Acta Biochimica et Biophysica Sinica (Nov 2022)

USP9x promotes CD8 <sup>+</sup> T-cell dysfunction in association with autophagy inhibition in septic liver injury

  • Sheng Lulu,
  • Chen Juntao,
  • Tong Yiqing,
  • Zhang Yi,
  • Feng Qiming,
  • Tang Zhenghao

DOI
https://doi.org/10.3724/abbs.2022174
Journal volume & issue
Vol. 54
pp. 1765 – 1774

Abstract

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Sepsis is a life-threatening condition manifested by concurrent inflammation and immunosuppression. Ubiquitin-specific peptidase 9, X-linked (USP9x), is a USP domain-containing deubiquitinase which is required in T-cell development. In the present study, we investigate whether USP9x plays a role in hepatic CD8 + T-cell dysfunction in septic mice. We find that CD8 + T cells are decreased in the blood of septic patients with liver injury compared with those without liver injury, the CD4/CD8 ratio is increased, and the levels of cytolytic factors, granzyme B and perforin are downregulated. The number of hepatic CD8 + T cells and USP9x expression are both increased 24 h after cecal ligation and puncture-induced sepsis in a mouse model, a pattern similar to liver injury. The mechanism involves promotion of CD8 + T-cell dysfunction by USP9x associated with suppression of cell cytolytic activity via autophagy inhibition, which is reversed by the USP9x inhibitor WP1130. In the in vivo studies, autophagy is significantly increased in hepatic CD8 + T cells of septic mice with conditional knockout of mammalian target of rapamycin. This study shows that USP9x has the potential to be used as a therapeutic target in septic liver injury.

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