Hepatocyte-specific Mas activation enhances lipophagy and fatty acid oxidation to protect against acetaminophen-induced hepatotoxicity in mice

Shuai Chen; Zhi Lu; Haoyu Jia; Bo Yang; Chun Liu; Yuxin Yang; Shuo Zhang; Zhijing Wang; Liu Yang; Shanshan Li; Jing Li; Changqing Yang

doi:10.1016/j.jhep.2022.10.028

Hepatocyte-specific Mas activation enhances lipophagy and fatty acid oxidation to protect against acetaminophen-induced hepatotoxicity in mice

J Hepatol. 2023 Mar;78(3):543-557. doi: 10.1016/j.jhep.2022.10.028. Epub 2022 Nov 9.

Authors

Shuai Chen¹, Zhi Lu², Haoyu Jia¹, Bo Yang¹, Chun Liu¹, Yuxin Yang³, Shuo Zhang¹, Zhijing Wang¹, Liu Yang¹, Shanshan Li¹, Jing Li⁴, Changqing Yang⁵

Affiliations

¹ Department of Gastroenterology and Hepatology, Tongji Hospital, School of Medicine, Tongji University, Shanghai 200092, China.
² Department of Automation, Tsinghua University, Beijing 100084, China; Institute for Brain and Cognitive Sciences, Tsinghua University, Beijing 100084, China.
³ Department of Automation, Tsinghua University, Beijing 100084, China.
⁴ Department of Gastroenterology and Hepatology, Tongji Hospital, School of Medicine, Tongji University, Shanghai 200092, China. Electronic address: lijingshengping@163.com.
⁵ Department of Gastroenterology and Hepatology, Tongji Hospital, School of Medicine, Tongji University, Shanghai 200092, China. Electronic address: cqyang@tongji.edu.cn.

PMID: 36368597
DOI: 10.1016/j.jhep.2022.10.028

Abstract

Background & aims: Acetaminophen (APAP) is the most common cause of drug-induced liver injury (DILI); however, treatment options are limited. Mas is a G protein-coupled receptor whose role in APAP-induced hepatotoxicity has not yet been examined.

Methods: Intrahepatic Mas expression was determined in both human and mouse DILI models. Mas1^-/-, Alb^creMas1^f/f, Ppara^-/-, Mas1^-/-Ppara^-/- and wild-type mice were challenged with APAP for the in vivo analyses of Mas-AKT-FOXO1 axis-dependent lipophagy and fatty acid oxidation (FAO), using pharmacological compounds and genetic tools. Liver samples were collected for RNA-sequencing, proteomics, metabolomics, lipidomics, and metabolic flux analysis. Live-imaging of liver and histological, biochemical, and molecular studies were performed to evaluate APAP-induced hepatotoxicity in mice. Primary hepatocytes and hepatic cell lines were exposed to APAP for in vitro analysis.

Results: Intrahepatic Mas expression was significantly upregulated in human and mouse DILI models. Mice with systemic, liver-specific, or hepatocyte-specific Mas1 deficiency were vulnerable to APAP-induced hepatotoxicity. They exhibited substantially impaired lipophagy and downstream FAO, which was accompanied by the activation of AKT and suppression of FOXO1. In addition, the prophylactic activation of Mas conferred strong protection against APAP challenge in mice, with remarkably enhanced lipophagy and FAO dependent on the AKT-FOXO1 axis. Moreover, the protective effects of AVE0991 were substantially diminished by the inhibition of either lipophagy or FAO.

Conclusions: The activation of Mas on hepatocytes enhanced AKT-FOXO1-dependent lipophagy and downstream FAO, protecting mice from APAP-induced hepatotoxicity and indicating that hepatocyte-specific Mas might be a novel therapeutic target for DILI.

Impact and implications: Mas signalling arises as a novel therapeutic target for patients with APAP-induced liver injury. The Mas-AKT/FOXO1-fatty acid degradation pathway could be critical for the development of treatment strategies for APAP overdose. When Mas signalling is targeted, the extent of liver injury should be considered at the time of administration. These findings obtained from APAP-challenged mice still need to be confirmed in a clinical context.

Keywords: Mas; acute liver failure; fatty acid degradation; sterile inflammation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Acetaminophen* / metabolism
Animals
Chemical and Drug Induced Liver Injury* / metabolism
Disease Models, Animal
Fatty Acids / metabolism
Hepatocytes / metabolism
Humans
Liver / pathology
Mice
Mice, Inbred C57BL
Proto-Oncogene Proteins c-akt / metabolism

Substances

Acetaminophen
Proto-Oncogene Proteins c-akt
Fatty Acids