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Role of Intrinsic Protein Disorder in the Function and Interactions of the Transcriptional Coactivators CREB-binding Protein (CBP) and p300

机译:固有蛋白紊乱在转录共激活因子CREB结合蛋白(CBP)和p300的功能和相互作用中的作用

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摘要

The transcriptional coactivators CREB-binding protein (CBP) and p300 undergo a particularly rich set of interactions with disordered and partly ordered partners, as a part of their ubiquitous role in facilitating transcription of genes. CBP and p300 contain a number of small structured domains that provide scaffolds for the interaction of disordered transactivation domains from a wide variety of partners, including p53, hypoxia-inducible factor 1α (HIF-1α), NF-κB, and STAT proteins, and are the targets for the interactions of disordered viral proteins that compete with cellular factors to disrupt signaling and subvert the cell cycle. The functional diversity of the CBP/p300 interactome provides an excellent example of the power of intrinsic disorder to facilitate the complexity of living systems.
机译:转录共激活因子CREB结合蛋白(CBP)和p300与无序和部分有序伴侣发生了特别丰富的相互作用,这是它们在促进基因转录中普遍存在的作用的一部分。 CBP和p300包含许多小的结构化结构域,这些结构域为来自众多配偶体(包括p53,缺氧诱导因子1α(HIF-1α),NF-κB和STAT蛋白)的无序反式激活结构域的相互作用提供了支架。是无序病毒蛋白与细胞因子竞争以破坏信号传导并破坏细胞周期的相互作用的靶标。 CBP / p300相互作用基因组的功能多样性提供了一个很好的例子,说明内在障碍促进了生命系统的复杂性。

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