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效应性 CD8 T 细胞亚群在慢性感染中的起源和精细化调整。

Origin and fine-tuning of effector CD8 T cell subpopulations in chronic infection.

机构信息

Division of Animal Physiology and Immunology, School of Life Sciences Weihenstephan, Technical University of Munich, 85354 Freising, Germany.

出版信息

Curr Opin Virol. 2021 Feb;46:27-35. doi: 10.1016/j.coviro.2020.10.003. Epub 2020 Nov 1.

Abstract

Persisting stimulation can skew CD8 T cells towards a hypofunctional state commonly referred to as T cell exhaustion. This functional attenuation likely constitutes a mechanism which evolved to balance T cell mediated viral control versus overwhelming immunopathology. Here, we highlight the recent progress in defining the genetic mechanisms and factors shaping the differentiation of exhausted CD8 T cells. We review how the transcription factor Tox imposes an exhausted phenotype in the Tcf1+ progenitors and how CD4 help fine-tunes the effector subsets that emerge from this progenitor population. Both processes critically shape the spectrum of effector function performed by CD8 T cells and the level of resulting virus control. Finally, we discuss how these insights can be exploited to boost the immune response in chronic infection and cancer.

摘要

持续的刺激会使 CD8 T 细胞向一种功能低下的状态倾斜,这种状态通常被称为 T 细胞耗竭。这种功能衰减可能是一种机制,它的进化是为了平衡 T 细胞介导的病毒控制与免疫病理的压倒性影响。在这里,我们强调了定义遗传机制和影响耗竭 CD8 T 细胞分化的因素的最新进展。我们回顾了转录因子 Tox 如何在 Tcf1+祖细胞中施加耗竭表型,以及 CD4 如何精细调节从该祖细胞群中出现的效应子亚群。这两个过程都严重影响了 CD8 T 细胞执行的效应功能谱和由此产生的病毒控制水平。最后,我们讨论了如何利用这些见解来增强慢性感染和癌症中的免疫反应。

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