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Targeted Sos1 deletion reveals its critical role in early T-cell development

机译:靶向的Sos1缺失揭示了其在早期T细胞发育中的关键作用

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摘要

Activation of the small G protein Ras is required for thymocyte differentiation. In thymocytes, Ras is activated by the Ras guanine exchange factors (RasGEFs) Sos1, Sos2, and RasGRP1. We report the development of a floxed allele of sos1 to assess the role of Sos1 during thymocyte development. Sos1 was required for pre–T-cell receptor (pre-TCR)– but not TCR-stimulated developmental signals. Sos1 deletion led to a partial block at the DN-to-DP transition. Sos1-deficient thymocytes showed reduced pre-TCR–stimulated proliferation, differentiation, and ERK phosphorylation. In contrast, TCR-stimulated positive selection, and negative selection under strong stimulatory conditions, remained intact in Sos1-deficient mice. Comparison of RasGEF expression at different developmental stages showed that relative to Sos2 and RasGRP1, Sos1 is most abundant in DN thymocytes, but least abundant in DP thymocytes. These data reveal that Sos1 is uniquely positioned to affect signal transduction early in thymocyte development.
机译:胸腺细胞分化需要激活小G蛋白Ras。在胸腺细胞中,Ras被Ras鸟嘌呤交换因子(RasGEFs)Sos1,Sos2和RasGRP1激活。我们报告了sos1的等位基因的发展,以评估在胸腺细胞发育过程中Sos1的作用。 T细胞前受体(pre-TCR)需要Sos1,但TCR刺激的发育信号则不需要。 Sos1删除导致了从DN到DP转换的部分阻止。 Sos1缺陷型胸腺细胞显示出降低的TCR前刺激的增殖,分化和ERK磷酸化。相比之下,在Sos1缺陷小鼠中,TCR刺激的阳性选择和强刺激条件下的阴性选择仍然完好无损。 RasGEF表达在不同发育阶段的比较表明,相对于Sos2和RasGRP1,Sos1在DN胸腺细胞中含量最高,而在DP胸腺细胞中含量最低。这些数据表明,Sos1独特地定位于在胸腺细胞发育早期影响信号转导。

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