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MXCT Maxcyte Inc

295.00
0.00 (0.00%)
26 Apr 2024 - Closed
Delayed by 15 minutes
Share Name Share Symbol Market Type Share ISIN Share Description
Maxcyte Inc LSE:MXCT London Ordinary Share COM STK USD0.01 (DI)
  Price Change % Change Share Price Bid Price Offer Price High Price Low Price Open Price Shares Traded Last Trade
  0.00 0.00% 295.00 290.00 300.00 295.00 295.00 295.00 5,668 08:00:00
Industry Sector Turnover Profit EPS - Basic PE Ratio Market Cap
Biological Pds,ex Diagnstics 41.29M -37.92M -0.3664 -9.93 376.76M

MaxCyte, Inc. Research & Development Agreement with NIAID (2054H)

06/06/2017 7:01am

UK Regulatory


Maxcyte (LSE:MXCT)
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RNS Number : 2054H

MaxCyte, Inc.

06 June 2017

MaxCyte, Inc.

("MaxCyte" or the "Company")

Cooperative Research and Development Agreement

MaxCyte and National Institute of Allergy and Infectious Diseases to

Collaborate on Research for Ultra-Rare Disease Therapy

- Researchers to explore development of new therapies for X-linked chronic granulomatous disease (CGD) using MaxCyte's gene-correction platform

Maryland, USA - 06 June 2017 - MaxCyte, Inc. (LSE: MXCT, MXCR) today announces it has entered into a Cooperative Research and Development Agreement ("CRADA") with the National Institutes of Health's ("NIH") National Institute of Allergy and Infectious Diseases ("NIAID") to develop treatments for X-linked chronic granulomatous disease ("CGD") using next-generation gene correction leveraging CRISPR/Cas9 and MaxCyte's Flow Electroporation(TM) Platform.

CGD is an inherited genetic disorder that impairs the function of the immune system and leads to ongoing and severe bacterial infections. The disease affects approximately 1 in 250,000* people worldwide and is currently only treatable through high-risk treatments, such as allogeneic bone marrow transplantation.

NIAID will conduct pre-clinical research evaluating the effectiveness and safety of CRISPR-Cas9 gene editing on models of CGD by "correcting" the faulty gene that causes the disease. MaxCyte will supply mRNA molecules and focus on leveraging its Flow Electroporation(TM) Platform to develop robust and scalable processes that result in a clinically meaningful correction of mutated gene sequences.

Doug Doerfler, President & CEO of MaxCyte, said: "We are delighted to continue our collaboration with NIAID, one of the world's leading infectious disease institutes, which is leveraging MaxCyte's expertise in developing a new generation of genome editing therapy for CGD patients. We believe that this work will validate the use of our platform for developing gene-editing therapies via rapid, cost-effective manufacturing. This agreement, along with recent data announced from a research effort between MaxCyte and NHLBI of NIH in sickle cell disease, further demonstrates our commitment to deliver new therapies to patients where there is an extremely high unmet medical need."

The MaxCyte/NIAID CRADA marks the latest step in the collaboration between the Company and the NIAID to advance new treatments for CGD, and reflects MaxCyte platform's ability to be used in multiple fields of indication. MaxCyte received Maryland Stem Cell Research Fund grants in 2015 and 2017 to pursue its collaboration with the NIAID to develop preclinical processes and clinical-scale protocols for CGD and other rare diseases. MaxCyte also presented data generated in the collaboration at the 2015 American Society of Gene and Cell Therapy (ASGCT) annual meeting on the ability of genome editing in hematopoietic stem cells to restore oxidase activity. Earlier this year, MaxCyte shared data from the collaboration at the ASGCT's annual meeting highlighting the achievement of therapeutic levels of gene correction in hematopoietic stem cells obtained from CGD patients.

References:

*MedScape

About MaxCyte

MaxCyte (LSE: MXCT, MXCR) is a US-based global company dedicated to driving the acceleration of the discovery, development, manufacturing and commercialization of next-generation, cell-based medicines. The Company provides its patented, high-performance cell engineering platform to biopharmaceutical partners engaged in drug discovery and development, biomanufacturing, and cell therapy, including gene editing and immuno-oncology. With its robust delivery platform, MaxCyte's team of scientific experts helps its partners to unlock their product potential and solve problems. This platform allows for the engineering of nearly all cell types, including human primary cells, with any molecule, at any scale. It also provides a high degree of consistency and minimal cell disturbance, thereby facilitating rapid, large-scale, clinical and commercial grade cell engineering in a non-viral system and with low-toxicity concerns. The Company's cell-engineering platform is FDA-accredited, providing MaxCyte's customers and partners with an established regulatory path to commercialize cell-based medicines. MaxCyte is also developing CARMA, its proprietary, breakthrough platform in immuno-oncology, to rapidly manufacture CAR therapies for a broad range of cancer indications, including solid tumors where existing CAR-T approaches face

significant challenges.   For more information, visit http://www.maxcyte.com/ 

###

 
   MaxCyte Inc. 
    Doug Doerfler, Chief Executive 
     Officer 
     Madhusudan V. Peshwa, PhD, 
     Chief Scientific Officer, 
     Executive Vice President, 
     Cellular Therapies 
     Ron Holtz, Chief Financial 
     Officer                               +1 301 944 1660 
    Nominated Adviser and Broker 
     Panmure Gordon 
    Freddy Crossley (Corporate 
     Finance) 
     Duncan Monteith 
     Ryan McCarthy 
     Tom Salvesen (Corporate Broking)      +44 (0) 20 7886 2500 
    Financial PR Adviser 
     Consilium Strategic Communications 
    Mary-Jane Elliott                      +44 (0)203 709 5700 
     Chris Welsh                            maxcyte@consilium-comms.com 
     Lindsey Neville 
 

This information is provided by RNS

The company news service from the London Stock Exchange

END

AGRDGGDLGSGBGRU

(END) Dow Jones Newswires

June 06, 2017 02:01 ET (06:01 GMT)

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