Cell Death and Disease (Apr 2022)

IL-1β-activated mTORC2 promotes accumulation of IFN-γ+ γδ T cells by upregulating CXCR3 to restrict hepatic fibrosis

  • Qihui Liu,
  • Quanli Yang,
  • Zengfeng Wu,
  • Yanfang Chen,
  • Miaomiao Xu,
  • Hua Zhang,
  • Jiliang Zhao,
  • Zonghua Liu,
  • Zerong Guan,
  • Jing Luo,
  • Zhi-yong Li,
  • Guodong Sun,
  • Qiong Wen,
  • Yan Xu,
  • Zhenhua Li,
  • Kebing Chen,
  • Xiaosong Ben,
  • Wanchun He,
  • Xueshi Li,
  • Zhinan Yin,
  • Jianlei Hao,
  • Ligong Lu

DOI
https://doi.org/10.1038/s41419-022-04739-3
Journal volume & issue
Vol. 13, no. 4
pp. 1 – 12

Abstract

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Abstract Liver fibrosis represents a severe stage of liver damage, with hallmarks of inflammation, hepatic stellate cell activation, and extracellular matrix accumulation. Although previous studies demonstrated γδ T cells are involved in liver fibrosis, the precise role and mechanisms of γδ T cells migrating to fibrotic liver have not been elucidated. Here, we aim to investigate the functional subsets of γδ T cells in hepatic fibrosis and to further explore the underlying causes and drivers of migration. In this study, we observed that γδ T cells accumulate in fibrotic liver. Adoptive transfer of γδ T, especially Vγ4 γδ T subset, can significantly alleviate liver fibrosis. In addition, CCl4 treatment also leads to activation of mTOR signaling in γδ T cells. Genetic deletion of the Rictor gene, but not Raptor, in γδ T cells markedly exacerbated liver fibrosis. Mechanistically, CCl4-induced liver injury causes macrophage accumulation in the liver, and IL-1β produced by macrophages promotes mTORC2 signaling activation in γδ T cells, which upregulates T-bet expression and eventually promotes CXCR3 transcription to drive γδ T cell migration. Moreover, hepatic γδ T cells ameliorated liver fibrosis by cytotoxicity against activated hepatic stellate cells in FasL-dependent manner, and secrete IFN-γ to inhibit the differentiation of pro-fibrotic Th17 cells. Thus, IL-1β-activated mTORC2 signaling in γδ T cells upregulates CXCR3 expression, which is critical for IFN-γ+ γδ T cells migration into the liver and amelioration of liver fibrosis. Our findings indicate that targeting the mTORC2 or CXCR3 in γδ T cells could be considered as a promising approach for γδ T cell immunotherapy against liver fibrosis.