草莓污视频导航

Nov. 9, 2022

草莓污视频导航 study points to potential new treatment for inflammatory bowel diseases

Research led by Simon Hirota details natural repair process in the human gut
Simon Hirota, Joshua Lee and Am茅line Delanne
From left: Simon Hirota, PhD, Joshua Lee, MSc candidate, and Am茅line Delanne, PhD. Snyder Institute for Chronic Diseases

People with inflammatory bowel diseases develop inflammation of the intestine that can cause thickening of the gut wall and life-threatening blockage of the intestinal tube. Twenty to 50 per cent of people with Crohn鈥檚 disease and ulcerative colitis are affected over their lifetime by this poorly understood condition, called 鈥渇ibrosis.鈥

鈥淐urrently there are no approved treatments for this condition, beyond surgery, to remove the blocked section of intestine,鈥 says Dr. Simon Hirota, PhD, Canada Research Chair in Host-Microbe Interactions and Chronic Disease, and member of the at the 草莓污视频导航鈥檚 .

A new led by Hirota and published in the journal Cellular and Molecular Gastroenterology and Hepatology, opens the door to developing a potential treatment for fibrosis. The study involved researchers at the 草莓污视频导航 and the Albert Einstein College of Medicine in New York.

The research teams investigated bacteria residing in the human gut 鈥 鈥渢he inner tube of life鈥 鈥 that release chemical substances called microbial metabolites (products of metabolism) that block inflammation and gut wall thickening. In people with inflammatory bowel diseases, these metabolites are present at reduced levels, as are the natural sensors that the body uses to detect them.

Hirota explains that while repair in the gut is necessary after injury, the 鈥渙ver-exuberant鈥 constant repair seen with inflammatory bowel diseases leads to disease-causing changes in the gut wall.

鈥淲e鈥檙e now starting to think about not only the lining of the gut playing a role in sensing and responding to metabolites, but also the fibroblast cells just below the lining,鈥 Hirota says.

Chemical interplay in the gut controls repair process

The researchers looked at a specific chemical receptor 鈥 or sensor 鈥 in the gut called PXR that鈥檚 involved in helping the gut heal. They focused on the interplay between this receptor and a metabolite called IPA.

Using cells from mice the researchers removed the PXR receptor, enabling them to determine which cells were involved in the interplay between the chemicals released by gut bacteria and the host. They used cells from the human gut to verify their findings in the animal model.

The findings suggest that drugs designed to target these sensors may provide a new treatment to prevent inflammation-associated gut blockage. Co-author Dr. Sridhar Mani, MD, and his research group have produced synthetic compounds based on the structure of the IPA metabolite that have been shown to inhibit inflammation 鈥 much like the natural IPA does.

鈥淭his new research has produced a field-driving publication that clearly implicates PXR as an important target for fibrosis,鈥 says Mani, professor at the . 鈥淲e hope to now use microbial metabolite mimicry as a strategy to target PXR to prevent this dreaded complication of IBD.鈥

Public databases proved invaluable

A key component in the research involved examining and re-analyzing publicly available datasets that include data on characteristics of people with inflammatory bowel diseases, genetics, and gut microbiota composition. This effort was led by Dr. Kyle Flannigan, PhD, lead author on the journal paper and Hirota鈥檚 senior postdoctoral researcher, and Dr. Hena Ramy, PhD, lead data scientist at 草莓污视频导航鈥檚 .

Flannigan and Ramy mined the data looking for associations between the IPA metabolite being investigated and some of the genes associated with the fibrosis process. 鈥淲e were able to see a signal in the human population using these datasets that suggested what we were seeing in our animal model might be playing out in human patients with IBDs,鈥 Hirota says. 

A next step would be to conduct clinical trials to see if the synthetic compounds have a beneficial effect on fibrosis and the remodelling process in the human gut. Hirota says that ideally, the 鈥渟ynthetic metabolite鈥 would be in a form that could be ingested and would pass through the stomach and be released in specific areas of the gut that are affected.

This research was supported by Crohn鈥檚 and Colitis Canada, the , and the Dr. Lloyd Sutherland Chair in IBD/GI (gastrointestinal) Research held by Hirota.

 is an associate professor the and Microbiology, Immunology & Infectious Diseases at the Cumming School of Medicine (CSM). He is a member of the  and the  at the CSM.

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