Rethinking Dieting
Scripps Research
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Scientists at Scripps Research have identified a molecule secreted by roundworm intestines that communicates with the brain to reduce the rate of fat loss during periods of food scarcity.
In a scenario that many dieters can likely relate to, the
less a Caenorhabditis elegans (C. elegans) worm eats,
the slower it sheds fat. Researchers at Scripps Research have now uncovered
the reason: a small molecule produced in the worms’ intestines during fasting
travels to the brain, where it blocks a signal responsible for burning fat
during this period.
Although the exact molecule they identified in the worms has
not yet been studied in humans, the new work helps scientists better understand
the complex crosstalk between the gut and the brain. It also may shed light on
why fasting—not eating for set periods of time—has benefits that are
independent from the number of calories a person eats. The new study
was published in Nature Communications on August 11,
2024.
“We’ve found for the first time that fasting is conveying
information to the brain beyond just caloric withdrawal,” says Scripps Research
Professor of Neuroscience Supriya Srinivasan, PhD, the senior author of
the new study. “These findings make me wonder whether there are
molecules made in the guts of other animals, including mammals, that explain
some of the health outcomes associated with fasting.”
Brain-Gut Communication in Fat Metabolism
Researchers have long known that the brain controls the
production and breakdown of fats in humans, other mammals, and model organisms
such as C. elegans. In 2017, Srinivasan’s group identified FLP-7, a brain hormone that triggers fat
burning in the roundworm’s gut. However, C. elegans do
not have sensory nerves in their intestines, so scientists have struggled to
pin down the reverse communication pathway: How does the gut signal the brain?
“We knew that altering the metabolic state of the gut could
change the properties of neurons in the brain, but it was very mysterious how
this actually happened,” says Srinivasan.
In the new work, Srinivasan and her colleagues removed more
than 100 signaling molecules from C. elegans intestines, one
at a time, and measured their impact on the brain’s production of FLP-7. They
found one molecule that had a large effect on FLP-7: a form of insulin known
as INS-7. In humans, insulin is most known as the hormone produced by the
pancreas that controls blood sugar levels. But this insulin molecule was
instead being made by gut cells and also impacting fat metabolism via the
brain.
“When we first found that this was an insulin, we thought it
was paradoxical,” recalls Srinivasan. “Insulin is so well studied in mammals,
and there was no precedent for an insulin molecule having this role.”
Discovery of a Unique Insulin Function
However, when the group probed how INS-7 was impacting
FLP-7-producing brain cells, they found that it was not activating insulin
receptors—as all previously discovered insulin molecules do—but by blocking the
insulin receptor. In turn, this blockade set off a cascade of other molecular
events that eventually made the brain cells stop producing FLP-7.
“INS-7 is basically a signal coming from the intestines that
tells the brain not to burn any more fat stores right now because there’s no
food coming in,” explains Srinivasan.
Studies have previously shown that periods of fasting can
influence the body in a variety of ways, but the mechanisms of those changes
have been unclear. The new study points toward one way that an empty gut can
signal the brain, which could potentially lead to a variety of health impacts
beyond fat.
The new results, Srinivasan says, help explain how the brain
and digestive system communicate in both directions to control metabolism based
on the availability of food. More research is needed to uncover which specific
pathways are involved in new gut-to-brain signals in mammals.
Compounds that mimic gut hormones—such as semaglutide,
commonly known under brand names such as Ozempic, Wegovy, and Rybelus—have
recently emerged as popular ways to control obesity and diabetes, so new gut
peptides could add to this drug class. Srinivasan is also planning experiments
to probe how C. elegans gut cells are triggered to produce
INS-7 during fasting and which types of brain cells are affected by the
molecule.
Reference: “A homeostatic gut-to-brain insulin antagonist
restrains neuronally stimulated fat loss” by Chung-Chih Liu, Ayub Khan, Nicolas
Seban, Nicole Littlejohn, Aayushi Shah and Supriya Srinivasan, 11 August
2024, Nature Communications.
DOI: 10.1038/s41467-024-51077-3
This work was supported by funding from the National
Institutes of Health (R01 DK124706 and R01 AG056648).
