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Mediator coordinates PIC assembly with recruitment of CHD1.

机译:调解员通过招募CHD1协调PIC组装。

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摘要

Murine Chd1 (chromodomain helicase DNA-binding protein 1), a chromodomain-containing chromatin remodeling protein, is necessary for embryonic stem (ES) cell pluripotency. Chd1 binds to nucleosomes trimethylated at histone 3 Lys 4 (H3K4me3) near the beginning of active genes but not to bivalent domains also containing H3K27me3. To address the mechanism of this specificity, we reproduced H3K4me3- and CHD1-stimulated gene activation in HeLa extracts. Multidimensional protein identification technology (MuDPIT) and immunoblot analyses of purified preinitiation complexes (PICs) revealed the recruitment of CHD1 to naive chromatin but enhancement on H3K4me3 chromatin. Studies in depleted extracts showed that the Mediator coactivator complex, which controls PIC assembly, is also necessary for CHD1 recruitment. MuDPIT analyses of CHD1-associated proteins support the recruitment data and reveal numerous components of the PIC, including Mediator. In vivo, CHD1 and Mediator are recruited to an inducible gene, and genome-wide binding of the two proteins correlates well with active gene transcription in mouse ES cells. Finally, coimmunoprecipitation of CHD1 and Mediator from cell extracts can be ablated by shRNA knockdown of a specific Mediator subunit. Our data support a model in which the Mediator coordinates PIC assembly along with the recruitment of CHD1. The combined action of the PIC and H3K4me3 provides specificity in targeting CHD1 to active genes.
机译:鼠Chd1(染色体结构域解旋酶DNA结合蛋白1)是一种含有染色体结构域的染色质重塑蛋白,对于胚胎干(ES)细胞多能性是必需的。 Chd1结合在活性基因开始附近的组蛋白3 Lys 4(H3K4me3)处三甲基化的核小体,但不结合也包含H3K27me3的二价域。为了解决这种特异性的机制,我们在HeLa提取物中复制了H3K4me3-和CHD1刺激的基因激活。多维蛋白质鉴定技术(MuDPIT)和纯化的预起始复合物(PIC)的免疫印迹分析显示,CHD1募集到幼稚的染色质,但增强了H3K4me3染色质。耗竭的提取物的研究表明,控制PIC组装的Mediator共激活剂复合物对于CHD1募集也是必需的。与CHD1相关的蛋白的MuDPIT分析支持募集数据,并揭示了PIC的许多组件,包括介体。在体内,CHD1和介体被募集到可诱导的基因,并且这两种蛋白的全基因组结合与小鼠ES细胞中的活性基因转录良好相关。最后,可通过特异介体亚基的shRNA敲除来消除细胞提取物中CHD1和介体的免疫共沉淀。我们的数据支持一个模型,在该模型中,调解员协调PIC组装以及CHD1的募集。 PIC和H3K4me3的共同作用提供了将CHD1靶向活性基因的特异性。

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