SAN FRANCISCO, Dec. 23, 2021 /PRNewswire/ -- Every day, the
billions of bacteria that inhabit your digestive system change; the
food you eat, medications you take, and germs you're exposed to
make some bacteria flourish more than others. Scientists know that
this ever-shifting balance of gut microbes is linked to your health
and disease, but have struggled to pin down what makes one
microbial balance better than another.
Over the past decade, scientists have generally described a
person's microbiome—the collection of microbes found in the human
gut—by characterizing what species of bacteria are present, and in
what amounts. Now, a group of researchers led by Katie Pollard, PhD, at Gladstone Institutes have
published two new studies that suggest monitoring the strains of
bacteria—and not just the species—may provide better insights into
the microbiome.
Bacterial strains are a little like dog breeds or tomato
varieties—parts of the same species, yet distinct from one
another.
"I think researchers have been missing a lot of information by
just focusing on the species of microbes," says Pollard, director
of the Gladstone Institute of Data Science and Biotechnology and
lead author of the two studies. "When we take a more fine-grained
approach and look at the strains of bacteria, I predict that we'll
start finding causal links between the microbiome and
diseases."
In one study published in the journal Nature
Biotechnology, Pollard's lab worked with Stephen Nayfach, PhD, a research scientist at
the US Department of Energy Joint Genome Institute, to develop
a new computational method to analyze the strains of bacteria
present in a microbiome sample much more quickly and affordably
than existing technologies. The new approach, Pollard says, will
enable researchers to carry out bigger and more precise analyses of
the microbiome than ever before.
In a separate paper published online in Genome Research,
Pollard collaborated with the labs of Benjamin Good, PhD, and Michael Snyder, PhD, at Stanford University to track the strains of
bacteria present in one person's microbiome at 19 different time
points over a 5-month period, including before and after a course
of antibiotics. They found that, in some cases, the abundance of a
species of bacteria remained constant between time points, but the
strains within that species changed dramatically.
Making Microbiomes Meaningful
Inside your gut, bacteria probably do more than just digest your
food. Indeed, studies have shown that people with diseases as
diverse as inflammatory bowel disease, asthma, autism, diabetes,
and cancer have different bacteria in their digestive systems
compared to healthy people. But few treatments targeting the
microbiome have emerged from these observations so far.
Since every bacterium has its own genetic code, scientists rely
on DNA sequencing to uncover what bacteria inhabits any given
person's microbiome. But analyzing the DNA sequences is difficult
due to the size and complexity of the data. Although researchers
can use existing methods to determine what species are present,
these only provide part of the picture of the microbiome's
diversity and function. That's because the different strains in a
single species of bacteria can harbor significant genetic
differences, which are often large enough to induce different
behaviors.
Until now, identifying genetic differences in a microbiome
sample has required high-performance computing power and cloud
storage—something not available to most labs. Researchers had to
compare millions of DNA fragments from the genomes of thousands of
bacteria present in the microbiome to a database with the sequences
of every known microorganism, using a technique known as sequence
alignment.
"The algorithms to analyze genetic sequences were developed for
human genomes," says Pollard, who is also a professor at UC San
Francisco and a Chan Zuckerberg Biohub investigator. "They work
great for the challenge of sequencing a single organism's genome,
but not for our purposes of sequencing the genomes of thousands of
unknown organisms at once."
Pollard and her colleagues knew that long stretches of genome
sequences are common among many bacterial species or strains. So,
these sequences cannot be used to help pinpoint a specific
bacterial strain. Inspired by approaches that analyze only the most
variable regions of the human genome, the team set out to find the
minimum amount of sequence information they'd need to cull from the
microbiome data to identify what strains it contained.
The researchers analyzed over 100,000 publicly available and
high-quality genomes from approximately 900 bacterial species
commonly found in the human gut. They discovered 104 million short
strings of DNA in the bacterial genomes that vary most often
between strains of bacteria. Then, they used this information to
design a new algorithm, dubbed GenoTyper for Prokaryotes (GT-Pro),
that searches the microbiome sequence data for exact matches to the
key strings that act as identifiers for bacterial strains. Unlike
previous sequence alignment methods, GT-Pro fits in the memory of a
laptop and doesn't require high-performance computing and cloud
credits.
"With the explosion of newly sequenced genomes from the gut
microbiome and other environments, we can now create detailed
genetic maps for thousands of bacterial species," says Nayfach.
"Our approach leverages this prior information to rapidly and
comprehensively identify the genetic variants in a microbiome
sample without performing time-consuming sequence alignments."
The research field has previously been limited by the fact that
only a few labs around the world have the money or computer
hardware to analyze microbiome data at the resolution of
strains.
"Our new algorithm opens the door for everyone to be able to
achieve this level of resolution on a personal computer," says
Pollard.
Before and after Antibiotics
One of the questions that microbiome researchers have been
striving to answer in recent years is how much the microbiome
changes in one person's body over time. This question has been
addressed at a species level; scientists have tracked how the
species composition of people's microbiomes changes along with
diet, disease, or environmental changes. But results have failed to
explain how the microbiome gains new functions, such as antibiotic
resistance or the ability to inactivate chemotherapy drugs, when
species composition remains stable from month to month.
Pollard and her colleagues wanted to delve into this question at
a deeper level, by analyzing how the strains of bacteria, rather
than just species, change over time. They repurposed a method
designed for sequencing single human cells and used it to barcode
bacterial DNA molecules. This enabled the group to track individual
strains of bacteria in one person over the course of a 5-month
study.
The team sequenced the microbiome of a healthy individual
approximately once a week over 5 months. During that time period,
the subject was surprisingly diagnosed with Lyme disease and
received a 2-week course of antibiotics—known to eliminate many
species of bacteria, including those that live in the human
gut.
"What we assumed is that a lot of microbes would become less
abundant with the antibiotics, and then recover, but the microbiome
at the end would more or less resemble the microbiome at the
start," says Good, assistant professor of applied physics at
Stanford.
In some cases, this was true—certain species, and strains, of
microbes were remarkably resilient, present with nearly unchanged
genomes at the start and finish of the 5-month period. But in other
cases, the strains present after antibiotics were genetically
different from those at the start even though the abundance of the
species did not change. Importantly, these differences would have
been missed if the team had only analyzed the species present in
each microbiome sample.
Although the GT-Pro algorithm was not yet available to be used
in this study, Pollard says it would make similar future studies
much easier—and cheaper—to conduct.
Charting a New Path for Microbiome Studies
The bacteria in your body are like a jungle—a living, changing
ecosystem with organisms co-existing in a delicate balance. When
looking at satellite images from above, ecologists can monitor the
most profound, drastic changes to a jungle, but they'll miss out on
the finer intricacies that shape the environment.
Similarly, those studying the microbiome by watching how species
change have been getting a high-level view of the network, and
seeing only the most obvious connections to health and disease. But
with GT-Pro and a new view of microbe strains, Pollard says, new
links will become apparent.
"There's still a lot of work to be done to understand the
functional consequences of differences in the microbiome," says
Pollard. "But until now, we haven't had the right measurement tools
to ask these questions—and now we do."
About the Studies
The paper "Fast and accurate metagenotyping of the human gut
microbiome with GT-Pro" was published by the journal Nature
Biotechnology on December 23,
2021. Other authors include Zhou
Jason Shi from Gladstone, and Boris
Dimitrov and Chunyu Zhao from
the Chan Zuckerberg Biohub. The study was funded in part by the
National Science Foundation (grant DMS-1563159) and the Chan
Zuckerberg Biohub.
The paper "Longitudinal linked-read sequencing reveals
ecological and evolutionary responses of a human gut microbiome
during antibiotic treatment" was published in the August 2021 issue of the journal Genome
Research. Other authors include Morteza Roodgar, Mohan Avula, Wenyu
Zhou, Samuel Lancaster,
Hayan Lee, Afshin Babveyh, and
Sophia Nesamoney from Stanford University; Nindita Garud of the
University of California, Los Angeles;
and Stephen Martis of the
University of California, Berkeley. The
work was supported in part by the US National Science Foundation
(DMS-1563159) and the Chan Zuckerberg Biohub.
About Gladstone Institutes
To ensure our work does the greatest good, Gladstone Institutes
focuses on conditions with profound medical, economic, and social
impact—unsolved diseases. Gladstone is an independent, nonprofit
life science research organization that uses visionary science and
technology to overcome disease. It has an academic affiliation with
the University of California, San
Francisco.
Media Contact: Julie Langelier |
Associate Director, Communications | julie.langelier@gladstone.org
| 415.734.5000
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