Military Medical Research (Apr 2024)

Interferon-α stimulates DExH-box helicase 58 to prevent hepatocyte ferroptosis

  • Kai-Wei Jia,
  • Ren-Qi Yao,
  • Yi-Wen Fan,
  • Ding-Ji Zhang,
  • Ye Zhou,
  • Min-Jun Wang,
  • Li-Yuan Zhang,
  • Yue Dong,
  • Zhi-Xuan Li,
  • Su-Yuan Wang,
  • Mu Wang,
  • Yun-Hui Li,
  • Lu-Xin Zhang,
  • Ting Lei,
  • Liang-Chen Gui,
  • Shan Lu,
  • Ying-Yun Yang,
  • Si-Xian Wang,
  • Yi-Zhi Yu,
  • Yong-Ming Yao,
  • Jin Hou

DOI
https://doi.org/10.1186/s40779-024-00524-9
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 18

Abstract

Read online

Abstract Background Liver ischemia/reperfusion (I/R) injury is usually caused by hepatic inflow occlusion during liver surgery, and is frequently observed during war wounds and trauma. Hepatocyte ferroptosis plays a critical role in liver I/R injury, however, it remains unclear whether this process is controlled or regulated by members of the DEAD/DExH-box helicase (DDX/DHX) family. Methods The expression of DDX/DHX family members during liver I/R injury was screened using transcriptome analysis. Hepatocyte-specific Dhx58 knockout mice were constructed, and a partial liver I/R operation was performed. Single-cell RNA sequencing (scRNA-seq) in the liver post I/R suggested enhanced ferroptosis by Dhx58 hep−/− . The mRNAs and proteins associated with DExH-box helicase 58 (DHX58) were screened using RNA immunoprecipitation-sequencing (RIP-seq) and IP-mass spectrometry (IP-MS). Results Excessive production of reactive oxygen species (ROS) decreased the expression of the IFN-stimulated gene Dhx58 in hepatocytes and promoted hepatic ferroptosis, while treatment using IFN-α increased DHX58 expression and prevented ferroptosis during liver I/R injury. Mechanistically, DHX58 with RNA-binding activity constitutively associates with the mRNA of glutathione peroxidase 4 (GPX4), a central ferroptosis suppressor, and recruits the m6A reader YT521-B homology domain containing 2 (YTHDC2) to promote the translation of Gpx4 mRNA in an m6A-dependent manner, thus enhancing GPX4 protein levels and preventing hepatic ferroptosis. Conclusions This study provides mechanistic evidence that IFN-α stimulates DHX58 to promote the translation of m6A-modified Gpx4 mRNA, suggesting the potential clinical application of IFN-α in the prevention of hepatic ferroptosis during liver I/R injury.

Keywords