Zhu Chen, Dixon Karen O, Newcomer Kathleen, Gu Guangxiang, Xiao Sheng, Zaghouani Sarah, Schramm Markus A, Wang Chao, Zhang Huiyuan, Goto Kouichiro, Christian Elena, Rangachari Manu, Rosenblatt-Rosen Orit, Okada Hitoshi, Mak Tak, Singer Meromit, Regev Aviv, Kuchroo Vijay
Evergrande Center for Immunologic Diseases and Ann Romney Center for Neurologic Diseases, Harvard Medical School and Brigham and Women's Hospital, Boston, MA 02115, USA.
Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA.
Sci Adv. 2021 Apr 30;7(18). doi: 10.1126/sciadv.abd2710. Print 2021 Apr.
T cell exhaustion has been associated with poor prognosis in persistent viral infection and cancer. Conversely, in the context of autoimmunity, T cell exhaustion has been favorably correlated with long-term clinical outcome. Understanding the development of exhaustion in autoimmune settings may provide underlying principles that can be exploited to quell autoreactive T cells. Here, we demonstrate that the adaptor molecule Bat3 acts as a molecular checkpoint of T cell exhaustion, with deficiency of Bat3 promoting a profound exhaustion phenotype, suppressing autoreactive T cell-mediated neuroinflammation. Mechanistically, Bat3 acts as a critical mTORC2 inhibitor to suppress Akt function. As a result, Bat3 deficiency leads to increased Akt activity and FoxO1 phosphorylation, indirectly promoting expression. Transcriptional analysis of T cells revealed up-regulation of dysfunction-associated genes, concomitant with down-regulation of genes associated with T cell effector function, suggesting that absence of Bat3 can trigger T cell dysfunction even under highly proinflammatory autoimmune conditions.
T细胞耗竭与持续性病毒感染和癌症的不良预后相关。相反,在自身免疫的背景下,T细胞耗竭与长期临床结果呈正相关。了解自身免疫环境中耗竭的发展可能会提供一些潜在的原理,可用于抑制自身反应性T细胞。在这里,我们证明衔接分子Bat3作为T细胞耗竭的分子检查点,Bat3的缺乏促进了深刻的耗竭表型,抑制了自身反应性T细胞介导的神经炎症。从机制上讲,Bat3作为一种关键的mTORC2抑制剂来抑制Akt功能。因此,Bat3缺乏导致Akt活性增加和FoxO1磷酸化,间接促进 表达。对 T细胞进行转录分析发现,功能障碍相关基因上调,同时与T细胞效应功能相关的基因下调,这表明即使在高度促炎的自身免疫条件下,Bat3的缺失也会引发T细胞功能障碍。
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