CD9 Counteracts Liver Steatosis and Mediates GCGR Agonist Hepatic Effects

Yi Zheng; Yuren Wang; Xin Xiong; Linlin Zhang; Jiaran Zhu; Bangliang Huang; Xiufei Liu; Jinbo Liu; Zhiming Zhu; Gangyi Yang; Hua Qu; Hongting Zheng

doi:10.1002/advs.202400819

Advanced Science (Aug 2024)

CD9 Counteracts Liver Steatosis and Mediates GCGR Agonist Hepatic Effects

Yi Zheng,
Yuren Wang,
Xin Xiong,
Linlin Zhang,
Jiaran Zhu,
Bangliang Huang,
Xiufei Liu,
Jinbo Liu,
Zhiming Zhu,
Gangyi Yang,
Hua Qu,
Hongting Zheng

Affiliations

Yi Zheng: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Yuren Wang: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Xin Xiong: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Linlin Zhang: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Jiaran Zhu: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Bangliang Huang: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Xiufei Liu: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Jinbo Liu: Department of Endocrinology Qilu Hospital of Shandong University Jinan 250012 China
Zhiming Zhu: Department of Hypertension and Endocrinology the Third Affiliated Hospital of Army Medical University Chongqing 400042 China
Gangyi Yang: Department of Endocrinology the Second Affiliated Hospital of Chongqing Medical University Chongqing 400010 China
Hua Qu: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China
Hongting Zheng: Department of Endocrinology Translational Research of Diabetes Key Laboratory of Chongqing Education Commission of China the Second Affiliated Hospital of Army Medical University Chongqing 400037 China

DOI: https://doi.org/10.1002/advs.202400819
Journal volume & issue: Vol. 11, no. 29
pp. n/a – n/a

Abstract

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Abstract Glucagon receptor (GCGR) agonism offers potentially greater effects on the mitigation of hepatic steatosis. However, its underlying mechanism is not fully understood. Here, it screened tetraspanin CD9 might medicate hepatic effects of GCGR agonist. CD9 is decreased in the fatty livers of patients and upregulated upon GCGR activation. Deficiency of CD9 in the liver exacerbated diet‐induced hepatic steatosis via complement factor D (CFD) regulated fatty acid metabolism. Specifically, CD9 modulated hepatic fatty acid synthesis and oxidation genes through regulating CFD expression via the ubiquitination‐proteasomal degradation of FLI1. In addition, CD9 influenced body weight by modulating lipogenesis and thermogenesis of adipose tissue through CFD. Moreover, CD9 reinforcement in the liver alleviated hepatic steatosis, and blockage of CD9 abolished the remission of hepatic steatosis induced by cotadutide treatment. Thus, CD9 medicates the hepatic beneficial effects of GCGR signaling, and may server as a promising therapeutic target for hepatic steatosis.

Published in Advanced Science

ISSN: 2198-3844 (Online)
Publisher: Wiley
Country of publisher: Germany
LCC subjects: Science
Website: https://onlinelibrary.wiley.com/journal/21983844

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