Virulence (Dec 2022)

Regulation of host factor γ-H2AX level and location by enterovirus A71 for viral replication

  • Jinghua Yu,
  • Wenyan Zhang,
  • Wenbo Huo,
  • Xiangling Meng,
  • Ting Zhong,
  • Ying Su,
  • Yumeng Liu,
  • Jinming Liu,
  • Zengyan Wang,
  • Fengmei Song,
  • Shuxia Zhang,
  • Zhaolong Li,
  • Xiaoyan Yu,
  • Xiaofang Yu,
  • Shucheng Hua

DOI
https://doi.org/10.1080/21505594.2022.2028482
Journal volume & issue
Vol. 13, no. 1
pp. 241 – 257

Abstract

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Numerous viruses manipulate host factors for viral production. We demonstrated that human enterovirus A71 (EVA71), a primary causative agent for hand, foot, and mouth disease (HFMD), increased the level of the DNA damage response (DDR) marker γ-H2AX. DDR is primarily mediated by the ataxia telangiectasia mutated (ATM), ATM and Rad3-related (ATR), or DNA-dependent protein kinase (DNA-PK) pathways. Upregulation of γ-H2AX by EVA71 was dependent on the ATR but not the ATM or DNA-PK pathway. As a nuclear factor, there is no previous evidence of cytoplasmic distribution of γ-H2AX. However, the present findings demonstrated that EVA71 encouraged the localization of γ-H2AX to the cytoplasm. Of note, γ-H2AX formed a complex with structural protein VP3, non-structural protein 3D, and the viral genome. Treatment with an inhibitor or CRISPR/Cas9 technology to decrease or silence the expression of γ-H2AX decreased viral genome replication in host cells; this effect was accompanied by decreased viral protein expression and virions. In animal experiments, caffeine was used to inhibit DDR; the results revealed that caffeine protected neonatal mice from death after infection with EVA71, laying the foundation for new therapeutic applications of caffeine. More importantly, in children with HFMD, γ-H2AX was upregulated in peripheral blood lymphocytes. The consistent in vitro and in vivo data on γ-H2AX from this study suggested that caffeine or other inhibitors of DDR might be novel therapeutic agents for HFMD.

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