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Melatonin alleviates alcoholic liver disease via EGFR–BRG1–TERT axis regulation

  • Zhaodi Che
  • , Yali Song
  • , Chengfang Xu
  • , Wei Li
  • , Zhiyong Dong
  • , Cunchuan Wang
  • , Yixing Ren
  • , Kwok Fai So
  • , George L. Tipoe
  • , Fei Wang
  • , Jia Xiao
  • First Affiliated Hospital of Jinan University
  • Sun Yat-Sen University
  • Toho University
  • North Sichuan Medical College
  • Jinan University
  • The University of Hong Kong
  • Seventh Affiliated Hospital of Sun Yat-sen University

科研成果: 期刊稿件文章同行评审

19 引用 (Scopus)

摘要

Chronic alcohol consumption causes liver steatosis, cell death, and inflammation. Melatonin (MLT) is reported to alleviate alcoholic liver disease (ALD)-induced injury. However, its direct regulating targets in hepatocytes are not fully understood. In the current study, a cell-based screening model and a chronic ethanol-fed mice ALD model were used to test the protective mechanisms of MLT. MLT ameliorated ethanol-induced hepatocyte injury in both cell and animal models (optimal doses of 10 μmol/L and 5 mg/kg, respectively), including lowered liver steatosis, cell death, and inflammation. RNA-seq analysis and loss-of-function studies in AML-12 cells revealed that telomerase reverse transcriptase (TERT) was a key downstream effector of MLT. Biophysical assay found that epidermal growth factor receptor (EGFR) on the hepatocyte surface was a direct binding and regulating target of MLT. Liver specific knock-down of Tert or Egfr in the ALD mice model impaired MLT-mediated liver protection, partly through the regulation of nuclear brahma-related gene-1 (BRG1). Long-term administration (90 days) of MLT in healthy mice did not cause evident adverse effect. In conclusion, MLT is an efficacious and safe agent for ALD alleviation. Its direct regulating target in hepatocytes is EGFR and downstream BRG1–TERT axis. MLT might be used as a complimentary agent for alcoholics.

源语言英语
页(从-至)100-112
页数13
期刊Acta Pharmaceutica Sinica B
13
1
DOI
出版状态已出版 - 1月 2023
已对外发布

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