TOX reinforces the phenotype and longevity of exhausted T cells in chronic viral infection

淋巴细胞性脉络膜脑膜炎 生物 效应器 细胞毒性T细胞 免疫学 免疫系统 T细胞 表型 抗原 胸腺细胞 免疫疗法 CD8型 基因 遗传学 体外
作者
Francesca Alfei,Kristiyan Kanev,Maike Hofmann,Ming Wu,Hazem E. Ghoneim,Patrick Roelli,Daniel T. Utzschneider,Madlaina von Hoesslin,Jolie G. Cullen,Yiping Fan,Vasyl Eisenberg,Dirk Wohlleber,Katja Steiger,Doron Merkler,Mauro Delorenzi,Percy A. Knolle,Cyrille J. Cohen,Robert Thimme,Ben Youngblood,Dietmar Zehn
出处
期刊:Nature [Nature Portfolio]
卷期号:571 (7764): 265-269 被引量:888
标识
DOI:10.1038/s41586-019-1326-9
摘要

Cytotoxic T cells are essential mediators of protective immunity to viral infection and malignant tumours and are a key target of immunotherapy approaches. However, prolonged exposure to cognate antigens often attenuates the effector capacity of T cells and limits their therapeutic potential1–4. This process, known as T cell exhaustion or dysfunction1, is manifested by epigenetically enforced changes in gene regulation that reduce the expression of cytokines and effector molecules and upregulate the expression of inhibitory receptors such as programmed cell-death 1 (PD-1)5–8. The underlying molecular mechanisms that induce and stabilize the phenotypic and functional features of exhausted T cells remain poorly understood9–12. Here we report that the development and maintenance of populations of exhausted T cells in mice requires the thymocyte selection-associated high mobility group box (TOX) protein13–15. TOX is induced by high antigen stimulation of the T cell receptor and correlates with the presence of an exhausted phenotype during chronic infections with lymphocytic choriomeningitis virus in mice and hepatitis C virus in humans. Removal of its DNA-binding domain reduces the expression of PD-1 at the mRNA and protein level, augments the production of cytokines and results in a more polyfunctional T cell phenotype. T cells with this deletion initially mediate increased effector function and cause more severe immunopathology, but ultimately undergo a massive decline in their quantity, notably among the subset of TCF-1+ self-renewing T cells. Altogether, we show that TOX is a critical factor for the normal progression of T cell dysfunction and the maintenance of exhausted T cells during chronic infection, and provide a link between the suppression of effector function intrinsic to CD8 T cells and protection against immunopathology. TOX is a critical factor for the normal progression of T cell dysfunction and the maintenance of exhausted T cells during chronic infections.
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