白介素-2 通过激活芳香烃受体调节肿瘤反应性 CD8 T 细胞耗竭。

IL-2 regulates tumor-reactive CD8 T cell exhaustion by activating the aryl hydrocarbon receptor.

机构信息

Department of Immunology & National Key Laboratory of Medical Molecular Biology, Institute of Basic Medical Sciences, Chinese Academy of Medical Sciences (CAMS) & Peking Union Medical College, Beijing, China.

Clinical Immunology Center, CAMS, Beijing, China.

出版信息

Nat Immunol. 2021 Mar;22(3):358-369. doi: 10.1038/s41590-020-00850-9. Epub 2021 Jan 11.

DOI:10.1038/s41590-020-00850-9

PMID:33432230

Abstract

CD8 T cell exhaustion dampens antitumor immunity. Although several transcription factors have been identified that regulate T cell exhaustion, the molecular mechanisms by which CD8 T cells are triggered to enter an exhausted state remain unclear. Here, we show that interleukin-2 (IL-2) acts as an environmental cue to induce CD8 T cell exhaustion within tumor microenvironments. We find that a continuously high level of IL-2 leads to the persistent activation of STAT5 in CD8 T cells, which in turn induces strong expression of tryptophan hydroxylase 1, thus catalyzing the conversion to tryptophan to 5-hydroxytryptophan (5-HTP). 5-HTP subsequently activates AhR nuclear translocation, causing a coordinated upregulation of inhibitory receptors and downregulation of cytokine and effector-molecule production, thereby rendering T cells dysfunctional in the tumor microenvironment. This molecular pathway is not only present in mouse tumor models but is also observed in people with cancer, identifying IL-2 as a novel inducer of T cell exhaustion.

摘要

CD8 T 细胞耗竭抑制抗肿瘤免疫。尽管已经确定了几种调节 T 细胞耗竭的转录因子，但 CD8 T 细胞进入耗竭状态的分子机制仍不清楚。在这里，我们表明白细胞介素-2 (IL-2) 作为一种环境线索，在肿瘤微环境中诱导 CD8 T 细胞耗竭。我们发现，持续高水平的 IL-2 导致 CD8 T 细胞中 STAT5 的持续激活，进而诱导色氨酸羟化酶 1 的强烈表达，从而催化色氨酸转化为 5-羟色氨酸 (5-HTP)。5-HTP 随后激活 AhR 核易位，导致抑制性受体的协调上调和细胞因子和效应分子产生的下调，从而使 T 细胞在肿瘤微环境中功能失调。这条分子途径不仅存在于小鼠肿瘤模型中，也存在于癌症患者中，将 IL-2 鉴定为 T 细胞耗竭的一种新诱导剂。

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白介素-2 通过激活芳香烃受体调节肿瘤反应性 CD8 T 细胞耗竭。

IL-2 regulates tumor-reactive CD8 T cell exhaustion by activating the aryl hydrocarbon receptor.

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