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SMAR1 and Cux/CDP modulate chromatin and act as negative regulators of the TCR beta enhancer (E beta)

机译:SMAR1和Cux / CDP调节染色质并充当TCR beta增强子(E beta)的负调节剂

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摘要

Chromatin modulation at various cis-acting elements is critical for V(D)J recombination during T and B cell development. MARbeta, a matrix-associated region (MAR) located upstream of the T cell receptor beta (TCRbeta) enhancer (Ebeta), serves a crucial role in silencing Ebeta-mediated TCR activation. By DNaseI hypersensitivity assays, we show here that overexpression of the MAR binding proteins SMAR1 and Cux/CDP modulate the chromatin structure at MARbeta. We further demonstrate that the silencer function of MARbeta is mediated independently by SMAR1 and Cux/CDP as judged by their ability to repress Ebeta-dependent reporter gene expression. Moreover, the repressor activity of SMAR1 is strongly enhanced in the presence of Cux/CDP. These two proteins physically interact with each other and colocalize within the perinuclear region through a SMAR1 domain required for repression. The repression domain of SMAR1 is separate from the MARbeta binding domain and contains a nuclear localization signal and an arginine-serine (RS)-rich domain, characteristic of pre-mRNA splicing regulators. Our data suggest that at the double positive stage of T cell development, cis-acting MARbeta elements recruit the strong negative regulators Cux and SMAR1 to control Ebeta-mediated recombination and transcription.
机译:在T和B细胞发育过程中,各种顺式作用元件的染色质调节对于V(D)J重组至关重要。 MARbeta是位于T细胞受体beta(TCRbeta)增强子(Ebeta)上游的基质相关区域(MAR),在沉默Ebeta介导的TCR激活中起着至关重要的作用。通过DNaseI超敏性检测,我们在这里显示了MAR结合蛋白SMAR1和Cux / CDP的过表达调节了MARbeta的染色质结构。我们进一步证明,MARbeta的沉默子功能是由SMAR1和Cux / CDP独立介导的,由其抑制Ebeta依赖性报道基因表达的能力来判断。此外,在Cux / CDP的存在下,SMAR1的阻遏物活性大大增强。这两种蛋白质彼此物理相互作用,并通过阻抑所需的SMAR1结构域共定位在核周区域内。 SMAR1的阻抑域与MARbeta结合域是分离的,并且包含一个核定位信号和一个富含精氨酸-丝氨酸(RS)的域,这是前mRNA剪接调节子的特征。我们的数据表明,在T细胞发育的双阳性阶段,顺式作用的MARbeta元件募集了强大的负调控因子Cux和SMAR1,以控制Ebeta介导的重组和转录。

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