Experimental Immunology Branch, National Cancer Institute, Bethesda, Maryland, USA.
Nat Immunol. 2013 Feb;14(2):143-51. doi: 10.1038/ni.2494. Epub 2012 Dec 16.
The maintenance of naive CD8(+) T cells is necessary for lifelong immunocompetence but for unknown reasons requires signaling via both interleukin 7 (IL-7) and the T cell antigen receptor (TCR). We now report that naive CD8(+) T cells required IL-7 signaling to be intermittent, not continuous, because prolonged IL-7 signaling induced naive CD8(+) T cells to proliferate, produce interferon-γ (IFN-γ) and undergo IFN-γ-triggered cell death. Homeostatic engagement of the TCR interrupted IL-7 signaling and thereby supported the survival and quiescence of CD8(+) T cells. However, CD8(+) T cells with insufficient TCR affinity for self ligands received prolonged IL-7 signaling and died during homeostasis. In this study we identified regulation of the duration of IL-7 signaling by homeostatic engagement of the TCR as the basis for in vivo CD8(+) T cell homeostasis.
幼稚 CD8(+) T 细胞的维持对于终生免疫能力是必要的,但原因未知,需要通过白细胞介素 7(IL-7)和 T 细胞抗原受体(TCR)进行信号传递。我们现在报告说,幼稚 CD8(+) T 细胞需要间歇性的 IL-7 信号,而不是连续的信号,因为持续的 IL-7 信号会诱导幼稚 CD8(+) T 细胞增殖、产生干扰素-γ(IFN-γ)并发生 IFN-γ 触发的细胞死亡。TCR 的生理性结合中断了 IL-7 信号,从而支持 CD8(+) T 细胞的存活和静止。然而,对于自身配体 TCR 亲和力不足的 CD8(+) T 细胞会接收到持续的 IL-7 信号,并在体内稳态过程中死亡。在这项研究中,我们确定了 TCR 的生理性结合对 IL-7 信号持续时间的调节是体内 CD8(+) T 细胞稳态的基础。
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