Regulatory mucosa-associated invariant T cells controlled by β1 adrenergic receptor signaling contribute to hepatocellular carcinoma progression

CXCR3型 肝细胞癌 FOXP3型 流式细胞术 癌症研究 生物 免疫系统 肿瘤进展 免疫学 趋化因子受体 癌症 趋化因子 遗传学
作者
Sicheng Fu,Muziying Liu,Chenwen Zhu,Huimin Zhang,Chao Zhao,Yaping Xie,Guanghou Chen,Daping Sheng,Jun Pan,Ziqing He,Ying Dai,Yufeng Gao,Xiaomei Li,Lijian Chen,Yeben Qian,Tengchuan Jin,Cheng Sun,Zhigang Tian,Hua Wang,Li Bai
出处
期刊:Hepatology [Wiley]
卷期号:78 (1): 72-87 被引量:5
标识
DOI:10.1097/hep.0000000000000014
摘要

The innate-like mucosa-associated invariant T (MAIT) cells are enriched in human liver and have been linked to human HCC. However, their contributions to the progression of HCC are controversial due to the heterogeneity of MAIT cells, and new MAIT cell subsets remain to be explored.Combining single cell RNA sequencing (scRNA-seq) and flow cytometry analysis, we performed phenotypic and functional studies and found that FOXP3 + CXCR3 + MAIT cells in HCC patients were regulatory MAIT cells (MAITregs) with high immunosuppressive potential. These MAITregs were induced under Treg-inducing condition and predominantly from FOXP3 - CXCR3 + MAIT cells, which displayed mild Treg-related features and represented a pre-MAITreg reservoir. In addition, the induction and function of MAITregs were promoted by β1 adrenergic receptor signaling in pre-MAITregs and MAITregs, respectively. In HCC patients, high proportion of the intratumoral MAITregs inhibited antitumor immune responses and was associated with poor clinical outcomes.Together, we reveal an immunosuppressive subset of MAIT cells in HCC patients that contributes to HCC progression, and propose a control through neuroimmune crosstalk.
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