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T细胞的发育受近端和远端Lck启动子在不同发育阶段发挥的协同作用调控。

T-cell development is regulated by the coordinated function of proximal and distal Lck promoters active at different developmental stages.

作者信息

Chiang Y Jeffrey, Hodes Richard J

机构信息

Experimental Immunology Branch, National Cancer Institute, Bethesda, MD, USA.

National Institute on Aging, National Institutes of Health, Bethesda, MD, USA.

出版信息

Eur J Immunol. 2016 Oct;46(10):2401-2408. doi: 10.1002/eji.201646440. Epub 2016 Aug 29.

Abstract

Expression of Lck, a T-cell lineage-specific tyrosine kinase critical for T-cell development and activation, can be mediated by either proximal or distal lck promoter. We generated BAC transgenic mice in which BAC lck promoter was deleted and bred these transgenes to an Lck knockout background. Lck-PROX mice, in which only the proximal promoter is functional, have maximal Lck protein and normal thymic development through CD4 CD8 double negative (DN) and CD4 CD8 double positive (DP) stages, but undetectable Lck later in development and reduced mature single positive thymocytes. In contrast, Lck-DIST mice, in which only distal promoter was functional, are deficient in Lck protein in DN and DP thymocytes and severely defective in early T-cell development, with a block at the DN3-DN4 beta checkpoint equivalent to complete Lck knockouts. The ability of the proximal lck promoter to support thymic development is independent of Fyn; while, in contrast, the distal lck promoter alone is completely unable to support development in the absence of Fyn. Notably, normal thymocyte development is restored by presence of both proximal and distal promoters, even when independently expressed on different lck genes. These results define distinct and complementary requirements for proximal and distal lck promoters during T-cell development.

摘要

Lck是一种对T细胞发育和激活至关重要的T细胞谱系特异性酪氨酸激酶,其表达可由近端或远端lck启动子介导。我们构建了BAC转基因小鼠,其中BAC lck启动子被删除,并将这些转基因培育到Lck基因敲除背景中。Lck-PROX小鼠中只有近端启动子起作用,其Lck蛋白水平最高,在通过CD4 CD8双阴性(DN)和CD4 CD8双阳性(DP)阶段时胸腺发育正常,但在发育后期检测不到Lck,成熟单阳性胸腺细胞减少。相比之下,Lck-DIST小鼠中只有远端启动子起作用,其DN和DP胸腺细胞中的Lck蛋白缺乏,早期T细胞发育严重缺陷,在DN3-DN4β检查点处受阻,相当于完全敲除Lck。近端lck启动子支持胸腺发育的能力独立于Fyn;相反,在没有Fyn的情况下,单独远端lck启动子完全无法支持发育。值得注意的是,即使近端和远端启动子在不同的lck基因上独立表达,两者同时存在也能恢复正常的胸腺细胞发育。这些结果确定了T细胞发育过程中近端和远端lck启动子的不同且互补的需求。

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