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首页> 外文期刊>Cell Reports >Brd4’s Bromodomains Mediate Histone H3 Acetylation and Chromatin Remodeling in Pluripotent Cells through P300 and Brg1
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Brd4’s Bromodomains Mediate Histone H3 Acetylation and Chromatin Remodeling in Pluripotent Cells through P300 and Brg1

机译:Brd4的Bromodomains通过P300和Brg1介导多能细胞中的组蛋白H3乙酰化和染色质重塑。

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h2 class="section-title"Summary/h2 p id="abspara0010"The pluripotent state of embryonic stem cells (ESCs) is defined by its transcriptome and epigenome. The chromatin reader Brd4 determines ESC identity. Although Brd4 regulation in gene transcription has been well described, its contribution to the chromatin landscape is less known. Here, we show that Brd4’s bromodomains partner with the histone acetyltransferase P300, increasing its enzymatic activities. Augmenting histone acetylation by Brd4-P300 interaction recruits the chromatin remodeler Brg1 altering chromatin structure. This pathway is important for maintaining the expression and chromatin patterns of pluripotency-associated genes, such as Oct4 , Nanog , and the X chromosome regulatory long noncoding RNAs Tsix and Xite . Furthermore, we show that the Brd4-P300 interaction regulates the de novo formation of chromatin marks during ESC differentiation, as exemplified by controlling the master regulators of mesoderm formation. Collectively, we delineate the function of Brd4 in organizing the chromatin structure that contributes to gene transcriptional regulation and cell fate determination.
机译:class =“ section-title”>摘要 id =“ abspara0010”>胚胎干细胞(ESC)的多能状态由其转录组和表观基因组定义。染色质读取器Brd4确定ESC身份。尽管已经很好地描述了在基因转录中的Brd4调控,但是它对染色质的贡献却鲜为人知。在这里,我们显示Brd4的bromodomains与组蛋白乙酰转移酶P300结合,增加了其酶促活性。通过Brd4-P300相互作用增强组蛋白乙酰化,可募集染色质重塑剂Brg1改变染色质结构。该途径对于维持多能性相关基因(例如Oct4,Nanog和X染色体调控长非编码RNA Tsix和Xite)的表达和染色质模式很重要。此外,我们表明Brd4-P300相互作用调节ESC分化过程中染色质标记的从头形成,如通过控制中胚层形成的主调节器所例证。我们共同描述了Brd4在组织染色质结构中的功能,该结构有助于基因转录调控和细胞命运的确定。

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