Scientific illustration depicting gut bacteria eroding the colon's mucus layer, causing dry stool and constipation, based on Nagoya University research.
Scientific illustration depicting gut bacteria eroding the colon's mucus layer, causing dry stool and constipation, based on Nagoya University research.
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Nagoya University study links chronic constipation to mucus-degrading gut bacteria, suggests new treatment target

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እውነት ተፈትሸ

Researchers at Nagoya University report that two common gut microbes can work together to break down the colon’s protective mucus layer, leaving stool dry and difficult to pass—an effect that standard laxatives may not address. The team also found higher levels of these bacteria in people with Parkinson’s disease, who often experience constipation decades before motor symptoms, and showed in mice that disabling a key bacterial enzyme prevented constipation.

Scientists at Nagoya University in Japan have identified two gut bacteria that appear to work in tandem to promote chronic constipation by eroding the colon’s protective mucus layer. The research, published in the journal Gut Microbes, focuses on Akkermansia muciniphila and Bacteroides thetaiotaomicron, which the researchers say can break down the mucus coating that helps keep the colon lubricated and stool hydrated.

According to the researchers, the mucus loss unfolds in stages. B. thetaiotaomicron produces enzymes that remove sulfate groups from mucin—chemical features the team says normally help protect mucin from being broken down. Once those sulfate groups are removed, A. muciniphila can more readily digest the exposed mucin. As mucin levels fall, stool can lose moisture and become harder and more difficult to pass.

The work is positioned as a possible explanation for why some people with persistent constipation do not respond well to standard therapies that primarily aim to soften stool or stimulate intestinal movement. The Nagoya group highlights chronic idiopathic constipation—constipation without a clear underlying cause—as an area where focusing on the mucus barrier and microbiome could be particularly relevant.

The team also reports a connection to Parkinson’s disease. Parkinson’s patients often experience constipation long before the emergence of hallmark movement symptoms, and the researchers found higher levels of these mucus-degrading bacteria in Parkinson’s patients. While constipation in Parkinson’s disease has frequently been attributed to neurological changes, the findings suggest that bacterial activity in the gut could also contribute to early gastrointestinal symptoms.

To test whether interrupting the process could prevent constipation, the researchers genetically modified B. thetaiotaomicron so it could no longer activate the enzyme sulfatase involved in removing sulfate groups from mucin. Lead author Tomonari Hamaguchi said: “We put these modified bacteria into germ-free mice together with Akkermansia muciniphila, and surprisingly the mice did not develop constipation; the mucin stayed protected and intact.”

In the mouse experiments, disabling that enzyme prevented the bacteria from degrading mucin and prevented constipation, the researchers reported. The team argues that the results point to sulfatase as a potential drug target, though they emphasize that translating the approach to humans would require further study.

More broadly, the findings add to growing research interest in how the gut microbiome may influence digestive symptoms and neurological disease—particularly as constipation can precede Parkinson’s motor symptoms by decades in some patients.

ሰዎች ምን እያሉ ነው

Early reactions on X to the Nagoya University study are neutral to positive, with the university, medical professionals, and news accounts sharing summaries of the discovery that two gut bacteria degrade colon mucus causing laxative-resistant constipation, noting higher levels in Parkinson's patients and potential for new enzyme-targeted treatments.

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Conceptual illustration of gut bacteria producing inflammatory glycogen triggering brain inflammation in C9orf72-linked ALS and FTD, with stool sample comparisons and mouse treatment outcomes.
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Study links microbial glycogen in the gut to inflammation in C9orf72-associated ALS and frontotemporal dementia

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Researchers at Case Western Reserve University report that some gut bacteria can make unusually inflammatory forms of glycogen and that this microbial glycogen can trigger immune activity linked to brain inflammation in models of disease tied to the C9orf72 mutation. In patient stool samples, the team found these glycogen forms more often in ALS and C9orf72-related frontotemporal dementia than in healthy controls, and enzymatically breaking down glycogen in the gut improved outcomes in mice.

Researchers reported at Digestive Disease Week (DDW) 2026 that older mice given fecal microbiota transplants made from their own preserved, younger-age stool samples showed less liver inflammation and injury—and none developed liver cancer in the experiment.

በAI የተዘገበ እውነት ተፈትሸ

A probiotic bacterium isolated from kimchi bound strongly to polystyrene nanoplastics in laboratory experiments and was linked to higher nanoplastic excretion in germ-free mice, according to a research summary released by South Korea’s National Research Council of Science & Technology.

Eliminating sucrose from a low-fat diet worsened glucose tolerance and altered the gut microbiome in mice over 16 weeks, according to results presented on Saturday, June 13, 2026, at ENDO 2026, the Endocrine Society’s annual meeting in Chicago.

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