白细胞介素-2 受体信号转导是影响调节性 T 细胞亚群分布的检查点

IF 4.6 2区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES iScience Pub Date : 2024-10-24 DOI:10.1016/j.isci.2024.111248

Acacia N. Shouse , Alejandro V. Villarino , Thomas R. Malek

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引用次数: 0

摘要

调节性T细胞（Tregs）需要IL-2才能在外周存活，但IL-2如何塑造Treg的异质性仍未明确。在这里，我们发现抑制胸腺后Tregs的IL-2R信号转导会导致循环Tregs（cTregs）的优先早期损失。与效应Tregs（eTregs）相比，cTregs的基因表达更依赖于IL-2R信号。意想不到的是，消减 cTregs 的 IL-2R 信号会导致 eTregs 的增殖、基因表达和发展成 eTregs 的能力增强。因此，IL-2R 信号通常作为一个检查点维持 cTreg 的平衡，同时限制它们发育成 eTregs。IL-2R 信号的缺失也改变了 eTreg 亚群的分布，IFNγR1+ eTregs 和 CXCR5+ PD-1+ T 滤泡调节（TFR）细胞增多，但肠 RORγt+ TR17 细胞减少。这些变化降低了 eTreg 的抑制功能，支持了分泌 IFNγ 的 T 效应细胞的扩增。因此，IL-2R 信号还能保障 Treg 的功能并许可特化 eTreg 的分化。

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Interleukin-2 receptor signaling acts as a checkpoint that influences the distribution of regulatory T cell subsets

Regulatory T cells (Tregs) require IL-2 for survival in the periphery, yet how IL-2 shapes Treg heterogeneity remains poorly defined. Here we show that inhibition of IL-2R signaling in post-thymic Tregs leads to a preferential early loss of circulating Tregs (cTregs). Gene expression of cTregs was more dependent on IL-2R signaling than effector Tregs (eTregs). Unexpectedly, ablation of IL-2R signaling in cTregs resulted in increased proliferation, expression of eTreg genes, and enhanced capacity to develop into eTregs. Thus, IL-2R signaling normally acts as a checkpoint to maintain cTreg homeostasis while restraining their development into eTregs. Loss of IL-2R signaling also alters the distribution of eTreg subsets, with increased IFNγR1⁺ eTregs and CXCR5⁺ PD-1⁺ T follicular regulatory (T_FR) cells but decreased intestinal RORγt⁺ T_R17 cells. These changes lower eTreg suppressive function supporting expansion of IFNγ-secreting T effector cells. Thus, IL-2R signaling also safeguards Treg function and licenses differentiation of specialized eTregs.

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来源期刊

iScience Multidisciplinary-Multidisciplinary

CiteScore

7.20

自引率

1.70%

发文量

1972

审稿时长

6 weeks

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