Discovery could pave the way for developing therapies to treat nonalcoholic steatohepatitis Skip to content Menu Medical Home Life Sciences Home Become a Member Search Medical Home Life Sciences Home About Functional Food News Health A-Z Drugs Medical Devices Interviews White Papers More... 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The finding, published in Immunity , could pave the way for developing therapies to treat nonalcoholic steatohepatitis (NASH). The team led by Zhenyu Zhong, Ph.D., and Shuang Liang, Ph.D., Assistant Professors of Immunology, revealed that persistent obesity can damage a macrophage receptor, called TREM2, thereby disabling a critical function that otherwise keeps liver inflammation in check. The imbalance then fuels chronic liver inflammation to enable NASH development. NASH is an aggressive form of nonalcoholic fatty liver disease (NAFLD) – a spectrum of chronic liver disorders that start out as benign fatty liver but can progress into more advanced disease stages including NASH, cirrhosis and even hepatocellular carcinoma (HCC), the dominant form of primary liver cancer. The underlying molecular mechanisms that cause fatty liver disease to progress to NASH and beyond have eluded researchers, creating significant hurdles to developing effective therapies. Bridging this knowledge gap, Drs. Zhong and Liang discovered that dietary obesity upregulates TREM2 expression in the liver-infiltrating macrophages – a critical population of immune cells responsible for removing lipid-damaged hepatocytes. "The clearance of these damaged cells by macrophages (a process also referred to as efferocytosis) is key to maintaining liver immune silence in the fatty liver to prevent chronic inflammation and NASH," Dr. Liang said. Upon examination of TREM2 expression during NASH development, the researchers unexpectedly found that persistent obesity significantly impaired macrophage-dependent removal of lipid-damaged hepatocytes by inducing TREM2 cleavage and inactivation. We discovered that two proinflammatory cytokines, TNF and IL-1β, activate a proteinase named ADAM17 in macrophages that in turn cleaves and inactivates TREM2. This leads to aberrant accumulation of lipid-loaded, dying hepatocytes in the liver where they cause chronic liver inflammation and subsequent NASH development. We reason that blocking TREM2 cleavage to restore the macrophage's ability to remove lipid-damaged hepatocytes has the great potential to treat NASH." Dr. Zhenyu Zhong, Ph.D., Member of the Harold C. Simmons Comprehensive Cancer Center and Cancer Prevention and Research Institute of Texas Scholar in Cancer Research at UT Southwestern Additionally, they discovered that the cleaved product, the soluble TREM2 (sTREM2), whose abundance is drastically elevated in the circulation of NASH-bearing mice and patients, can serve as a noninvasive biomarker for NASH. The Zhong Lab is focused on understanding the fundamental molecular mechanisms by which chronic liver inflammation is established. "With the unprecedented obesity epidemic, NASH has become a major chronic liver disorder, affecting approximately 3%-5% of the global population," said Dr. Zhong, a member of the Division of Basic Science of UT Southwestern's Graduate School of Biomedical Sciences. "By deploying a combination of biochemical, genetic, molecular, immunological, imaging, and histochemical tools as well as single-cell 'omics' analyses, our ultimate goal is to reveal the fundamental molecular mechanisms underlying chronic liver inflammation and explore if such novel mechanistic insights could be applied to benefit liver repair and regeneration after injury, thereby preventing NAFLD progression into NASH and HCC." Related Stories Liver-derived protein supports bone health in males Cornell study finds existing drug could boost liver cancer immunotherapy Obesity drives one in ten infectious disease deaths Other UTSW researchers who contributed to the study are Xiaochen Wang, Chuanli Zhou, Danhui Liu, Naoto Fujiwara, Naoto Kubota, Arielle Click, Polly Henderson, Janiece Vancil, Cesia Ammi Marquez, and Yujin Hoshida. This study was supported by grants from the American Association for the Study of Liver Diseases, the Cancer Prevention and Research Institute of Texas, and the National Institutes of Health. Additional support included computational support from the BioHPC supercomputing facility in the Lyda Hill Department of Bioinformatics at UT Southwestern, the UTSW Flow Cytometry Core facility, and UTSW Circle of Friends Award in Cancer Research, among others. Source: UT Southwestern Medical Center Journal reference: Wang, X., et al. (2022) Prolonged hypernutrition impairs TREM2-dependent efferocytosis to license chronic liver inflammation and NASH development. Immunity. doi.org/10.1016/j.immuni.2022.11.013 . Posted in: Medical Science News | Medical Research News | Medical Condition News Comments (0) Download PDF Copy Suggested Reading Researchers develop new score to predict the risk of liver cancer Obesity drives shared genetic risk behind many chronic disease combinations Research shows the effect of losing weight in preventing multiple diseases Study explores whether a bidirectional causal link exists between MASLD and sarcopenia SynGenSys introduces Liver.SET synthetic promoter library for liver-specific gene expression for in vivo gene therapies Do cocoa flavanols influence heart and fatty liver risk factors? 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Simmons Comprehensive Cancer Center and Cancer Prevention and Research Institute of Texas Scholar in Cancer Research at UT Southwestern Additionally, they discovered that the cleaved product, the soluble TREM2 (sTREM2), whose abundance is drastically elevated in the circulation of NASH-bearing mice and patients, can se

…emove lipid-damaged hepatocytes has the great potential to treat NASH." Dr. Zhenyu Zhong, Ph.D., Member of the Harold C. Simmons Comprehensive Cancer Center and Cancer Prevention and Research Institute of Texas Scholar in Cancer Research at UT Southwestern Additionally, they discovered that the cleaved product, the soluble TREM2 (sTREM2), whose abundance is drastically elevated in the circulation of NASH-bearing mice and patients, can s erve as a noninvasive biomarker for NASH. The Zhong Lab is focused on understanding the fundamental molecular mechanisms…

Upon examination of TREM2 expression during NASH development, the researchers unexpectedly found that persistent obesity significantly impaired macrophage-dependent removal of lipid-damaged hepatocytes by inducing TREM2 cleavage and inactivation.

…is key to maintaining liver immune silence in the fatty liver to prevent chronic inflammation and NASH," Dr. Liang said. Upon examination of TREM2 expression during NASH development, the researchers unexpectedly found that persistent obesity significantly impaired macrophage-dependent removal of lipid-damaged hepatocytes by inducing TREM2 cleavage and inactivation . We discovered that two proinflammatory cytokines, TNF and IL-1β, activate a proteinase named ADAM17 in macrophages tha…

Astaxanthin and Human Health: Evidence on Skin, Vision, Brain, and Aging The Gut–Brain–Skin Axis: How Diet and Gut Health Influence Mood, Skin, and Aging How Morning Routines Influence Cognitive Performance, Mood, and Circadian Rhythm Camel Milk Nutrition Facts and Potential Health Benefits Explained Edible Insects as

… Rosanna Zhang from ACROBiosystems about utilizing organoids for disease modeling in the field of neuroscience research. Astaxanthin and Human Health: Evidence on Skin, Vision, Brain, and Aging The Gut–Brain–Skin Axis: How Diet and Gut Health Influence Mood, Skin, and Aging How Morning Routines Influence Cognitive Performance, Mood, and Circadian Rhythm Camel Milk Nutrition Facts and Potential Health Benefits Explained Edible Insects as Food: Nutritional Benefits, Safety, and Environmental Impact Latest News Researchers discover a way to breach cancer’s …