Gut bacteria brew all sorts of chemicals, but we don't know what most of them do. A new study suggests that one such compound, previously linked to cancer, may serve as a bizarre weapon in microbial skirmishes.
From: Howard Hughes Medical Institute
February 23, 2022 -- Some
gut bacteria have a spooky superpower: they can reanimate dormant viruses
lurking within other microbes.
This viral awakening
unleashes full-blown infections that destroy the virus-carrying cells, Howard
Hughes Medical Institute Investigator Emily Balskus's lab first published as a
preprint on bioRxiv and later in the journal Nature on
February 23, 2022. A cryptic molecule called colibactin can summon the killer
viruses from their slumber, they found.
Microbes often generate
noxious compounds to attack one another within the cramped quarters of the gut.
But among these chemical weapons, colibactin appears unusual, says Balskus, a
chemical biologist at Harvard University. "It doesn't directly kill the
target organisms, which is what we normally think of bacterial toxins doing
within microbial communities." Instead, colibactin tweaks microbial cells
just so, activating latent -- and lethal -- viruses tucked away in some
bacteria's genomes.
Humans have long sought
out the potent compounds that microbes produce. "We know a lot about their
chemical properties, we purify them in the lab, and we use them as medicine,
including antibiotics," says Breck Duerkop, who studies bacterial viruses
at the University of Colorado School of Medicine.
But why bacteria make
these compounds and what effects they have on neighboring organisms are
open-ended questions, says Duerkop, who was not involved in this research. He
calls Balskus's teams new work "one step in the right direction."
Chemical dark matter
Scientists have known
for years that colibactin can wreak havoc on human cells. Research by Balskus
and many others has shown that the compound damages DNA, which can lead to
colorectal cancer. But establishing a connection between this compound and
disease proved particularly formidable.
In 2006, a French team
reported that mammalian cells that encountered the gut bacteria E. coli suffered
fatal damage to their DNA. The researchers linked this damage to a cluster
of E. coli genes encoding machinery for building a complex
molecule. Dubbed colibactin, the molecule was extraordinarily difficult to
study. After many tries, researchers simply couldn't isolate it from the E.
coli making it.
Colibactin is one of
many ephemeral compounds that scientists suspect microbes make. Like invisible
particles of dark matter in space, this "chemical dark matter"
requires creative means to study. As part of her exploration of the gut's
microbial chemistry, Balskus uses indirect approaches to examine these elusive
molecules.
Over the past 10 years,
her team has probed colibactin by studying the microbial machinery that
manufactures it. She and her colleagues have pieced together colibactin's
structure and determined that it damages DNA by forming errant connections
within the double helix.
Building off this work,
scientists elsewhere uncovered a definitive link to cancer: the molecule's
distinctive fingerprints appear in genes known to drive colorectal tumor
growth.
A role for viruses
Balskus's most recent
colibactin study got its start with another disease: COVID-19. Like many other
labs, hers had to rearrange things to reduce physical contact among
researchers. As part of the reshuffling, postdoc Justin Silpe and graduate
student Joel Wong ended up working near one another for the first time. Their
conversations led them and Balskus to wonder how colibactin affected other
microbes in a crowded gut.
Early on, they found
that exposing colibactin-producing bacteria to non-producers had little effect,
suggesting that, on its own, the molecule isn't particularly deadly. Silpe and
Wong weren't sure if colibactin, a large, unstable molecule, could even enter
bacterial cells to damage their DNA. They then wondered if a third party --
bacteria-infecting viruses -- might be involved. Hardly more than bits of
genetic information, these viruses can slip into bacteria's DNA and lie quietly
in wait. Then, once triggered, they cause an infection that blows up the cell
like a landmine.
When the researchers
grew colibactin producers alongside bacteria carrying such latent viruses, they
saw the number of viral particles spike, and the growth of many
virus-containing bacteria drop. That suggested the molecule sparked a surge in
active, cell-killing infections. Colibactin does indeed enter bacteria and
damage DNA, the team showed. That damage sounds a cellular wake-up bell that
rouses the viruses.
Many microbes appeared
equipped to protect themselves against colibactin. Balskus's lab identified a
resistance gene encoding a protein that neutralizes the compound in a wide
variety of bacteria.
Though colibactin
clearly has a dangerous side, it may serve as more than just a lethal weapon,
Balskus says. For example, both DNA damage and awakened viruses can also induce
genetic changes, rather than death, in neighboring bacteria, potentially
benefiting colibactin producers.
Balskus's team's
discoveries suggest that cancer may be collateral damage caused by whatever
else colibactin-producing bacteria are doing. "We always suspected that
bacteria made this toxin to target other bacteria in some way," she says.
"It didn't make sense from an evolutionary perspective that they acquired
it to target human cells."
Next, Balskus plans to
investigate how the compound alters the community of microbes in the gut --
which ones disappear and which thrive after exposure to the compound. "The
key to preventing cancer may be understanding the effects colibactin has on the
microbe community and how its production is controlled," she says.
https://www.sciencedaily.com/releases/2022/02/220223111242.htm
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