胸腺细胞因子的信号传导,而不是 T 细胞抗原受体,决定了 CD8 谱系的选择,并促进了细胞毒性 T 细胞的分化。
Signaling by intrathymic cytokines, not T cell antigen receptors, specifies CD8 lineage choice and promotes the differentiation of cytotoxic-lineage T cells.
机构信息
Experimental Immunology Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, USA.
出版信息
Nat Immunol. 2010 Mar;11(3):257-64. doi: 10.1038/ni.1840. Epub 2010 Jan 31.
Abstract
Immature CD4(+)CD8(+) (double-positive (DP)) thymocytes are signaled via T cell antigen receptors (TCRs) to undergo positive selection and become responsive to intrathymic cytokines such as interleukin 7 (IL-7). We report here that cytokine signaling is required for positively selected thymocytes to express the transcription factor Runx3, specify CD8 lineage choice and differentiate into cytotoxic-lineage T cells. In DP thymocytes genetically engineered to be cytokine responsive, IL-7 signaling induced TCR-unsignaled DP thymocytes to express Runx3 and to differentiate into mature CD8(+) T cells, completely circumventing positive selection. We conclude that TCR-mediated positive selection converts DP cells into cytokine-responsive thymocytes, but it is subsequent signaling by intrathymic cytokines that specifies CD8 lineage choice and promotes differentiation into cytotoxic-lineage T cells.
摘要
未成熟的 CD4(+)CD8(+)(双阳性 (DP)) 胸腺细胞通过 T 细胞抗原受体 (TCRs) 发出信号,经历阳性选择并对胸腺内细胞因子(如白细胞介素 7 (IL-7)) 产生反应。我们在这里报告,细胞因子信号对于阳性选择的胸腺细胞表达转录因子 Runx3、指定 CD8 谱系选择和分化为细胞毒性谱系 T 细胞是必需的。在经过基因工程改造以对细胞因子有反应的 DP 胸腺细胞中,IL-7 信号诱导 TCR 未发出信号的 DP 胸腺细胞表达 Runx3 并分化为成熟的 CD8(+) T 细胞,完全绕过阳性选择。我们的结论是,TCR 介导的阳性选择将 DP 细胞转化为细胞因子反应性胸腺细胞,但随后由胸腺内细胞因子发出的信号指定 CD8 谱系选择并促进分化为细胞毒性谱系 T 细胞。
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