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CD8+ T 细胞记忆的全球转录特征。

Global transcriptional characterization of CD8+ T cell memory.

机构信息

Immunobiology Laboratory, Cancer Research UK, United Kingdom.

Institute of Molecular Immunology, München Rechts der Isar, Technische Universität München, Germany; Institute of Experimental Immunology, Universität Bonn, Germany.

出版信息

Semin Immunol. 2015 Feb;27(1):4-9. doi: 10.1016/j.smim.2015.03.001. Epub 2015 Apr 2.

Abstract

The differentiation of memory CD8T cells after acute infections comprises generation of functionally distinct populations that either have proliferative potential or display cytotoxic effector functions and that either recirculate into lymphoid tissues or remain tissue-resident. The development of these functionally distinct cell populations is dictated by defined signals from the microenvironment that result in a coordinated expression of a network of transcription factors, which determine the functionality of memory T cells. Distinct transcriptional regulation observed during chronic viral infection that results in generation of T cells that control viral replication in the absence of immunopathology suggests the existence of so far unappreciated functional adaptation of T cell function to the particular need during chronic infections to control infection and avoid immunopathology. Furthermore, the non-canonical generation of CD8T cell memory outside of lymphoid tissues in the liver in the absence of inflammation is correlated with a distinct transcriptional profile and indicates further complexity in the commensurate immune response to infectious pathogens that escape innate immunity. Taken together, distinct profiles of transcriptional regulation are linked to CD8T cells with different functions and provide important mechanistic insight into the continuous functional adaptation of CD8T cells to generate a commensurate immune response to infectious challenges.

摘要

急性感染后记忆 CD8T 细胞的分化包括产生具有增殖潜力或显示细胞毒性效应功能的功能不同的群体,这些群体要么循环进入淋巴组织,要么留在组织中。这些功能不同的细胞群体的发展是由微环境中的特定信号决定的,这些信号导致转录因子网络的协调表达,从而决定记忆 T 细胞的功能。在慢性病毒感染过程中观察到的不同转录调控导致产生能够在没有免疫病理学的情况下控制病毒复制的 T 细胞,这表明 T 细胞功能存在迄今为止尚未被认识到的针对慢性感染中特定需要的功能适应性,以控制感染并避免免疫病理学。此外,在没有炎症的情况下,肝脏等淋巴组织外的非典型 CD8T 细胞记忆的产生与独特的转录谱相关,这表明对逃避先天免疫的传染性病原体的免疫反应更加复杂。总之,不同的转录调控谱与具有不同功能的 CD8T 细胞相关联,为 CD8T 细胞对感染性挑战产生协调免疫反应的持续功能适应性提供了重要的机制见解。

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