The Selective Peroxisome Proliferator‐Activated Receptor Gamma Modulator CHS‐131 Improves Liver Histopathology and Metabolism in a Mouse Model of Obesity and Nonalcoholic Steatohepatitis

Nikolaos Perakakis; Aditya Joshi; Natia Peradze; Konstantinos Stefanakis; Georgia Li; Michael Feigh; Sanne Skovgard Veidal; Glenn Rosen; Michael Fleming; Christos S. Mantzoros

doi:10.1002/hep4.1558

Hepatology Communications (Sep 2020)

The Selective Peroxisome Proliferator‐Activated Receptor Gamma Modulator CHS‐131 Improves Liver Histopathology and Metabolism in a Mouse Model of Obesity and Nonalcoholic Steatohepatitis

Nikolaos Perakakis,
Aditya Joshi,
Natia Peradze,
Konstantinos Stefanakis,
Georgia Li,
Michael Feigh,
Sanne Skovgard Veidal,
Glenn Rosen,
Michael Fleming,
Christos S. Mantzoros

Affiliations

Nikolaos Perakakis: Department of Internal Medicine Boston VA Healthcare System Boston MA
Aditya Joshi: Department of Internal Medicine Boston VA Healthcare System Boston MA
Natia Peradze: Department of Internal Medicine Boston VA Healthcare System Boston MA
Konstantinos Stefanakis: Department of Internal Medicine Boston VA Healthcare System Boston MA
Georgia Li: Coherus Biosciences San Franscisco CA
Michael Feigh: Gubra Hørsholm Denmark
Sanne Skovgard Veidal: Gubra Hørsholm Denmark
Glenn Rosen: Coherus Biosciences San Franscisco CA
Michael Fleming: Coherus Biosciences San Franscisco CA
Christos S. Mantzoros: Department of Internal Medicine Boston VA Healthcare System Boston MA

DOI: https://doi.org/10.1002/hep4.1558
Journal volume & issue: Vol. 4, no. 9
pp. 1302 – 1315

Abstract

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CHS‐131 is a selective peroxisome proliferator‐activated receptor gamma modulator with antidiabetic effects and less fluid retention and weight gain compared to thiazolidinediones in phase II clinical trials. We investigated the effects of CHS‐131 on metabolic parameters and liver histopathology in a diet‐induced obese (DIO) and biopsy‐confirmed mouse model of nonalcoholic steatohepatitis (NASH). Male C57BL/6JRj mice were fed the amylin liver NASH diet (40% fat with trans‐fat, 20% fructose, and 2% cholesterol). After 36 weeks, only animals with biopsy‐confirmed steatosis and fibrosis were included and stratified into treatment groups (n = 12‐13) to receive for the next 12 weeks (1) low‐dose CHS‐131 (10 mg/kg), (2) high‐dose CHS‐131 (30 mg/kg), or (3) vehicle. Metabolic parameters, liver pathology, metabolomics/lipidomics, markers of liver function and liver, and subcutaneous and visceral adipose tissue gene expression profiles were assessed. CHS‐131 did not affect body weight, fat mass, lean mass, water mass, or food intake in DIO‐NASH mice with fibrosis. CHS‐131 improved fasting insulin levels and insulin sensitivity as assessed by the intraperitoneal insulin tolerance test. CHS‐131 improved total plasma cholesterol, triglycerides, alanine aminotransferase, and aspartate aminotransferase and increased plasma adiponectin levels. CHS‐131 (high dose) improved liver histology and markers of hepatic fibrosis. DIO‐NASH mice treated with CHS‐131 demonstrated a hepatic shift to diacylglycerols and triacylglycerols with a lower number of carbons, increased expression of genes stimulating fatty acid oxidation and browning, and decreased expression of genes promoting fatty acid synthesis, triglyceride synthesis, and inflammation in adipose tissue. Conclusion: CHS‐131 improves liver histology in a DIO and biopsy‐confirmed mouse model of NASH by altering the hepatic lipidome, reducing insulin resistance, and improving lipid metabolism and inflammation in adipose tissue.

Published in Hepatology Communications

ISSN: 2471-254X (Online)
Publisher: Wolters Kluwer Health/LWW
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the digestive system. Gastroenterology
Website: https://journals.lww.com/hepcomm/pages/default.aspx

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