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    Home»Conditions»Experimental drug reverses severe fatty liver disease by repairing the gut
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    Experimental drug reverses severe fatty liver disease by repairing the gut

    stamilhstgr0518@gmail.comBy stamilhstgr0518@gmail.comJuly 11, 2026No Comments6 Mins Read
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    Experimental drug reverses severe fatty liver disease by repairing the gut
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    Experimental drug reverses severe fatty liver disease by repairing the gut

    A new experimental drug reversed severe fatty liver disease in animals by repairing the gut, raising hopes for a powerful new treatment for MASH

    Date:
    July 11, 2026
    Source:
    Michigan Medicine – University of Michigan
    Summary:
    An experimental drug called DT-109 reversed severe fatty liver disease in animal studies by repairing the gut and preventing harmful toxins from damaging the liver. The discovery could open the door to a new class of treatments for MASH and potentially other diseases tied to gut health.
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    FULL STORY

    An experimental drug developed at Michigan Medicine has shown the ability to reverse severe fatty liver disease in animal studies by restoring gut health. The findings, published in The Journal of Clinical Investigation, suggest that targeting the connection between the gut and liver could offer a promising new approach for treating metabolic dysfunction-associated steatohepatitis (MASH)

    MASH is a serious form of fatty liver disease that affects about 7% of people worldwide. It can progress to cirrhosis, liver cancer, and liver failure, yet effective treatment options remain limited

    The investigational compound, known as DT-109, is a glycine-based tripeptide. Researchers found that it reversed MASH in animal models by interrupting a harmful biological process linking the gut and liver

    “We see clear evidence that DT-109 protects the gut epithelial barrier, reducing the systemic influx of harmful microbial products that are thought to contribute to MASH development and progression,” said Eugene Chen, M.D., Ph.D., senior author of the study and Frederick G. L. Huetwell Professor of Cardiovascular Medicine at the University of Michigan Medical School

    “This compound shows benefits to the gastrointestinal system and has great potential as a treatment for MASH.”

    How Gut Bacteria Can Drive Liver Disease

    Earlier studies from Chen’s laboratory had already shown that DT-109 could improve MASH in animals. The new research explains how the compound produces those benefits

    The team first identified a major contributor to the disease: an overgrowth of the bacterium Clostridium perfringens, which generates ammonia inside the gut

    High ammonia levels damage the lining of the digestive tract, weakening the intestinal barrier. Once that protective barrier is compromised, harmful microbial products can enter the bloodstream, reach the liver, and trigger inflammatory immune responses, including excessive activation of CD8+ T cells

    Through a series of experiments, the researchers found that DT-109 disrupted this chain of events, helping restore the health of both the gut and the liver

    DT-109 Restores the Gut Barrier

    In both mice and nonhuman primates, DT-109 reduced Clostridium perfringens levels and lowered ammonia production in the intestines. As a result, the intestinal barrier became stronger, limiting the movement of harmful substances from the gut into the body

    The results were especially encouraging in nonhuman primates, whose liver biology and gut microbiota more closely resemble those of humans. In these animals, DT-109 reduced liver inflammation and significantly improved the severity of MASH

    “DT-109 connects microbiota modulation with liver protection by restoring gut barrier integrity and limiting the systemic translocation of ammonia and other pro-inflammatory microbial products within the gut-liver axis,” said Jifeng Zhang, Ph.D., co-author and research professor of cardiovascular medicine at U-M Medical School

    “We also found that DT-109 primarily acts in the gastrointestinal tract, but its reach stretches much further.”

    Potential Benefits Beyond MASH

    The researchers believe DT-109 may have uses beyond treating fatty liver disease

    Previous studies have shown that the compound can reduce the formation of atherosclerosis plaques and prevent vascular calcification in nonhuman primates, suggesting it could also become a treatment for cardiovascular disease

    Because breakdown of the intestinal barrier has also been linked to several digestive disorders, the team believes DT-109 could eventually be explored as a treatment for conditions such as inflammatory bowel disease (IBD)

    Future research will focus on additional testing needed to move DT-109 into clinical trials and evaluate its safety and effectiveness in people

    “This study presents novel evidence about the pathogenesis of MASH and provides excitement about a therapeutic avenue to explore for a condition that remains difficult to treat,” said Elliot Tapper, M.D., Academic Director of Hepatology at Michigan Medicine

    “What patients with MASH need is a safe and effective therapy capable of improving their liver and heart health — of course we are excited about these developments.”

    Additional authors include Yang Zhao, Ph.D., Ying Zhao M.S., and Yanhong Guo, MD., Ph.D., all of the University of Michigan. Additional co-authors are listed in the published study

    Ying Zhao, Oren Rom, Jifeng Zhang, and Y. Eugene Chen are inventors on the patent application (Tripeptides and treatment of metabolic, cardiovascular, and inflammatory disorders)

    Chen is also an inventor of DT-109. The University of Michigan has patented the compound and licensed it to Diapin Therapeutics. Chen and the university hold an ownership interest in the company. Diapin Therapeutics supplied DT-109 for the study and is continuing to develop the compound

    The study protocol involving humans, all amendments and the informed consent form were reviewed and approved by the Institutional Review Boards at each site, including the First Affiliated Hospital of Xi’an Jiaotong University (approval number: XJTU1AF2023LSK330), and the Institutional Review Board of Jinan University (approval number: 2016-017) and the University of Hong Kong/Hospital Authority Hong Kong West Cluster (approval number: UW 20-700). All experimental protocols involving non-human primates were approved by the Laboratory Animal Care Committee of Xi’an Jiaotong University (approval number: 20191278) and the Institutional Animal Care and Use Committee of Spring Biological Technology Development Co., Ltd. (approval number: 201901). The study was performed in accordance with the National Institutes of Health Guide for the Care and Use of Laboratory Animals.

    Story Source:

    Materials provided by Michigan Medicine – University of Michigan. Note: Content may be edited for style and length

    Journal Reference:

    1. Pengxiang Qu, Shusi Ding, Yanru Zhang, Yang Zhao, Erfei Song, Liangshuo Hu, Ruike Ding, Wenbin Cao, Yiting Hou, Jia Qi, Juan Zhao, Chenjing Duan, Shuangqing Liu, Chong Shen, Ying Zhao, Yanhong Guo, Zuowen Zheng, Shiwei Luo, Huizhong Hu, Liang Bai, Sihai Zhao, Bo Wang, Shuixiang He, Yi Wu, Xuelian Xiong, Qiutong Wu, Weiwang Gu, Oren Rom, Aimin Xu, Lemin Zheng, Jifeng Zhang, Enqi Liu, Y. Eugene Chen. Metabolic dysfunction–associated steatohepatitis exacerbated by Clostridium perfringens–derived ammonia is attenuated by tripeptide DT-109. Journal of Clinical Investigation, 2026; 136 (13) DOI: 10.1172/JCI200522

    Cite This Page:

    Michigan Medicine – University of Michigan. “Experimental drug reverses severe fatty liver disease by repairing the gut.” ScienceDaily. ScienceDaily, 11 July 2026. <www.sciencedaily.com/releases/2026/07/260711010116.htm>.
    Michigan Medicine – University of Michigan. (2026, July 11). Experimental drug reverses severe fatty liver disease by repairing the gut. ScienceDaily. Retrieved July 11, 2026 from www.sciencedaily.com/releases/2026/07/260711010116.htm
    Michigan Medicine – University of Michigan. “Experimental drug reverses severe fatty liver disease by repairing the gut.” ScienceDaily. www.sciencedaily.com/releases/2026/07/260711010116.htm (accessed July 11, 2026).
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