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Genome-wide assessment of differential roles for p300 and CBP in transcription regulation

机译:全基因组评估p300和CBP在转录调控中的不同作用

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摘要

Despite high levels of homology, transcription coactivators p300 and CREB binding protein (CBP) are both indispensable during embryogenesis. They are largely known to regulate the same genes. To identify genes preferentially regulated by p300 or CBP, we performed an extensive genome-wide survey using the ChIP-seq on cell-cycle synchronized cells. We found that 57% of the tags were within genes or proximal promoters, with an overall preference for binding to transcription start and end sites. The heterogeneous binding patterns possibly reflect the divergent roles of CBP and p300 in transcriptional regulation. Most of the 16 103 genes were bound by both CBP and p300. However, after stimulation 89 and 1944 genes were preferentially bound by CBP or p300, respectively. Target genes were found to be primarily involved in the regulation of metabolic and developmental processes, and transcription, with CBP showing a stronger preference than p300 for genes active in negative regulation of transcription. Analysis of transcription factor binding sites suggest that CBP and p300 have many partners in common, but AP-1 and Serum Response Factor (SRF) appear to be more prominent in CBP-specific sequences, whereas AP-2 and SP1 are enriched in p300-specific targets. Taken together, our findings further elucidate the distinct roles of coactivators p300 and CBP in transcriptional regulation.
机译:尽管同源性很高,但转录共激活因子p300和CREB结合蛋白(CBP)在胚胎发生过程中都是必不可少的。众所周知,它们调节相同的基因。为了鉴定优先受p300或CBP调控的基因,我们使用ChIP-seq对细胞周期同步细胞进行了广泛的全基因组调查。我们发现57%的标签位于基因或近端启动子内,总体上更喜欢与转录起始和终止位点结合。异质结合模式可能反映了CBP和p300在转录调控中的不同作用。 16103个基因中的大多数都与CBP和p300结合。但是,刺激后,分别有89和1944个基因分别被CBP或p300结合。发现靶基因主要参与代谢和发育过程以及转录的调控,CBP对转录负调控的活跃基因表现出比p300更强的偏好。对转录因子结合位点的分析表明,CBP和p300有许多共同的伴侣,但是AP-1和血清反应因子(SRF)在CBP特异性序列中似乎更为突出,而AP-2和SP1在p300-具体目标。综上所述,我们的发现进一步阐明了共激活因子p300和CBP在转录调控中的独特作用。

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