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效应性 CD8 T 细胞的内在 IL-2 产生影响 IL-2 信号转导,并促进命运决定、干性和保护。

Intrinsic IL-2 production by effector CD8 T cells affects IL-2 signaling and promotes fate decisions, stemness, and protection.

机构信息

Department of Microbiology, University of Alabama at Birmingham, Birmingham, AL 35294, USA.

Department of Genetics, University of Alabama at Birmingham, Birmingham, AL 35294, USA.

出版信息

Sci Immunol. 2022 Feb 11;7(68):eabl6322. doi: 10.1126/sciimmunol.abl6322.

DOI:10.1126/sciimmunol.abl6322
PMID:35148200
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8923238/
Abstract

Here, we show that the capacity to manufacture IL-2 identifies constituents of the expanded CD8 T cell effector pool that display stem-like features, preferentially survive, rapidly attain memory traits, resist exhaustion, and control chronic viral challenges. The cell-intrinsic synthesis of IL-2 by CD8 T cells attenuates the ability to receive IL-2-dependent STAT5 signals, thereby limiting terminal effector formation, endowing the IL-2-producing effector subset with superior protective powers. In contrast, the non-IL-2-producing effector cells respond to IL-2 signals and gain effector traits at the expense of memory formation. Despite having distinct properties during the effector phase, IL-2-producing and nonproducing CD8 T cells appear to converge transcriptionally as memory matures to form populations with equal recall abilities. Therefore, the potential to produce IL-2 during the effector, but not memory stage, is a consequential feature that dictates the protective capabilities of the response.

摘要

在这里,我们表明制造 IL-2 的能力确定了具有干细胞样特征的扩增 CD8 T 细胞效应池的组成部分,这些细胞优先存活、迅速获得记忆特征、抵抗衰竭并控制慢性病毒挑战。CD8 T 细胞内在合成的 IL-2 减弱了接收 IL-2 依赖性 STAT5 信号的能力,从而限制了终末效应器的形成,使产生 IL-2 的效应子亚群具有更好的保护能力。相比之下,非产生 IL-2 的效应细胞响应 IL-2 信号并获得效应器特征,而牺牲了记忆形成。尽管在效应期具有不同的特性,但产生 IL-2 和不产生 IL-2 的 CD8 T 细胞似乎在记忆成熟时在转录上趋于一致,形成具有同等召回能力的群体。因此,在效应期而不是记忆期产生 IL-2 的潜力是决定反应保护能力的重要特征。

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