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T-cell receptor signaling induces proximal Runx1 transactivation via a calcineurin-NFAT pathway

机译:t细胞受体信号诱发近端Runx1通过calcineurin-NFAT transactivation途径

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摘要

Runx1 transcription factor is a key player in the development and function of T cells. Runx1 transcripts consist of two closely related isoforms (proximal and distal Runx1) whose expressions are regulated by different promoters. Which Runx1 isoform is expressed appears to be tightly regulated. The regulatory mechanism for differential transcription is, however, not fully understood. In this study, we investigated the regulation of the proximal Runx1 promoter in T cells. We showed that proximal Runx1 was expressed at a low level in na?ve T cells from C57BL/6 mice, but its expression was remarkably induced upon T-cell activation. In the promoter of proximal Runx1, a highly conserved region was identified which spans from -412 to the transcription start site and harbors a NFAT binding site. In a luciferase reporter assay, this region was found to be responsive to T-cell activation through Lck and calcineurin pathways. Mutagenesis studies and chromatin immunoprecipitation assay indicated that the NFAT site was essential for NFAT binding and transactivation of the proximal Runx1 promoter. Furthermore, TCR signaling-induced expression of proximal Runx1 was blocked by treatment of cells with cyclosporin A. Together, these results demonstrate that the calcineurin-NFAT pathway regulates proximal Runx1 transcription upon TCR stimulation.
机译:Runx1转录因子是一个关键球员T细胞的发育和功能。成绩单由两个密切相关的亚型(近端和远端Runx1)的表达式是由不同的启动子。这Runx1表达似乎是同种型严格监管。然而,微分转录不完全理解。Runx1近端启动子的调控T细胞。na表达在低水平?但C57BL / 6小鼠,其表达式非常在t细胞活化诱导。近端Runx1、高度保守的区域从-412年到大的了NFAT转录起始站点和港口结合位点。这个地区被发现对t细胞的反应通过Lck和钙调磷酸酶通路激活。诱变研究和染色质免疫沉淀反应试验表明,NFAT网站是NFAT绑定和必要条件transactivation Runx1近端启动子。此外,TCR signaling-induced表达近端Runx1被治疗的细胞和环孢菌素a在一起,这些结果证明calcineurin-NFAT通路调节近端对TCR Runx1转录刺激。

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