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Membrane-delimited signaling and cytosolic action of MG53 preserve hepatocyte integrity during drug-induced liver injury

肝损伤 肝细胞 肝保护 细胞外 细胞生物学 胞浆 药理学 硫代乙酰胺 生物 生物化学 体外 谷胱甘肽
作者
Yu Han,Sylvester M. Black,Zhengfan Gong,Zhi Chen,Jae‐Kyun Ko,Zhongshu Zhou,Tianyang Xia,Dandong Fang,Donghai Yang,Daqian Gu,Ziyue Zhang,Hongmei Ren,Xudong Duan,Brenda F. Reader,Ping Chen,Yongsheng Li,Jung‐Lye Kim,Zhong‐Guang Li,Xuehong Xu,Li Guo
出处
期刊:Journal of Hepatology [Elsevier BV]
卷期号:76 (3): 558-567 被引量:34
标识
DOI:10.1016/j.jhep.2021.10.017
摘要

Drug-induced liver injury (DILI) remains challenging to treat and is still a leading cause of acute liver failure. MG53 is a muscle-derived tissue-repair protein that circulates in the bloodstream and whose physiological role in protection against DILI has not been examined.Recombinant MG53 protein (rhMG53) was administered exogenously, using mice with deletion of Mg53 or Ripk3. Live-cell imaging, histological, biochemical, and molecular studies were used to investigate the mechanisms that underlie the extracellular and intracellular action of rhMG53 in hepatoprotection.Systemic administration of rhMG53 protein, in mice, can prophylactically and therapeutically treat DILI induced through exposure to acetaminophen, tetracycline, concanavalin A, carbon tetrachloride, or thioacetamide. Circulating MG53 protects hepatocytes from injury through direct interaction with MLKL at the plasma membrane. Extracellular MG53 can enter hepatocytes and act as an E3-ligase to mitigate RIPK3-mediated MLKL phosphorylation and membrane translocation.Our data show that the membrane-delimited signaling and cytosolic dual action of MG53 effectively preserves hepatocyte integrity during DILI. rhMG53 may be a potential treatment option for patients with DILI.Interventions to treat drug-induced liver injury and halt its progression into liver failure are of great value to society. The present study reveals that muscle-liver cross talk, with MG53 as a messenger, serves an important role in liver cell protection. Thus, MG53 is a potential treatment option for patients with drug-induced liver injury.
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