall have a final opportunity to cure such breach as follows: (i) any breach involving the failure to make a payment when due may be cured by paying such amount and applicable interest calculated in accordance with Section 8.13 within [***] following such final decision; and (ii) any other breach (other than BMS’s breach of its Diligence Efforts obligations with respect to the Development and Commercialization of Products) may be cured by such Party promptly taking the cure measures specified by the dispute resolution tribunal that made such final decision. It is understood and agreed that during the pendency of such dispute, all of the terms and conditions of this Agreement shall remain in effect and the Parties shall continue to perform all of their respective obligations hereunder.

(c) Following issuance of any Termination Notice, any milestone payments under Section 8.4 will be due, and no milestone payments under Sections 8.2 and 8.3 will be due, on any such milestones achieved after the date of the Termination Notice but prior to the effective date of termination, and BMS will pay to BN the applicable milestone payment due for each milestone so achieved as set forth in Section 8.4; provided, however that if the breach is disputed pursuant to Section 12.3(b) and such dispute is resolved in a manner in which no termination of this Agreement occurs, then upon such resolution BMS will promptly pay to BN the milestone payment for each milestone under Sections 8.2 and 8.3 achieved during the period between issuance of the Termination Notice and the resolution of such dispute.

(d) For purposes of this Section 12.3, a material breach of the Supply Agreement shall be considered to be a material breach of this Agreement for purposes of allowing the non-breaching Party to terminate this Agreement if the non-breaching Party terminates the Supply Agreement; provided, however, that any dispute as to whether a material breach of the Supply Agreement has occurred shall be resolved in accordance with the terms of the Supply Agreement and not as set forth in Section 12.3(b); and provided, further, that a material breach of the Supply Agreement shall not in and of itself entitle the non-breaching Party to damages under this Agreement unless the material breach under the Supply Agreement is, or results in, a breach hereunder for which the non-breaching Party would be entitled to damages hereunder and in such circumstances the non-breaching Party shall not be entitled to recover the same damages under both this Agreement and the Supply Agreement.

12.4 Termination by Either Party for Insolvency. A Party shall have the right to terminate this Agreement upon written notice if the other Party incurs an Insolvency Event; provided, however, in the case of any involuntary bankruptcy proceeding, such right to terminate shall only become effective if the Party that incurs the Insolvency Event consents to the involuntary bankruptcy or if such proceeding is not dismissed or stayed within [***] after the filing thereof. “Insolvency Event” means circumstances under which a Party (a) has a receiver or similar officer appointed over all or a material part of its assets or business; (b) passes a resolution for winding-up of all or a material part of its assets or business (other than a winding-up for the purpose of, or in connection with, any solvent amalgamation or

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

reconstruction) or a court enters an order to that effect; (c) has entered against it an order for relief recognizing it as a debtor under any insolvency or bankruptcy laws (or any equivalent order in any jurisdiction); (d) enters into any composition or arrangement with its creditors with respect to all or a material part of its assets or business (other than relating to a solvent restructuring); (e) ceases to carry on normal business operations; or (f) is unable generally to pay its debts as they become due in the ordinary course of business.

12.5 Limitations on Termination Remedy.

(a) Notwithstanding anything herein to the contrary, (i) in the event that BN terminates, or has the right to terminate, this Agreement pursuant to Section 12.3 with respect to a Product in the U.S., [***] and [***], then BN shall have the right to terminate this Agreement with respect to such Product in the entire Territory, (ii) BN shall not have the right to terminate this Agreement pursuant to Section 12.3 with respect to the Europe Region unless and until BN has such right to terminate this Agreement pursuant to Section 12.3 with respect to such Product with respect to any [***], and (iii) if BN terminates, or has the right to terminate this Agreement pursuant to Section 12.3 with respect to a Product with respect to any [***], then BN shall have the right to terminate this Agreement with respect to such Product in the entire Europe Region. BN may not terminate this Agreement pursuant to Section 12.3 as to any country in the Europe Region unless BN also has the right to terminate, and actually does terminate, this Agreement with respect to all of the Europe Region.

(b) Prior to the License Effective Date, BMS may only terminate this Agreement in respect of all Products in the entire Territory and shall not be permitted to terminate on a Product-by-Product or Region-by-Region basis prior to the License Effective Date.

12.6 Effects of Termination Prior to License Effective Date. Upon termination of this Agreement prior to the License Effective Date by either Party under Section 2.4, by BMS under Section 12.2, or by BN under Section 12.3(a) or Section 12.4, all rights in and to the Option under Article 2 shall terminate and BMS shall have no further rights in and to any Products.

12.7 Effects of Termination Following License Effective Date. Upon termination of this Agreement on or after the License Effective Date by BMS under Section 12.2 or by either Party under Section 12.3 or Section 12.4 (except as the application of such Sections may be limited as provided in a given subsection of this Section 12.7), the following shall apply with respect to the terminated Product(s) and terminated Region(s) (in addition to any other rights and obligations under this Agreement with respect to such termination):

(a) Licenses. The licenses granted to BMS in Section 4.1 shall terminate solely with respect to the Product(s) and Region(s) in which the termination becomes effective and BMS shall retain a non-exclusive, worldwide license under Section 4.1 to sell, offer for sale and import Products during the Commercialization Wind-Down Period in accordance with Section 12.7(b) (including the right to sell such Products through BMS Sublicensees if BMS were using such Sublicensees to sell same prior to such termination date). To the extent such

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

obligations existed prior to such termination, BMS shall not have any Diligent Efforts obligations after the effective date of termination with respect to the Development and Commercialization of the terminated Product(s) and terminated Region(s).

(b) Commercialization. BMS, its Affiliates and Sublicensees shall be entitled to continue to sell (but not to actively promote after the effective date of termination) any existing inventory of Products in each terminated Region of the Territory for which Regulatory Approval and all pricing and reimbursement approvals therefor have been obtained (provided that such Products shall have launched in each such terminated country as of the applicable effective date of termination), in accordance with the terms and conditions of this Agreement, for a period not to exceed [***] from the effective date of such termination (the “Commercialization Wind-Down Period”). Any Products sold or disposed of by BMS, its Affiliates or Sublicensees during the Commercialization Wind-Down Period shall be subject to the same Total Compensation under Section 8.5 as would have applied had this Agreement otherwise remained in force and effect with respect to such terminated Product(s) and terminated Region(s). After the Commercialization Wind-Down Period, BMS, its Affiliates and Sublicensees shall not sell such terminated Products in such terminated Region(s) or make any representation regarding BMS’s status as a licensee of such Product in such Region(s). Either (i) at the request of BN at the end of the Commercialization Wind-Down Period or (ii) prior to the end of the Commercialization Wind-Down Period, if BN has assumed responsibilities for regulatory activities under the Regulatory Approval, has received all clearances and Regulatory Approvals needed to sell and import the terminated Product in a given terminated country, and provides written notice to BMS that it wishes to assume sale of the terminated Product in a terminated country, then, in either case (i) or (ii), at BN’s election, BMS shall sell and transfer to BN such portion of the terminated Product inventory then held by BMS or its Affiliates which is in a saleable condition (including that it is undamaged, has been stored in proper conditions and has no less than [***] shelf-life remaining) as had been allocated to the terminated Region(s) [***]. This Section 12.7(b) shall not apply in the case of termination by BMS under Section 12.2(b) based on Safety Reasons.

(c) Supply. BN shall not be obliged under this Agreement or the Supply Agreement to supply any terminated Product for sale in the terminated Region(s) after the effective date of termination.

(d) Regulatory Materials. Upon BN’s written request, subject to Section 12.7(l), BMS shall assign and transfer, or cause to be assigned and transferred, to BN all Regulatory Materials (and shall assign to BN all related documentation transferred as set forth below) for the terminated Product(s) in each country in the terminated Region(s) that are held or controlled by or under authority of BMS, its Affiliates or Sublicensees, and shall take such actions and execute such other instruments, assignments and documents as may be reasonably necessary to effect the transfer of rights under such Regulatory Materials and related documentation to BN. The Parties shall complete such transfers/assignments within [***] after the applicable effective date of termination, unless otherwise mutually agreed in writing. During such [***] period, BMS shall provide to BN copies of all such

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Regulatory Materials, and shall use all reasonable efforts thereafter to provide as promptly as practicable all related documentation, including preclinical and clinical data (including investigator reports, both preliminary and final, statistical analyses, expert opinions and reports, safety and other electronic databases) not already provided to BN during the Term that are held by and reasonably available to BMS. BMS may retain such a copy of all transferred documents (and originals where required by Applicable Law).

(e) Product Marks. If, following any termination after the License Effective Date, BN notifies BMS in writing within [***] after the date of termination that BN wishes to acquire any Product Mark used in connection with the terminated Product(s), BMS shall, subject to Section 12.7(l), assign to BN, or cause the assignment to BN of, all rights in and to such Product Mark for the terminated Product(s) in the terminated Region(s), together with all associated goodwill. It is understood that such assignment shall not include the BMS name or trademark for the BMS company itself, or any other trademark owned or Controlled by BMS and not specific to a Product. BMS will provide such written confirmation and execute such instruments as BN may reasonably request to confirm BN’s title, rights and interests and will reasonably cooperate with BN in registering such assignments with appropriate Governmental Authorities. Any Product Marks that BN does not request to have assigned to it in accordance with this Section 12.7(e) shall remain the property of BMS and BMS shall be free to use such Product Marks anywhere in the world, in any manner and with any product as it may determine in its sole discretion, without further consulting BN.

(f) Clinical Trials After Termination. BMS shall, subject to Section 12.7(l), be responsible for completing (in accordance with the established protocols) any Clinical Trials (other than the PROSPECT Study and Clinical Trials conducted under the NIH CRADA) that were commenced prior to the termination of this Agreement; provided that if BMS terminates this Agreement for safety reasons pursuant to Section 12.2(b), BMS’s only obligation under this clause (f) shall be to wind down such Clinical Trials. Commencement shall mean the point at which the first Clinical Trial subject has been dosed with the relevant Product. BMS shall carry out any such studies in accordance with Section 5. BMS shall not commence any Clinical Trial at any time after it has given or received a notice of termination pursuant to this Article 12. In the event that the Parties agree (including as to the meeting of the ongoing costs of such Clinical Trials), the sponsorship of the Clinical Trials may be transitioned to BN. To the extent BMS is obligated to perform activities under this clause (f) at its own expense pursuant to Section 12.7(l), it shall only be required to do so at its own expense during the period between notice of termination and the effective date of termination.

(g) Return of Materials and Seed Banks. To the extent that BMS has been provided with the same, upon termination for any reason, BMS shall, subject to Section 12.7(l), at BN’s option and in accordance with BN’s written instructions, either destroy or return to BN all BN Materials provided to BMS including any master and working seed banks provided to BMS by or on behalf of BN.

(h) Provision of Promotional and Marketing Materials After Termination. Promptly following the effective date of termination, BMS shall, subject to Section 12.7(l), provide to BN at least one electronic and one paper copy of all promotional and marketing materials used in the promotion of the terminated Products in each country in the

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

terminated Region(s) which were the subject of the termination and hereby grants a license to BN in the Territory or the relevant Region(s), effective as of the date of termination, to use and/or create any such materials, copies or derivative works thereof in BN’s promotion of Products; provided that such license does not extend to use of any corporate trade name, corporate trademark, corporate name or logo, or corporate service mark of BMS and its Affiliates or Sublicensees. BN shall be entitled to sublicense the rights to any Third Party it grants the right to market Products in the Territory. BN shall indemnify, defend and hold harmless BM, its Affiliates and Sublicensees from and against any claims, losses, damages and costs arising from BN’s or its sublicensees’ use of such materials.

(i) Transition Assistance. BMS agrees to provide reasonable cooperation to BN and its designee(s), at BN’s sole expense, to facilitate, and the Parties agree to use reasonable efforts to effect, a reasonable, orderly and prompt transition of the Development (and as applicable, Commercialization) activities relating to the terminated Product(s) in the terminated Region(s) to BN and/or its designee(s) following delivery of notice of termination so that BN can be prepared to assume responsibility for same as of the termination date. Where the same cannot be fully achieved prior to termination, then, except where BMS provided [***] notice of termination, BMS agrees to continue to provide reasonable cooperation to BN and its designee(s), at BN’s sole expense, to facilitate an orderly transition, as promptly as possible thereafter, of the Development (and, as applicable, Commercialization) activities relating to the terminated Product(s) in the terminated Region(s) to BN and/or its designee(s) following such termination. In the event this Agreement is terminated only in certain Regions with respect to a particular Product, BMS and BN shall discuss in good faith and enter into a written agreement restricting, to the extent permitted under Applicable Law, each Party from intentionally and directly Commercializing the Product in the other Party’s territory and coordinating the global safety and pharmacovigilance activities with respect to such Product.

(j) Return of Confidential Information. Within [***] after the end of the Commercialization Wind-Down Period, BMS shall destroy all tangible items comprising, bearing or containing any Confidential Information of BN that are in BMS’s or its Affiliates’ possession or control, and provide written certification of such destruction, or prepare such tangible items of Confidential Information for shipment to BN, as BN may direct, at BN’s expense; provided that BMS may retain one copy of such Confidential Information for its legal archives, and provided further that BMS shall not be required to destroy electronic files containing Confidential Information that are made in the ordinary course of its business information back-up procedures pursuant to its electronic record retention and destruction practices that apply to its own general electronic files and information.

(k) Remaining Inventories. Subject to Sections 12.7(b) and 12.7(l), BMS shall provide to BN any or all reference standards and stability material and other similar materials used by BMS in the Development or Commercialization of terminated Product(s) held by or on behalf of BMS as of the date of termination. BMS shall provide a list of such materials in writing within [***] after the effective date of termination and BN shall notify BMS whether BN elects to exercise such right within [***] of receipt of such notice.

(l) Reversion Costs. Following any termination by BMS pursuant to Section 12.3 or 12.4, BMS’s obligation to perform any activity set forth in clauses (d), (e), (f), (g), (h) or

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with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(k) of this Section 12.7 shall be subject to BN’s prior written agreement [***].

(m) Damages Offset. Notwithstanding Section 12.9(a), if BN terminates this Agreement pursuant to Section 12.3, then the amount by which (i) [***].

12.8 Effects of Expiration of TC Term. Upon the expiration of the TC Term (i.e., in the case where there is no earlier termination pursuant to this Article 12), on a Product-by-Product and country-by-country basis, the license granted to BMS under Section 4.1(b) with respect to BN Technology shall convert to a non-exclusive, perpetual, irrevocable, fully paid-up, non-royalty-bearing, sublicensable license and the licenses granted to BMS under Sections 4.1(c) and 4.1(d) shall survive and become perpetual and irrevocable.

12.9 Other Remedies. Termination or expiration of this Agreement for any reason shall not release either Party from any liability or obligation that already has accrued prior to such expiration or termination, nor affect the survival of any provision hereof to the extent it is expressly stated to survive such termination. Subject to and without limiting the terms and conditions of this Agreement, expiration or termination of this Agreement shall not preclude any Party from (a) claiming any other damages, compensation or relief that it may be entitled to upon such expiration or termination, (b) any right to receive any amounts accrued under this Agreement prior to the expiration or termination date but which are unpaid or become payable thereafter and (c) any right to obtain performance of any obligation provided for in this Agreement which shall survive expiration or termination.

12.10 Survival. Termination or expiration of this Agreement shall not affect rights or obligations of the Parties under this Agreement that have accrued prior to the date of termination or expiration of this Agreement. Notwithstanding anything to the contrary, the following provisions shall survive and apply after expiration or termination of this Agreement: Sections 4.4, 4.5, 8.11, 8.12, 9.1, 9.5(a), 9.7, 9.16, 11.1, 11.2, 11.3 and Articles 1 (to the extent necessary to interpret other surviving sections), 12, 14, 15 and 16. In addition, the other applicable provisions of Article 8 shall survive to the extent required to make final payments with respect to Net Sales incurred or accrued prior to the date of termination or expiration. All provisions not

surviving in accordance with the foregoing shall terminate upon expiration or termination of this Agreement and be of no further force and effect.

12.11 Termination of PHS License Agreement. Upon any termination of the PHS License Agreement, the provisions of Section 4.3 of the PHS License Agreement shall apply. Following any such conversion, BMS shall continue to make the payments to BN hereunder but shall be entitled to deduct from any amounts payable to BN hereunder any amounts payable by BMS to PHS in respect of Products pursuant to such direct license.

13. REPRESENTATIONS AND WARRANTIES AND COVENANTS

13.1 Mutual Representations and Warranties. Each Party hereby represents, warrants, and covenants (as applicable) to the other Party as of the Effective Date as follows, save as disclosed in Exhibit K:

(a) It is a company or corporation duly organized, validly existing, and in good standing under the laws of the jurisdiction in which it is incorporated, and has full corporate power and authority and the legal right to own and operate its property and assets and to carry on its business as it is now being conducted and as contemplated in this Agreement, including the right to grant the licenses granted by it hereunder.

(b) It has the full corporate power and authority and the legal right to enter into this Agreement and perform its obligations hereunder. It has taken all necessary corporate action on its part required to authorize the execution and delivery of this Agreement and the performance of its obligations hereunder. This Agreement has been duly executed and delivered on behalf of such Party, and constitutes a legal, valid, and binding obligation of such Party that is enforceable against it in accordance with its terms.

(c) It is not a party to any agreement, outstanding order, judgment or decree of any court or Governmental Authority that would prevent it from granting the rights granted to the other Party under this Agreement or performing its obligations under this Agreement.

(d) It has not, and will not, after the Effective Date and during the Term, grant any right to any Third Party that would conflict with the rights granted to the other Party hereunder.

13.2 Additional Representations and Warranties by BN. BN hereby represents and warrants that, save as disclosed in and subject to Exhibit K, as of the Effective Date and, where denoted below, covenants to BMS as follows:

(a) BN has sufficient legal and/or beneficial title, ownership or license under its Patents and Information necessary for the purposes contemplated by this Agreement. The BN Technology existing as of the Effective Date is free and clear from any Liens, and BN has sufficient legal and/or beneficial title, ownership or license thereunder to grant the licenses to BMS as purported to be granted pursuant to this Agreement. As of the Effective Date, BN is the sole owner of all right, title and interest in and to (free and clear from any Liens of any kind) the BN Patents listed in section (I) of Exhibit A1. All fees required to maintain such issued Patent

rights have been paid to date. To BN’s knowledge, the BN Patents listed on Exhibits A1 and A2 constitute all Patents Controlled by BN that would be infringed by the manufacture (as currently conducted), use or sale of Products (but for the license granted by BN to BMS under Section 4.1).

(b) There is no agreement in effect, either oral or written, between BN and any other Person, relating to the Development, Commercialization or manufacture of the Products except the Existing Product Agreements.

(c) BN has not received any written notice from any Third Party asserting or alleging that the discovery, research and/or Development of Products by BN prior to the Effective Date infringes the intellectual property rights of such Third Party. The BN Technology owned by BN, and to BN’s knowledge, all BN Technology Controlled but not owned by BN, that exists as of the Effective Date was not obtained in violation of any contractual or fiduciary obligation owed by BN or its employees or authorized agents to any Third Party or through the misappropriation of the intellectual property rights (including any trade secrets) from any Third Party.

(d) To BN’s knowledge, the Development, Commercialization and manufacture of the Products can be carried out in the manner contemplated as of the Effective Date without infringing any published patent applications (evaluating such patent applications as though they were issued with the claims as published as of the Effective Date) or issued patents owned or controlled by a Third Party. To BN’s knowledge, the research, Development and manufacture of PROSTVAC prior to the Effective Date by or on behalf of BN has been carried out without infringing any published patent applications (evaluating such patent applications as though they were issued with the claims as published as of the Effective Date) or issued patents owned or controlled by a Third Party.

(e) There are no pending, and BN has not received any notice in writing threatening any, actions, suits or proceedings against BN involving the BN Technology.

(f) To BN’s knowledge, no Third Party is infringing or has misappropriated any of the BN Technology as it relates to Products (in the case of pending claims in any Patent, evaluating them as if issued as of the Effective Date).

(g) To the knowledge of BN’s legal counsel, each of the claims included in each issued BN Patent are valid and enforceable.

(h) There is no agreement currently in effect under which BN or any of its Affiliates has granted (and BN covenants that during the Term it and its Affiliates shall not grant) any license or any option for a license under the BN Technology to any Third Party to make, use or sell any Product in any country in the Territory in any manner that would conflict with this Agreement. BN covenants that during the Term it and its Affiliates shall not grant any license or any option for a license to any Third Party, under any Patent that comes into the Control of BN in connection with this Agreement after the Effective Date (including a Patent for a BN Sole Invention or Joint Invention), to make, use or sell in the Field any Product in any country in the Territory (save where this Agreement has been terminated in respect of such

Product and/or such country, in which case BN shall be free to grant such rights in respect of such Product and/or such country in its absolute discretion). Neither BN nor any of its Affiliates has granted any Lien which is still in force at the Effective Date with respect to this Agreement or any of the BN Technology licensed to BMS under this Agreement. BN and its Affiliates have not granted to any Third Party any right or license or option to enforce or obtain any patent term extension for any of the Product Specific Patents.

(i) BN has disclosed in writing to BMS’s patent counsel (i) all BN Patents existing as of the Effective Date that would be infringed by the Development, Commercialization or manufacture of Products by BMS, but for the licenses granted in this Agreement, and (ii) the jurisdiction(s) by or in which each such BN Patent has been issued or in which an application for such BN Patent has been filed, together with the respective patent or application numbers. All fees required to maintain such issued BN Patent rights have been paid.

(j) No person, other than former or current employees of BN who are obligated in writing to assign his/her inventions to BN, is an inventor of any of the inventions claimed in the BN Patents owned by BN filed or issued as of the Effective Date, except for those Third Party inventors of those inventions that fall within the BN Technology Controlled by BN and in respect of which, as far as BN is aware, PHS and/or NCI has obtained an assignment as of the Effective Date. All inventors of any inventions claimed in the BN Patents that are existing as of the Effective Date and owned by BN have assigned or have a contractual obligation to assign or license their entire right, title and interest in and to such inventions and the corresponding Patent rights to BN. No present or former employee or consultant of BN owns or has any proprietary, financial or other interest, direct or indirect, in the BN Technology. No claims have been asserted in writing challenging the inventorship of the BN Patents owned by BN or to BN’s knowledge the BN Patents Controlled but not owned by BN.

(k) To BN’s knowledge, the research and Development of PROSTVAC has been conducted prior to the Effective Date by BN, its Affiliates, its licensors, its licensees, and its independent contractors, in compliance in all material respects with all Applicable Law, including all public health, environmental, and safety provisions thereof, and all permits, governmental licenses, registrations, approvals, concessions, franchises, authorizations, orders, injunctions and decrees that apply to BN.

(l) To BN’s knowledge, all PROSTVAC used in Clinical Trials has been manufactured in compliance with cGMPs.

(m) (i) All Regulatory Materials filed by BN with respect to PROSTVAC (including the INDs therefor) were, at the time of filing, true, complete and accurate in all material respects, (ii) no serious adverse event information has come to the attention of BN that is materially different in terms of the incidence, severity or nature of such serious adverse events than that which was filed as safety updates to the IND for PROSTVAC and (iii) all written data summaries prepared by BN that were included in such Regulatory Materials and that are based on clinical studies conducted or sponsored by BN accurately summarize in all material respects the corresponding raw data underlying such summaries.

(n) BN has not received any written notice which has led it to believe that any of the INDs held by BN for PROSTVAC may not be currently in good standing with the FDA. BN has made available to BMS complete and accurate copies of all INDs held by BN for PROSTVAC. BN has filed with the FDA all required notices, supplemental applications and annual or other reports or documents, including adverse experience reports, with respect to each IND held by BN which are material to the continued Development of PROSTVAC.

(o) BN has not received any written notice that any United States governmental or regulatory agency (including the FDA) has commenced, or, to its knowledge, threatened in writing to initiate any action to withdraw an active IND held by BN, or, to BN’s knowledge, commenced or threatened in writing to initiate any action to enjoin production of PROSTVAC at its or any of its supplier’s facilities.

(p) BN has made available to BMS copies of all material (i) reports of inspection observations, if any, that are in its possession or of any of its Affiliates relating to PROSTVAC, (ii) establishment inspection reports that are in its possession or of any of its Affiliates relating to PROSTVAC, and (iii) warning letters, if any, as well as any other documents, if any, that are in its possession or of any of its Affiliates that assert past or ongoing material lack of compliance with any Applicable Laws or regulatory requirements (including those of the FDA) by BN or its Affiliates, and to its knowledge, its suppliers relating to clinical Development of PROSTVAC.

(q) To BN’s knowledge, neither it, any of its Affiliates, or any of its or their respective officers, employees, or agents has made an untrue statement of material fact or fraudulent statement to FDA or any other Regulatory Authority with respect to the Development of PROSTVAC, failed to disclose a material fact required to be disclosed to the FDA or any other Regulatory Authority with respect to the Development of PROSTVAC, or committed an act, made a statement, or failed to make a statement with respect to the Development of PROSTVAC that could reasonably be expected to provide a basis for the FDA to invoke its policy respecting “Fraud, Untrue Statements of Material Facts, Bribery, and Illegal Gratuities”, set forth in 56 Fed. Reg. 46191 (September 10, 1991) and any amendments thereto.

(r) BN has disclosed to BMS, through the Virtual Data Room or otherwise in writing to BMS, all material information known by BN with respect to the safety and efficacy of PROSTVAC.

(s) Prostatic diseases, as used herein and in the PHS License Agreement, include prostate cancer.

(t) BN has maintained in full force and effect all the Existing Product Agreements. It and its Affiliates are in compliance in all material respects with each Existing Product Agreement, and have performed all obligations required to be performed by them to date under the Existing Product Agreement. Neither BN nor its Affiliates are (with or without the lapse of time or the giving of notice, or both) in breach or default in any respect under the Existing Product Agreement and, to the knowledge of BN, no other party to any Existing Product Agreement is (with or without the lapse of time or the giving of notice, or both) in breach or default in any respect thereunder.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

(u) No agreement to which BN or any of its Affiliates is a party as of the Effective Date obligates BMS to grant, assign or otherwise convey to BN or any of its Affiliates, or to any other Person, any rights under any Patents or Information that BMS or its Affiliates may own or control (other than such BN Technology as is licensed to BMS hereunder) during or following the Term.

(v) BN will be the sole owner of all rights to the clinical data generated in the course of the performance of the PROSPECT Trial, has not granted any Third Party any right to use such clinical data for commercial purposes and to the best of BN’s knowledge BN has the sole right to use for commercial purposes all rights to the clinical data generated in any other Clinical Trial that has been completed or is ongoing as of the Effective Date.

(w) In the course of the Development of Products, BN has not used to the best of BN’s knowledge prior to the Effective Date, and shall not use during the Option Term, any employee, agent or independent contractor who has been debarred by any Regulatory Authority, or, to the best of BN’s knowledge, is the subject of debarment proceedings by a Regulatory Authority.

13.3 No Other Representations or Warranties. EXCEPT AS EXPRESSLY STATED IN THIS ARTICLE 13 OR ELSEWHERE IN THIS AGREEMENT, NO REPRESENTATIONS OR WARRANTIES WHATSOEVER, WHETHER EXPRESS OR IMPLIED, INCLUDING WARRANTIES OF MERCHANTABILITY, FITNESS FOR A PARTICULAR PURPOSE OR NON-INFRINGEMENT OF THIRD PARTY INTELLECTUAL PROPERTY RIGHTS, OR THAT ANY OF THE DEVELOPMENT AND/OR COMMERCIALIZATION EFFORTS WITH REGARD TO ANY PRODUCT WILL BE SUCCESSFUL, IS MADE OR GIVEN BY OR ON BEHALF OF A PARTY. EXCEPT AS EXPRESSLY STATED IN THIS AGREEMENT, ALL REPRESENTATIONS AND WARRANTIES, WHETHER ARISING BY OPERATION OF LAW OR OTHERWISE, ARE HEREBY EXPRESSLY EXCLUDED.

13.4 Disclosure. BN shall not be in breach of any representation or warranty set out in this Agreement including in this Article 13, and BMS may not bring any claim for breach of the representations and warranties in this Agreement, in respect of any matter, event, condition, fact or circumstance which was disclosed in Exhibit K or is an agreement that is listed on Exhibit K and was included in the Virtual Data Room available to BMS at least [***] prior to the Effective Date.

13.5 Certain Covenants of BN.

(a) Save where this Agreement has been terminated in respect of a Product and/or in respect of a Region (in which case BN shall be free to grant such rights in respect of such Product and/or Region in its absolute discretion) BN shall not, and shall ensure that its Affiliates shall not: (i) sell, assign, transfer, fail to maintain, abandon or otherwise dispose of, or grant any Lien in (or permit any Lien to attach to), any BN Technology, to the extent that the same is Controlled by BN and subject to the terms of the Existing Product Agreements and the Oxford Biomedica Agreement disclosed in Exhibit K, with respect to any Product in the Field or this Agreement, (ii) negotiate or grant any license or sublicense (including any covenant not to

sue), option for a license or sublicense or covenant not to sue under any BN Technology, or any other right, with respect to any Product in the Field, (iii) amend or modify any existing contract with a Third Party, including any Existing Product Agreement, that could cause or otherwise result in any of the foregoing described in (i) and/or (ii), (iv) grant to any Third Party any right or license or option to enforce or obtain any patent term extension for any of the Non-Combination Product Specific Patents Controlled by BN as of the Effective Date or for any of the Existing Combination Product Patents to the extent that they Cover PROSTVAC, and/or (v) grant any other right, title or interest in or to or take any action (including entering into any contract) with respect to any of the BN Technology that may in any way impair, interfere with or prevent BMS’s full exercise of its rights under this Agreement. Without limiting BN’s obligations or BMS’s rights hereunder, BN shall not, and shall ensure that its Affiliates shall not, assign or otherwise transfer any BN Technology to any Third Party, unless it is to a Third Party successor-in-interest or purchaser of all or substantially all of the business or assets of BN to which this Agreement relates (including this Agreement), whether in a merger, combination, reorganization, sale of stock, sale of assets or other transaction, in accordance with Section 16.8.

(b) BN shall promptly notify BMS upon receiving written notice from any Governmental Authority of any material noncompliance with any Applicable Laws by, or any inquiries by any Regulatory Authorities with respect to, BN or any of its Affiliates or Third Party independent contractors (including any notice from any Regulatory Authority of any investigation or inspection) to the extent relating to the PROSPECT Trial (including any facilities or clinical trial material used in connection therewith) or any Product. If BN learns that any employee or consultant performing on its behalf under this Agreement has been debarred by any Regulatory Authority, or has become the subject of debarment proceedings by any Regulatory Authority, BN will promptly notify BMS and will prohibit such employee or consultant from performing on its behalf under this Agreement.

(c) BN shall, shall ensure that any of its Affiliates, and shall use Diligent Efforts to ensure that any Third Party independent contractor performing any part of the PROSPECT Trial, enter into and maintain valid and enforceable confidentiality agreements with its employees to protect and maintain the BN Technology and its and BMS’s rights with respect thereto (including with respect to any Know-How that arises in connection with the PROSPECT Trial).

13.6 Certain Covenants of BN Relating to the Existing Product Agreements.

(a) BN shall not, and shall ensure that its Affiliates shall not, assign or otherwise transfer any of the Existing Product Agreements without the prior written consent of BMS unless it is to a Third Party successor-in-interest or purchaser of all or substantially all of the business or assets of BN to which this Agreement relates (including this Agreement), whether in a merger, combination, reorganization, sale of stock, sale of assets or other transaction, in accordance with Section 16.8.

(b) BN shall not, and shall ensure that its Affiliates shall not, without BMS’s prior written consent: (i) waive, amend, cancel or terminate any material provision of, or fail to maintain, the PHS License Agreement in any manner that would be detrimental to the rights granted to BMS hereunder or that would impose additional or more onerous obligations on BMS,

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

including any changes to the diligence benchmarks in Appendix E of the PHS License Agreement as modified by the second amendment to that agreement, (ii) waive, amend, cancel or terminate any material provision of, or fail to maintain, and of the other Existing Product Agreements in any manner that would be materially detrimental to the rights granted to BMS hereunder or that would impose additional or more onerous obligations on BMS, or (iii) take or fail to take any action that would give any counterparty to any Existing Product Agreement the right to terminate such Existing Product Agreement.

(c) Promptly (but in no event later than [***]) after BN’s or its Affiliate’s receipt of any notice (written or oral) relating to any Existing Product Agreement (i) terminating or providing notice of termination of such Existing Product Agreement, (ii) alleging any material breach of or default under such Existing Product Agreement by BN or any of its Affiliates, BN shall provide a written notice to BMS describing in reasonable detail the relevant breach, default or termination event, including a copy of any written notice received from such licensor, and describing the corrective action BN or its Affiliate proposes to take. Subject to BMS’s rights under Section 13.6(d), BN shall, and shall cause its Affiliates to, as applicable thereafter use its best efforts to cure such breach, default or termination event.

(d) Without limiting any other right or remedy of BMS under this Agreement and in order to prevent, ameliorate, mitigate or cure a breach of any of the Existing Product Agreements, in the event that BN or any of its Affiliates fail to perform any of its material obligations under any Existing Product Agreement and (i) such failure is not cured within [***] after written notice from BMS, (ii) BN does not notify BMS that such failure has been contested, and/or (iii) BN does not notify BMS that a settlement has been reached in relation to the failure with the counterparty to the Existing Product Agreement (in each case within at least [***] prior to the end of any cure period set forth in such Existing Product Agreement), BMS may perform such obligation on behalf of BN and/or its Affiliates and, unless such failure was as a consequence of BMS’s actions or failure to act, BN shall reimburse BMS for BMS’s internal and out-of-pocket costs in connection with such performance. This Agreement sets forth the obligations of the Parties inter se, and nothing in this Agreement (including any standard of effort set forth herein) shall limit or modify the obligations of BN and/or its Affiliates under the Existing Product Agreements.

(e) Whenever BN or any of its Affiliates provides any report, notice or other communication relating to a Product and/or this Agreement to PHS, or to any counterparty to any other Existing Product Agreement if such notice would have a material and adverse effect on BMS’s rights under this Agreement, BN shall provide a copy of such report, notice, or other communication to BMS at least [***] prior to the time such report, notice or communication is provided to such counterparty or, if it is impracticable for BN to do so, BN shall provide such copy to BMS as soon as possible prior to the provision thereof to the counterparty.

(f) From and after the License Effective Date, BN shall (and/or, if applicable, shall cause its Affiliate to), if reasonably requested by BMS, use Diligent Efforts to exercise any of BN’s (and/or, if applicable, its Affiliate’s) material rights, and/or to enforce any material obligation of a counterparty to the relevant Existing Product Agreement, in each case as it relates to any Product and/or this Agreement. To the extent any such action would require the payment

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

of any out-of-pocket costs then, to extent the allocation of such costs is not otherwise addressed in this Agreement, the Parties will discuss and agree in good faith as to how such costs are to be allocate between them provided always that in the absence of such agreement any action or inaction shall be entirely at BN’s discretion and BN shall have no liability therefor.

13.7 BMS Covenants and Additional Representation.

(a) In respect of the Existing Product Agreements, BMS covenants that:

(i) BMS shall not, and shall ensure that its Affiliates and require that its Sublicensees shall not, take any action or fail to act in any way that would result in BN being in breach of any material provision of any Existing Product Agreement, or agree to do any of the foregoing;

(ii) BMS shall, and shall ensure that its Affiliates and require that its Sublicensees shall, comply with the provisions of such agreements applicable to BMS and its Affiliates and Sublicensee. BMS shall and shall ensure that its Affiliates and require that its Sublicensees shall provide such assistance, at BN’s expense, as is reasonably requested by BN in relation to BN’s compliance with the provisions of such agreements;

(iii) To the extent that BMS or any of its Affiliates or Sublicensees receives any communication, correspondence or notice from any Existing Product Agreement Licensor, BMS shall, and shall ensure that its Affiliates and require that its Sublicensees shall, promptly, and in no event later than [***] after such receipt, provide a copy to BN;

(iv) BMS shall, and shall ensure that its Affiliates and require that its sublicensees shall, provide all information in such Person’s possession reasonably requested by BN that BN requires for its compliance with such agreements; and

(v) BMS shall not, and shall ensure that its Affiliates and require that its Sublicensees shall not, have any contact or dealing directly with the Existing Product Agreement Licensors with respect to the specific subject matter of the Existing Product Agreements, other than with BN’s prior written consent (not to be unreasonably withheld) both to the timing, fact and the subject matter of the contact or dealing, and excluding situations (A) involving BN’s or an Affiliate’s breach (or cure thereof) of any such agreement, (B) following insolvency or bankruptcy of BN or an applicable Affiliate, (C) as required or permitted by any such Existing Product Agreements, (D) relating to the prosecution, maintenance, defense and enforcement of Patent Rights and Know-How sublicensed to BMS under the Existing Product Agreement, or (E) involving any waiver to the obligation under the PHS License Agreement to substantially manufacture in the United States quantities of Product for sale in the United States that are not supplied by BN under the Supply Agreement.

(b) BMS covenants that it shall, and shall ensure that its Affiliates and require that its Sublicensees shall, comply with Section 6.3.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

[***].

14.4 Indemnification Procedures. The Party claiming indemnity under this Article 14 (the “Indemnified Party”) shall give written notice to the Party from whom indemnity is being sought (the “Indemnifying Party”) promptly after learning of the claim, suit, proceeding or cause of action for which indemnity is being sought (“Claim”), and, provided that the Indemnifying Party is not contesting the indemnity obligation, shall permit the Indemnifying Party to control and assume the defense of any litigation relating to such Claim and disposition of any such Claim. Notwithstanding the foregoing, if the Indemnifying Party is also a party (or likely to be named a party) to the proceeding in which such Claim is made and the Indemnified Party gives notice to the Indemnifying Party that it may have defenses to such Claim that are in conflict with the interests of the Indemnifying Party, then the Indemnifying Party shall not be so entitled to assume the defense of the case. If the Indemnifying Party does assume the defense of any Claim, it (a) shall act diligently and in good faith with respect to all matters relating to the settlement or disposition of any Claim as the settlement or disposition relates to Parties being indemnified under this Article 14, (b) shall cause such defense to be conducted by counsel reasonably acceptable to the Indemnified Party and (c) shall not settle or otherwise resolve any Claim without prior notice to the Indemnified Party and the consent of the Indemnified Party if such settlement involves anything other than the payment of money by the Indemnifying Party. The Indemnified Party shall reasonably cooperate with the Indemnifying Party in its defense of any claim for which the Indemnifying Party has assumed the defense in accordance with this Section 14.4, and shall have the right (at its own expense) to be present in person or through counsel at all legal proceedings giving rise to the right of indemnification. So long as the Indemnifying Party is diligently defending the Claim in good faith, the Indemnified Party shall not settle any such Claim without the prior written consent of the Indemnifying Party. If the Indemnifying Party does not assume and conduct the defense of the Claim as provided above, (x) the Indemnified Party may defend against, and consent to the entry of any judgment or enter into any settlement with respect to, the Claim in any manner the Indemnified Party may deem reasonably appropriate (and the Indemnified Party need not consult with, or obtain any consent from, the Indemnifying Party in connection therewith), and (y) the Indemnifying Party will remain responsible to indemnify the Indemnified Party as provided in this Article 14.

Nothing in this Article 14 shall act to negate any obligation under common law of either Party to mitigate damages resulting from or arising as a consequence of any circumstances giving rise to any Claim for which such Party is being indemnified against or held harmless by the other Party hereunder or any claim or cause of action under which a Party intends to seek damages from the other Party pursuant to this Agreement or at law or in equity.

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

BMS with written evidence of such insurance upon request. BN shall provide BMS with written notice at least [***] prior to the cancellation, non-renewal or material change in such insurance.

14.7 Insurance as it Relates to Certain Claims for Damages. The amount of a breaching Party’s liability for any claim for damages by the non-breaching Party for a breach of representations or warranties under this Agreement (other than with respect to indemnification obligations under this Article 14) shall be reduced by any sum which is recoverable under any insurance policies maintained by the non-breaching Party or any of its Affiliates in respect of the loss or damage suffered by reason of the relevant breach, less the amount of any reasonable costs and expenses incurred in obtaining payment of that sum; and if the breaching Party has paid to the non-breaching Party any amount in respect of the claim before the recovery of that sum, the non-breaching Party shall repay to it, or procure the repayment to it of the amount by which its liability is so reduced.

15. DISPUTE RESOLUTION

15.1 Disputes; Resolution by Executive Officers. The Parties recognize that disputes as to certain matters may from time to time arise during the Term that relate to decisions to be made by the Parties herein or to the Parties’ respective rights and/or obligations hereunder. It is the desire of the Parties to establish procedures to facilitate the resolution of disputes arising under this Agreement in an expedient manner by mutual cooperation and without resort to arbitration or litigation. To accomplish this objective, the Parties agree to follow the procedures set forth in this Article 15 if and when a dispute arises under this Agreement, subject to Section 16.9. Accordingly, any disputes, controversies or differences other than a matter within the final decision-making authority of BMS or BN, which may arise between the Parties out of or in relation to or in connection with this Agreement, shall be promptly presented to the Alliance Managers for resolution. If the Alliance Managers are unable to resolve such dispute within [***] after a matter has been presented to them, then upon the request of either Party by written notice, the Parties agree to meet and discuss in good faith a possible resolution thereof, which good faith efforts shall include at least one in-person meeting between the Executive Officers of each Party within [***] after receipt by the other Party of such written notice. If the matter is not resolved within [***] following presentation to the Executive Officers, then either Party may pursue such remedies as it may deem necessary or appropriate.

15.2 Patent or Trademark Disputes. Notwithstanding Section 16.9, any dispute, controversy or claim relating to the inventorship, scope, validity, enforceability or infringement of any Patents Covering the manufacture, use, importation, offer for sale or sale of Products or to any Product Mark shall be submitted to a court of competent jurisdiction in the country in which such patent or trademark rights were granted or arose.

16. MISCELLANEOUS

16.1 Entire Agreement; Amendments. This Agreement, including the Exhibits hereto (which are incorporated into and made a part of this Agreement), sets forth the complete, final and exclusive agreement and all the covenants, promises, agreements, warranties,

representations, conditions and understandings between the Parties hereto with respect to the subject matter hereof and supersedes, as of the Effective Date, all prior agreements and understandings between the Parties with respect to the subject matter hereof, including the Prior CDA. There are no covenants, promises, agreements, warranties, representations, conditions or understandings, either oral or written, between the Parties other than as are set forth herein and therein. No subsequent alteration, amendment, change or addition to this Agreement shall be binding upon the Parties unless reduced to writing and signed by an authorized representative of each Party; provided that BNInc’s signature shall not be required for any alteration, amendment, change or addition to provisions other than the BNInc Provisions.

16.2 Export Control. This Agreement is made subject to any restrictions concerning the export of products or technical information from the U.S. or other countries which may be imposed upon or related to BN or BMS from time to time. Each Party agrees that it shall not export, directly or indirectly, any technical information acquired from the other Party under this Agreement or any products using such technical information to a location or in a manner that at the time of export requires an export license or other governmental approval, without first obtaining the written consent to do so from the appropriate agency or other governmental entity.

16.3 Rights in Bankruptcy, Insolvency and Similar Circumstances.

(a) In the event of any bankruptcy, insolvency, administration, liquidation, receivership, or similar proceeding or event under any Applicable Law, including any proceeding (including any chapter 15 proceeding) under Title 11 of the United States Code (the “U.S. Bankruptcy Code”) or under the laws of Denmark (any such proceeding or event being referred to herein as a “Bankruptcy Event”), all license rights granted under or pursuant to this Agreement are and shall be, and shall be deemed to be, fully vested in the Party not subject to the Bankruptcy Event and not revocable or terminable at the option of the Party subject to such Bankruptcy Event or such Party’s trustee or other representative in such Bankruptcy Event. In addition, all license rights granted under or pursuant to this Agreement are and shall be, and shall be deemed to be, for all purposes of Section 365(n) of the U.S. Bankruptcy Code and any other Applicable Law of any jurisdiction, licenses of rights to “intellectual property” as defined in the U.S. Bankruptcy Code or such other Applicable Law, and, in the case of any Bankruptcy Event, the Party not subject to such Bankruptcy Event shall have all rights under Section 365(n) of the U.S. Bankruptcy Code and all other rights to retain its license rights granted under or pursuant to this Agreement, notwithstanding such Bankruptcy Event or any action or event within or as a result of such Bankruptcy Event, including any rejection, termination, or other disavowal of this Agreement.

(b) During the Term, each Party shall create and maintain current copies to the extent practicable of all intellectual property subject to license rights granted under or pursuant to this Agreement. Without limiting the Parties’ rights under Section 365(n) of the U.S. Bankruptcy Code or other Applicable Law, in the case of any Bankruptcy Event, the Party not subject to such Bankruptcy Event shall be entitled to a copy of any and all such intellectual property and all embodiments of such intellectual property, and the same, if not in the possession of such other Party, shall be promptly delivered to it. All rights of the Parties under this Section 16.3 and under Section 365(n) of the U.S. Bankruptcy Code are in addition to and not in substitution of any and all other rights, powers, and remedies that each Party may have under this

Agreement, the U.S. Bankruptcy Code, and any other Applicable Law. In the case of any Bankruptcy Event, the Party not subject to such Bankruptcy Event shall have the right to perform the obligations of the Party subject to the Bankruptcy Event hereunder with respect to any intellectual property addressed herein, notwithstanding such Bankruptcy Event or any action or event within or as a result of such Bankruptcy Event, including any rejection, termination, or other disavowal of this Agreement, but neither such provision nor such performance by such other Party shall release the Party subject to the Bankruptcy Event from any such obligation or liability for failing to perform it. Any intellectual property provided pursuant to the provisions of this Section 16.3 shall be subject to the licenses set forth elsewhere in this Agreement and the payment obligations of this Agreement, which shall be deemed to be royalties for purposes of Title 11.

(c) The Parties agree that they intend the foregoing rights to extend to the maximum extent permitted by law and any provisions of applicable contracts with Third Parties, including for purposes of the U.S. Bankruptcy Code and any other Applicable Law, (i) the right of access to any intellectual property (including all embodiments thereof) of the Party subject to any Bankruptcy Event or any Third Party with whom the Party subject to any Bankruptcy Event contracts to perform an obligation of the Party subject to any Bankruptcy Event under this Agreement, and, in the case of the Third Party, which is necessary for the Development, Regulatory Approval and/or manufacture of Products and (ii) the right to contract directly with any Third Party described in (i) in this sentence to complete the contracted work.

(d) In the event that after the Effective Date BN enters into, or has as of the Effective Date entered into, a license agreement with a Third Party with respect to intellectual property that will be sublicensed to BMS hereunder (including the Existing Product Agreements), BN will use commercially reasonable efforts to enable BMS to concurrently enter arrangements with BN and any such Third Party whereby BMS will receive a direct license from any such Third Party in the event that such license agreement between BN and such Third Party is terminated during the Term solely on account of BN becoming subject to any Bankruptcy Event.

(e) Notwithstanding anything to the contrary in Article 9, in the event that BN is subject to any Bankruptcy Event, BMS may take appropriate actions in connection with the Prosecution and/or enforcement of any BN Patent rights licensed to BMS under this Agreement without being required to consult with BN before taking any such actions, provided that such actions are otherwise consistent with this Agreement.

16.4 Force Majeure. Each Party shall be excused from the performance of its obligations under this Agreement to the extent that such performance is prevented by force majeure (defined below) and the nonperforming Party promptly provides notice of such prevention to the other Party. Such excuse shall be continued so long as the condition constituting force majeure continues. The Party affected by such force majeure also shall notify the other Party of the anticipated duration of such force majeure, any actions being taken to avoid or minimize its effect after such occurrence, and shall take reasonable efforts to remove the condition constituting such force majeure. For purposes of this Agreement, “force majeure” shall include conditions beyond the control of the Parties, including an act of God, acts of terrorism, voluntary or involuntary compliance with any regulation, law or order of any

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

government, war, acts of war (whether war be declared or not), labor strike or lock-out, civil commotion, epidemic, failure or default of suppliers, public utilities or common carriers, destruction of production facilities or materials by fire, earthquake, storm or like catastrophe. The payment of invoices due and owing hereunder shall in no event be delayed by the payer because of a force majeure affecting the payer.

16.5 Notices. Any notice required or permitted to be given under this Agreement shall be in writing, shall specifically refer to this Agreement, and shall be addressed to the appropriate Party at the address specified below or such other address as may be specified by such Party in writing in accordance with this Section 16.5, and shall be deemed to have been given for all purposes (a) when received, if hand-delivered or sent by a reputable international expedited delivery service, or (b) [***] after mailing, if mailed by first class certified or registered mail, postage prepaid, return receipt requested.

For BN or BNInc: Bavarian Nordic A/S
Hejreskovvej 10A
DK-3490 Kvistgaard
Denmark
Attention: Chief Executive Officer

With a copy to: Bavarian Nordic Inc.
2425 Garcia Ave
Mountain View CA 94043
Attention: President

For BMS: Bristol-Myers Squibb Company
Route 206 and Province Line Road
Princeton, NJ 08543-4000
United States
Attention: Vice President, Transactions

With a copy to: Bristol-Myers Squibb Company
Route 206 and Province Line Road
Princeton, NJ 08543-4000
United States
Attention: Vice President and Assistant General Counsel, Business Development and Licensing

Furthermore, a copy of any notices required or given under Section 9.7 of this Agreement shall also be addressed to the Vice President and Chief Intellectual Property Counsel of BMS at the address set forth above. For the avoidance of doubt, the non-delivery of a copy of a notice shall not mean that the notice is invalid.

16.6 Independent Contractors. Each Party shall act solely as an independent contractor, and nothing in this Agreement shall be construed to give either Party the power or authority to act for, bind, or commit the other Party in any way. Nothing herein shall be

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

construed to create the relationship of partners, principal and agent, or joint-venture partners between the Parties.

16.7 Maintenance of Records. Each Party shall, and shall ensure that any of its Affiliates and Third Party independent contractors performing any Development of Products on behalf of a Party (including any part of the PROSPECT Trial), maintain complete and accurate records of all work conducted under this Agreement and all results, data and developments made pursuant to its efforts under this Agreement. Such records shall be complete and accurate and shall fully and properly reflect all work done and results achieved in the performance of this Agreement in sufficient detail and in good scientific manner appropriate for patent and regulatory purposes. Each Party shall maintain such records for a period of [***] after such records are created; provided that records may be maintained for an appropriate longer period in accordance with each Party’s internal policies on record retention in order to ensure the preservation, prosecution, maintenance or enforcement of intellectual property rights. Each Party shall keep and maintain all records required by Applicable Law with respect to Products.

16.8 Assignment. Neither Party may assign this Agreement or assign or transfer any rights or obligations hereunder without the prior written consent of the other, except that a Party may make such an assignment or transfer without the other Party’s consent (a) to any Affiliate of such Party, provided that such transfer shall not adversely affect the other Party’s rights and obligations under this Agreement and that such assigning/transferring Party remains jointly and severally liable with such Affiliate for the performance of this Agreement and/or the assigned obligations, or (b) to any Third Party successor-in-interest or purchaser of all or substantially all of the business or assets of such Party to which this Agreement relates, whether in a merger, combination, reorganization, sale of stock, sale of assets or other transaction; provided, however, that, with respect to both Parties, the assigning Party provides written notice to the other Party of such assignment and the assignee shall have agreed in writing to be bound (or is otherwise required by operation of Applicable Law to be bound) in the same manner as such assigning Party hereunder. In addition, either Party may assign its right to receive proceeds under this Agreement or grant a security interest in such right to receive proceeds under this Agreement to one or more Third Parties providing financing to such Party pursuant to the terms of a security or other agreement related to such financing (e.g., for purposes of a royalty financing arrangement). Any permitted assignment shall be binding on the successors of the assigning Party.

In the event that control (as “control” is defined under the Affiliate definition in Article 1) of BN is acquired by a Third Party after the Effective Date (such Third Party, hereinafter referred to as an “Acquirer”), then the intellectual property of such Acquirer held or developed by such Acquirer (and Affiliates of such Acquirer that are not controlled (as “control” is defined under the Affiliate definition in Article 1) by BN following such acquisition) prior to or after such acquisition (other than intellectual property developed by such Acquirer or such Affiliates in the course of conducting BN’s activities under this Agreement) shall be excluded from the BN Technology existed prior to such acquisition and which are not controlled by BN following such acquisition) shall be excluded from the Affiliate definition (other than with respect to intellectual property developed by such Acquirer or such Affiliates in the course of conducting BN’s activities under this Agreement) solely for purposes of the applicable components of the BN Technology. For clarity, any intellectual property developed by the Acquirer in the course of

conducting BN’s activities under this Agreement or in the Field through use of the BN Technology or BN’s Confidential Information shall be included within the BN Technology to the extent such intellectual property would have been so included had it been developed by BN.

Any assignment or attempted assignment by either Party in violation of the terms of this Section 16.8 shall be null, void and of no legal effect. For clarity, the provisions of this Section 16.8 shall not apply to or encompass sublicensing of the rights licensed to a Party under this Agreement.

16.9 Governing Law. This Agreement shall be governed by and construed and enforced under the laws of England, excluding any conflicts or choice of law rule or principle that might otherwise make this Agreement subject to the substantive law of another jurisdiction. Any disputes, controversies or differences which may arise between the Parties out of or in relation to or in connection with this Agreement, shall be governed by and construed and enforced in accordance with the laws of England and the Parties hereby irrevocably submit to the exclusive jurisdiction of the English Courts. Notwithstanding the foregoing, (a) any dispute relating to the inventorship, scope, validity, enforceability or infringement of any Patent right shall be governed by and construed and enforced in accordance with the patent laws of the applicable jurisdiction, (b) each Party shall have at any time the right to seek or obtain preliminary, interim or conservatory measures from any court having jurisdiction, and (c) each Party may seek to enforce any final judgment of a court in any other court.

16.10 Performance by Affiliates. Subject to the terms and conditions of this Agreement, each Party may discharge any obligations and exercise any right hereunder through any of its Affiliates. Each Party hereby guarantees the performance by its Affiliates of such Party’s obligations under this Agreement, and shall cause its Affiliates to comply with the provisions of this Agreement in connection with such performance. Any breach by a Party’s Affiliate of any of such Party’s obligations under this Agreement shall be deemed a breach by such Party, and the other Party may proceed directly against such Party without any obligation to first proceed against such Party’s Affiliate.

16.11 Personal Rights. None of the provisions of this Agreement is intended to provide any rights or remedies to any Person other than the Parties hereto and their respective successors and assigns (if any).

16.12 Further Actions. Each Party agrees to execute, acknowledge and deliver such further instruments, and to do all such other acts, as may be necessary or appropriate in order to carry out the purposes and intent of this Agreement.

16.13 Compliance with Applicable Law. Each Party shall comply with Applicable Law in the course of performing its obligations or exercising its rights pursuant to this Agreement. Neither Party (nor any of their Affiliates) shall be required under this Agreement to take any action or to omit to take any action otherwise required to be taken or omitted by it under this Agreement if the taking or omitting of such action, as the case may be, could in its opinion violate any settlement, consent order or decree, corporate integrity agreement, or judgment to which it may be subject from time to time during the Term. Notwithstanding anything to the contrary in this Agreement, neither Party nor any of its Affiliates shall be required to take, or

shall be penalized for not taking, any action that such Party reasonably believes is not in compliance with Applicable Law.

16.14 Severability. If any one or more of the provisions of this Agreement are held to be invalid or unenforceable by an arbitrator or any court of competent jurisdiction from which no appeal can be or is taken, the provision shall be considered severed from this Agreement and shall not serve to invalidate any remaining provisions hereof. The Parties shall make a good faith effort to replace any invalid or unenforceable provision with a valid and enforceable one such that the objectives contemplated by the Parties when entering this Agreement may be realized.

16.15 No Waiver. Neither Party may waive or release any of its rights or interests in this Agreement except in writing. The failure of either Party to assert a right hereunder or to insist upon compliance with any term or condition of this Agreement shall not constitute a waiver of that right or excuse a similar subsequent failure to perform any such term or condition. No waiver by either Party of any condition or term in any one or more instances shall be construed as a continuing waiver of such condition or term or of another condition or term.

16.16 Interpretation. The captions and headings to this Agreement are for convenience only, and are to be of no force or effect in construing or interpreting any of the provisions of this Agreement. Unless specified to the contrary, references to Articles, Sections or Exhibits mean the particular Articles, Sections or Exhibits of this Agreement and references to this Agreement include all Exhibits hereto. Unless context otherwise clearly requires, whenever used in this Agreement: (a) the words “include”, “includes” or “including” shall be construed as incorporating also the phrase “but not limited to” or “without limitation”; (b) the word “day” or “quarter” shall mean a calendar day or quarter, unless otherwise specified; (c) the word “notice” shall mean notice in writing (whether or not specifically stated) and shall include notices, consents, approvals and other written communications contemplated under this Agreement; (d) the words “hereof,” “herein,” “hereby” and derivative or similar words refer to this Agreement (including any Exhibits); (e) provisions that require that a Party, the Parties or the JC hereunder to “agree,” “consent” or “approve” or the like shall require that such agreement, consent or approval be specific and in writing, whether by written agreement, letter, approved minutes or otherwise; (f) words of any gender include the other gender; (g) words using the singular or plural number also include the plural or singular number, respectively; (h) references to any specific law, rule or regulation, or article, section or other division thereof, shall be deemed to include the then-current amendments thereto or any replacement law, rule or regulation thereof; and (i) the word “will” shall be construed to have the same meaning and effect as the word “shall”. Ambiguities, if any, in this Agreement shall not be construed against any Party, irrespective of which Party may be deemed to have authored the ambiguous provision. The language of this Agreement shall be deemed to be the language mutually chosen by the Parties and no rule of strict construction shall be applied against either Party hereto. This Agreement should be interpreted in its entirety and the fact that certain provisions of this Agreement may be cross-referenced in a Section shall not be deemed or construed to limit the application of other provisions of this Agreement to such Section and vice versa.

16.17 Counterparts. This Agreement may be executed in counterparts with the same effect as if each signatory had signed the same document, each of which shall be deemed an

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

IN WITNESS WHEREOF, the Parties have caused this Option and License Agreement to be executed by their duly authorized representatives, and BNInc has executed this Option and License Agreement as a deed, effective as of the Effective Date.

Bristol-Myers Squibb Company	Bavarian Nordic A/S

By:	By:	[***]

Name:	Name:	[***]

Title:	Title:	President & CEO

Solely with respect to the BNInc Provisions:

Executed as a deed by:

Bavarian Nordic Inc.

By:

Name:

Title:

In the presence of:

Signature:

Name:

Address:

Occupation:

***Text Omitted and Filed Separately

with the Securities and Exchange Commission.

Confidential Treatment Requested

Under 17 C.F.R. Sections 200.80(b)(2), (4), (5) and (6) and 230.406

Bristol-Myers Squibb Company			Bavarian Nordic A/S

By:	[***]		By:

Name:	[***]		Name:

Title:	Chief Financial Officer		Title:


Solely with respect to the BNInc Provisions:

Executed as a deed by:

Bavarian Nordic Inc.

By:	[***]

Name:	[***]

Title:	President

In the presence of:

Signature:		[***]

Name:		[***]

Address:		2425 Garcia Avenue
		Mountain View
Occupation:		SVP Business Development

	*Per ADS*	*Total*

Price to the public	$	$
Underwriting commission⁽¹⁾	$	$
Proceeds, before expenses, to us	$	$


American Depositary Shares (ADSs) offered by us		ADSs
ADSs		Each ADS represents one-third of a share. As an ADS holder, you will not be treated as one of our shareholders, you will not have shareholder rights, and you may not be able to exercise your right to vote the shares underlying your ADSs. You will have the contractual rights of an ADS holder as provided in the deposit agreement among us, the depositary and holders and beneficial owners of ADSs from time to time. ADS holders may only exercise voting rights with respect to the shares underlying the ADSs in accordance with the provisions of the deposit agreement, which provides that a holder may vote the shares underlying any ADSs for any particular matter to be voted on by our shareholders either by withdrawing the shares underlying the ADSs or, to the extent permitted by applicable law and as permitted by the depositary, by requesting a temporary registration as shareholder and authorizing the depositary to act as proxy. At our 2016 annual general meeting, we intend to propose that our articles of association be amended to permit pass-through voting by ADS holders, who, assuming the success of such proposal, would thereafter be permitted to indicate their voting preference to the depositary in accordance with and subject to the depositary's procedures. The depositary will try, as far as practical, to vote the shares underlying the ADSs as instructed by ADS holders. To better understand the terms of the ADSs, see the sections of this Prospectus entitled "Description of American Depositary Shares" and "Risk Factors—Risks Related to this Offering." We also encourage you to read the deposit agreement, which is filed as an exhibit to the registration statement of which this prospectus forms a part.
Shares to be outstanding after this offering		shares (including shares underlying the ADSs issued in this offering), provided the option granted to the underwriters to purchase up to additional ADSs is not exercised. If the underwriters exercise the option to purchase additional ADSs in full, the shares outstanding after this offering will be shares. See the calculation of our shares to be outstanding after this offering on page 11 of this prospectus.
Option to purchase additional ADSs		We have granted the underwriters an option, exercisable within 30 days from the date of this prospectus, to purchase up to additional ADSs representing shares.
Depositary		Deutsche Bank Trust Company Americas


Use of proceeds		We estimate that the net proceeds from this offering will be approximately $ million, or approximately $ million if the underwriters exercise their option to purchase additional ADSs in full after deducting the underwriting commission and estimated offering expenses payable by us, based on an assumed initial public offering price of $ per ADS, the U.S. dollar equivalent of the closing price of our shares on Nasdaq Copenhagen on , 2016 of DKK , at the U.S. dollar/DKK exchange rate of as of , 2016 and an ADS-to-share ratio of 3:1. We expect to use the net proceeds from this offering to advance our infectious disease and cancer immunotherapy portfolios, to build line extensions to our existing manufacturing capabilities and to fund working capital and for general corporate purposes.
		See "Use of Proceeds" for a more complete description of the intended use of proceeds from this offering.
Risk factors		See "Risk Factors" and other information included in this prospectus for a discussion of factors that you should consider carefully before deciding to invest in the ADSs.
Proposed symbol on The NASDAQ Global Select Market		"BAVN"

	As of September 30, 2015

	Actual				Pro Forma(1)
(in millions)	$(2)		DKK		$(2)	DKK
Securities, cash and cash equivalents	$	185.3		1,233.9	$
Total assets	$	321.2		2,139.1	$
Retained earnings	$	158.0		1,052.1	$
Equity	$	195.6		1,302.7	$
Non-current debt to credit institutions	$	4.7		31.8	$
Current debt to credit institutions	$	0.3		2.0	$
Total liabilities	$	125.6		836.4	$

	As of September 30, 2015

	Actual						Pro Forma(1)
(in millions)	$(2)			DKK			$(2)	DKK
Cash and cash equivalents	$	69.4			462.0		$



Debt
Credit institutions	$	5.1			33.8		$

Total debt		5.1			33.8		$
Equity
Share capital⁽³⁾		41.8			278.3
Retained earnings		158.0			1,052.1
Other reserves		(4.2	)		(27.7	)

Total equity		195.6			1,302.7

Total capitalization	$	200.7			1,336.4


The Kingdom of Denmark (State or other jurisdiction of incorporation or organization)		2836 (Primary Standard Industrial Classification Code Number)		NOT APPLICABLE (I.R.S. Employer Identification Number)


Copies to:
Divakar Gupta Joshua A. Kaufman John Wilkinson Cooley LLP The Grace Building 1114 Avenue of the Americas New York, NY 10036 Telephone: (212) 479-6000 Facsimile: (212) 479-6275		Jonathan L. Kravetz Brian P. Keane John T. Rudy Mintz, Levin, Cohn, Ferris, Glovsky and Popeo, P.C. One Financial Center Boston, MA 02111 Telephone: (617) 542-6000 Facsimile: (617) 542-2241


PROSPECTUS (Subject to Completion)		Dated January 11, 2016

		Page

Presentation of Financial Information			ii
Presentation of Share Information			ii
Prospectus Summary			1
Risk Factors			14
Special Note Regarding Forward-Looking Statements			46
Market, Industry and Other Data			48
Use of Proceeds			49
Dividend Policy			50
Capitalization			51
Dilution			52
Exchange Rate Information			54
Selected Consolidated Financial Data			55
Management's Discussion and Analysis of Financial Condition and Results of Operations			57
Business			77
Management			132
Certain Relationships and Related Party Transactions			145
Principal Shareholders			146
Description of Share Capital			148
Description of American Depositary Shares			164
Shares and ADSs Eligible for Future Sale			175
Certain Material U.S. Federal Income Tax Considerations			177
Certain Material Danish Income Tax Considerations			183
Underwriting			187
Expenses of This Offering			196
Legal Matters			196
Experts			196
Enforcement of Civil Liabilities			197
Where You Can Find More Information			197
Index to Consolidated Financial Statements			F-1


Assumed initial public offering price per ADS⁽¹⁾					$
Historical net tangible book value per ADS as of September 30, 2015⁽²⁾
Increase in pro forma net tangible book value per ADS attributable to new investors

Pro forma net tangible book value per ADS after this offering

Dilution per ADS to new investors participating in this offering					$

	Shares or Share Equivalents(1) Subscribed For/ Purchased

							Average Price Per Share or Share Equivalents
				Total Consideration
	Number	Percent		Amount	Percent
Existing shareholders			%	$		%	$
Investors participating in this offering			%	$		%	$

Total			%	$		%	$

	Period-end

	(DKK per U.S. dollar)
Year Ended December 31:
2013		5.4127	5.6160	5.4002	5.8371
2014		6.1214	5.6190	5.3492	6.1214
2015		6.8300	6.7269	6.1807	7.0806
Nine Months Ended:
September 30, 2014		5.9152	5.5085	5.3492	5.9152
September 30, 2015		6.6588	6.6973	6.1807	7.0806
Month Ended:
July 31, 2015		6.8036	6.7836	6.6721	6.8757
August 31, 2015		6.6544	6.7013	6.4866	6.8563
September 30, 2015		6.6588	6.6493	6.5340	6.6982
October 31, 2015		6.7694	6.6411	6.5226	6.8231
November 30, 2015		7.0521	6.9497	6.7608	7.0521
December 31, 2015		6.8300	6.8627	6.7893	7.0379

	Year Ended December 31,

	2014				2013			Change
(in millions)	$		DKK		DKK			DKK			%
Revenue	$	182.7		1,216.8		1,212.5			4.3			0%
Production costs		74.4		495.1		484.7			10.4			2%

Gross profit		108.3		721.7		727.8			(6.1	)		(1%	)
Research and development costs		71.9		478.9		496.6			(17.7	)		(4%	)
Distribution costs		6.8		45.1		40.8			4.3			11%
Administrative costs		27.1		181.0		157.0			24.0			15%

Income before interest and tax (EBIT)		2.5		16.7		33.4			(16.7	)		(50%	)
Financial income		8.6		57.3		6.6			50.7			768%
Financial expenses		1.5		9.7		33.8			(24.1	)		(71%	)

Income before company tax		9.6		64.3		6.2			58.1			937%
Tax on income for the year		5.7		38.4		52.9			(14.5	)		(27%	)

Net profit (loss) for the period	$	3.9		25.9		(46.7	)		72.6			—%

	Payments due by period

(DKK in millions)	2015		2016		2017		2018		2019		After 2019		Total
Contractual obligations:
Short and long-term debt⁽¹⁾		3.5		3.5		3.5		3.5		3.5		32.9		50.4
Operating lease obligations		20.7		20.6		8.2		6.2		—		—		55.7
Collaborative agreements		13.4		14.1		38.6		—		3.1		12.2		81.4
Other contractual obligations		27.5		0.2		—		—		—		—		27.7

Total contractual obligations		65.1		38.4		50.3		9.7		6.6		45.1		215.2

	Payments due by period

($ in millions)	2015		2016		2017		2018		2019		After 2019		Total
Contractual obligations:
Short and long-term debt⁽¹⁾	$	0.5	$	0.5	$	0.5	$	0.5	$	0.5	$	4.9	$	7.4
Operating lease obligations		3.2		3.2		1.3		0.9		—		—		8.6
Collaborative agreements		2.0		2.1		5.8		—		0.5		1.8		12.2
Other contractual obligations		4.1		—		—		—		—		—		4.1

Total contractual obligations	$	9.8	$	5.8	$	7.6	$	1.4	$	1.0	$	6.7	$	32.3


Cowen and Company		Piper Jaffray
Nomura


Martin Faarborg State Authorised Public Accountant		Henrik Kjelgaard State Authorised Public Accountant

Product	Partner	Summary Description of Contract	Upfront Payment to Bavarian Nordic	Potential Options & Milestones Payments to Bavarian Nordic	Date of Contract

*PROSTVAC*	Bristol-Myers Squibb	Global commercialization	$60 million	$915 million	March 2015
*MVA-BN Filo*	Janssen	Product license agreement	$25 million plus $43 million equity investment	Up to $20 million in regulatory, sales and development milestones	October 2014
*MVA-BN HPV*	Janssen	Collaboration and License Agreement	$9 million	Up to $162 million in regulatory, sales and development milestones	December 2015
			Amounts Received (Paid)	Contingent Amounts to be Received (Paid)

*MVA-BN Filo*	Janssen	Supply contract (approximately 2,000,000 doses)	$71 million; $16 million pro rata as bulk are delivered	$12 million pro rata as bulk are delivered	October 2014
*IMVAMUNE/IMVANEX (liquid frozen)*	BARDA	Contract for bulk order	N/A	$133 million	July 2015
*IMVAMUNE/IMVANEX (freeze dried)*	BARDA	Vaccine development contract	$60 million	$34 million	April 2011
*PROSTVAC*	NCI/PHS	License Agreement	($7 million)	($17 million)	August 2008
*CV 301 and Brachyury*	NCI/PHS/NIH	License Agreements	($4 million)	($18 million)	October 2011

Name	Age	Position(s)

Paul Chaplin	48	President and Chief Executive Officer
Ole Larsen	50	Executive Vice President, Chief Financial Officer

Time of grant / warrant program		Exercise period(s)

August 2011	54.1	Two weeks after publication of Q1 2016 report	5,000	—	—	—	10,000	15,000
May 2012	54	Two weeks after publication of the annual report for 2015 and/or two weeks after publication of Q2 2016 report and/or two weeks after publication of annual report for 2016	—	—	—	7,500	22,500	30,000
August 2012	59.1	Two weeks after publication of Q1 2016 report and/or two weeks after publication of Q3 2016 report and/or two weeks after publication of Q1 2017 report	20,000	25,000	25,000	115,501	48,002	233,503
February 2013	55	Two weeks after publication of annual report for 2015 and/or two weeks after Q2 2016 report and/or two weeks after publication of annual report for 2016 report and/or two weeks after Q2 2017 report	—	—	—	—	40,000	40,000
August 2013	73.9	Two weeks after publication of Q3 2016 report and/or two weeks after publication of Q1 2017 report and/or two weeks after publication of Q3 2017 report and/or two weeks after publication of Q1 2018 report	25,000	30,000	30,000	178,700	179,900	443,600
December 2013	96.5	Two weeks after publication of annual report for 2016 and/or two weeks after publication of Q2 2017 report and/or two weeks after publication of annual report for 2017 and/or two weeks after publication of Q2 2018 report	—	—	—	30,000	40,000	70,000
August 2014	131.4	Two weeks after publication of Q3 2017 report and/or two weeks after publication of annual report for 2017 and/or two weeks after publication of Q1 2018 report and/or two weeks after publication of Q2 2018 report and/or two weeks after publication of Q3 2018 report and/or two weeks after publication of annual report for 2018 and/or two weeks after publication of Q1 2019 report and/or two weeks after publication of Q2 2019 report	—	50,000	40,000	292,500	75,000	457,500
December 2015(1)	366.85	Two weeks after publication of annual report for 2018 and/or two weeks after publication of Q1 2019 report and/or two weeks after publication of Q2 2019 report and/or two weeks after publication of Q3 2019 report and/or two weeks after publication of annual report for 2019 and/or two weeks after publication of Q1 2020 report and/or two weeks after publication of Q2 2020 report and/or two weeks after publication of Q3 2020 report	—	41,005	28,797	265,200	—	335,002

Total			50,000	146,005	123,797	889,401	415,402	1,624,605

2014 - 2017 program

Total number of awarded phantom shares as of December 31, 2015	96.5	144	144	58,558	58,846
Expected maximum number of phantom shares per December 31, 2016	96.5	216	216	88,018	88,450

2015 - 2018 program

Total number of awarded phantom shares as of December 31, 2015	212.25	72	72	28,996	29,140
Expected maximum number of phantom shares per December 31, 2017	212.25	216	216	87,904	88,336

	Beneficial Ownership Prior to this Offering									Beneficial Ownership After this Offering

			Number of Warrants Exercisable Within 60 Days		Fully Diluted Number of Shares Beneficially Owned					Beneficial Ownership After this Offering
Name and Address of Beneficial Owner	Number of Shares Beneficially Owned		Number of Warrants Exercisable Within 60 Days		Fully Diluted Number of Shares Beneficially Owned		Fully Diluted Percentage of Beneficial Ownership			Number of Shares Beneficially Owned		Percentage of Beneficial Ownership
5% and Greater Shareholders
ATP, Denmark⁽¹⁾		2,106,972		—		2,106,972		8.3	%
Board Members, Board Member Nominee and Executive Management
Anders Gersel Pedersen		500		—		500		*			500
Claus Braestrup		6,385		—		6,385		*			6,385
Erik Gregers Hansen⁽²⁾		29,000		—		29,000		*			29,000
Frank Verwiel
Gerard van Odijk		4,000		—		4,000		*			4,000
Ole Larsen		6,000		—		6,000		*			6,000
Peter Kürstein⁽³⁾		6,665		—		6,665		*			6,665
Paul Chaplin		26,800		—		26,800		*			26,800
All board members, board member nominee and executive management as a group (8 persons)		79,350		—		79,350		*			79,350



Share capital at December 31, 2005			5,797,055	57,970,550
2006
Capital increase, March 2006 at a price of DKK 410 per share (private placement)	579,125	237.4	6,376,180	63,761,800
2007
Capital increase, February 2007 at a price of DKK 365 per share (1:5 rights issue)	1,275,236	465.5	7,651,416	76,514,160
Capital increase, May 2007 at a price of DKK 283 per share (exercise of employee warrants)	155,603	44.0	7,807,019	78,070,190
Capital increase, May 2007 at a price of DKK 437 per share (exercise of employee warrants)	8,549	3.7	7,815,568	78,155,680
2009
Non-cash contribution, November 2009 (payment of minority interests in BNIT)	136,177		7,951,745	79,517,450



2010
Capital increase, February 2010 at a price of DKK 80 per share (1:2 rights issue)	3,960,307	316.8	11,912,052	119,120,520
Capital increase, November 2010 at a price of DKK 195 per share (private placement)	1,050,000	204.8	12,962,052	129,620,520
2011
Capital increase, May 2011 at a price of DKK 54 per share (1:1 rights issue)	12,918,593	697.6	25,880,645	258,806,450
Debt conversion, November 2011 at a price of DKK 38,65 per share (U.S. employee program)	213,716		26,094,361	260,943,610
2014
Capital increase, May 2014 at a price of DKK 114 per share (exercise of employee warrants)	18,502	2.1	26,112,863	261,128,630
Capital increase, October 2014 at a price of DKK 188,44 per share (private placement)	1,331,984	250.9	27,444,847	274,448,470
Capital increase, November 2014 at a price of DKK 54,1 per share (exercise of employee warrants)	121,750	6.6	27,566,597	275,665,970
Capital increase, November 2014 at a price of DKK 54,1 per share (exercise of employee warrants)	104,650	5.7	27,671,247	276,712,470
2015
Capital increase, March 2015 at a price of DKK 194 per share (exercise of employee warrants)	39,203	7.6	27,710,450	277,104,500
Capital increase, March 2015 at a price of DKK 192 per share (exercise of employee warrants)	21,543	4.1	27,731,993	277,319,930
Capital increase, May 2015 at a price of DKK 54,1 per share (exercise of employee warrants)	80,000	4.3	27,811,993	278,119,930
Capital increase, September 2015 at a price of DKK 194 per share (exercise of employee warrants)	3,881	0.8	27,815,874	278,158,740
Capital increase, September 2015 at a price of DKK 54 per share (exercise of employee warrants)	18,500	1.0	27,834,374	278,343,740
Capital increase, November 2015 at a price of DKK 54.1 per share (exercise of employee warrants)	35,500	1.9	27,869,874	278,698,740
Capital increase, November 2015 at a price of DKK 59.1 per share (exercise of employee warrants)	149,797	8.9	28,019,671	280,196,710


Service		Fees
§ to any person to whom ADSs are issued or to any person to whom a distribution is made in respect of ADS distributions pursuant to stock dividends or other free distributions of stock, bonus distributions, stock splits or other distributions (except where converted to cash)		Up to $0.05 per ADS issued
§ to any person surrendering ADSs for withdrawal of deposited securities, including, inter alia, cash distributions made pursuant to a cancellation or withdrawal		Up to $0.05 per ADS cancelled
§ distribution of cash dividends		Up to $0.05 per ADS held
§ distribution of cash proceeds, including proceeds from the sale of rights and other entitlements, not made pursuant to a cancellation or withdrawal		Up to $0.05 per ADS held
§ distribution of ADSs pursuant to exercise of rights		Up to $0.05 per ADS held
§ depositary services		Up to $0.05 per ADS held on the applicable record date(s) established by the depositary bank

Underwriter		Number of ADSs

Cowen and Company, LLC
Piper Jaffray & Co.
Nomura Securities International, Inc.

Total

		Total

	Per ADS	Without Overallotment	With Overallotment
Public offering price	$	$	$
Underwriting commission	$	$	$
Proceeds, before expenses, to us	$	$	$

Item	Amount to be paid

SEC registration fee	$		*
FINRA filing fee		2,000
The NASDAQ Global Select Market Listing fee		25,000
Printing and engraving expenses			*
Legal fees and expenses			*
Accounting fees and expenses			*
Miscellaneous expenses			*

Total	$		*

DKK thousand

Revenue	3	1,216,815	1,212,501
Production costs	4,8,9	495,081	484,705

Gross profit		721,734	727,796

Research and development costs	5,8,9	478,930	496,608
Distribution costs	6,8,9	45,107	40,782
Administrative costs	7,8,9,10	181,022	156,991

Total operating costs		705,059	694,381

Income before interest and tax (EBIT)		16,675	33,415

Financial income	11	57,385	6,612
Financial expenses	12	9,700	33,825

Income before company tax		64,360	6,202

Tax on income for the year	13	38,420	52,931

Net profit for the year		25,940	(46,729	)



Earnings per share (EPS)—DKK
Basic earnings per share of DKK 10	14	1.0	(1.8	)
Diluted earnings per share of DKK 10	14	1.0	(1.8	)

DKK thousand

Non-current assets
Acquired licenses		24,719	20,517
Software		4,835	3,208
IMVAMUNE/IMVANEX development project		78,357	76,955
Other intangible assets in progress		1,283	3,949

Intangible assets	15	109,194	104,629

Land and buildings		226,144	178,085
Leasehold improvements		892	1,293
Plant and machinery		64,606	82,796
Other fixtures and fittings, other plant and equipment		20,900	21,265
Assets under construction		24,031	39,307

Property, plant and equipment	16	336,573	322,746

Other receivables	19	792	831

Financial assets		792	831

Deferred tax assets	13	121,586	123,631

Total non-current assets		568,145	551,837



Current assets
Inventories	17	121,847	233,651

Trade receivables	18	186,783	110,117
Tax receivables		4,913	—
Other receivables	19	14,516	12,614
Prepayments	20	11,357	11,906

Receivables		217,569	134,637

Securities	22	581,350	185,282
Cash and cash equivalents		398,357	346,799

Securities, cash and cash equivalents		979,707	532,081

Total current assets		1,319,123	900,369



Total assets		1,887,268	1,452,206

DKK thousand

Equity
Share capital		276,712	260,944
Retained earnings		972,321	652,021
Other reserves		3,061	63,325

Equity		1,252,094	976,290



Liabilities
Provisions	23	18,603	14,830
Debt to credit institutions	24	33,293	71,834

Non-current liabilities		51,896	86,664

Debt to credit institutions	24	1,885	8,481
Prepayment from customers	25	375,190	150,425
Trade payables		58,666	113,510
Company tax		40	496
Provisions	23	4,214	2,273
Other liabilities	21	143,283	114,067

Current liabilities		583,278	389,252

Total liabilities		635,174	475,916



Total equity and liabilities		1,887,268	1,452,206



Significant accounting policies	1
Significant accounting estimates, assumptions and uncertainties	2
Financial risks and financial instruments	22
Related party transactions	26
Share-based payment	27
Contingent liabilities and other contractual obligations	28
Significant events after the balance sheet date	29
Approval of the consolidated financial statements	30

DKK thousand

Equity as of January 1, 2014	260,944	652,021		6,367		56,958		976,290
Comprehensive income for the year
Net profit for the year	—	25,940		—		—		25,940
Other comprehensive income
Exchange rate adjustments on translating foreign operations	—	—		(41,552	)	—		(41,552	)
Total comprehensive income for the year	—	25,940		(41,552	)	—		(15,612	)
Transactions with owners
Share-based payment	—	—		—		6,888		6,888
Warrant programs exercised	2,448	18,342		—		(6,433	)	14,357
Warrant programs expired		38,438				(38,438	)	—
Capital increase through direct placement	13,320	237,680		—		—		251,000
Costs related to issue of new shares	—	(100	)	—		—		(100	)
Tax related to items recognized directly in equity	—	—		—		19,271		19,271
Total transactions with owners	15,768	294,360		—		(18,712	)	291,416

Equity as of December 31, 2014	276,712	972,321		(35,185	)	38,246		1,252,094

DKK thousand

Equity as of January 1, 2013	260,944	683,032		(6,341	)	(549	)	62,590		999,676
Comprehensive income for the year
Net profit for the year	—	(46,729	)	—		—		—		(46,729	)
Other comprehensive income
Exchange rate adjustments on translating foreign operations	—	—		12,708		—		—		12,708
Fair value of financial instruments	—	—		—		549		—		549
Total comprehensive income for the year	—	(46,729	)	12,708		549		—		(33,472	)
Transactions with owners
Share-based payment	—	—		—		—		10,086		10,086
Warrant programs expired	—	14,515		—		—		(14,515	)	—
Adjustment	—	1,203		—		—		(1,203	)	—
Total transactions with owners	—	15,718		—		—		(5,632	)	10,086

Equity as of December 31, 2013	260,944	652,021		6,367		—		56,958		976,290

DKK thousand

Share capital as of January 1	260,944	260,944	260,944	129,620	79,517
Issue of new shares	15,768	—	—	131,324	50,103

Share capital as of December 31	276,712	260,944	260,944	260,944	129,620

Company summary	Domicile

Subsidiaries
Bavarian Nordic GmbH	Germany	100	%	100	%
Bavarian Nordic, Inc.	USA	100	%	100	%
Aktieselskabet af 1. juni 2011 I	Denmark	100	%	100	%
BN Infectious Diseases A/S	Denmark	100	%	100	%
Bavarian Nordic Washington DC, Inc.	USA	100	%	100	%
Representative office
Bavarian Nordic A/S	Singapore

DKK thousand

IMVAMUNE/IMVANEX sale	1,024,236	839,143

IMVAMUNE/IMVANEX sale, development results	—	172,988
Contract work	192,579	200,370

Sale of services	192,579	373,358

Revenue	1,216,815	1,212,501