首页> 外文OA文献 >Nerve growth factor receptor signaling induces histone acetyltransferase domain-dependent nuclear translocation of p300/CREB-binding protein-associated factor and hGCN5 acetyltransferases.
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Nerve growth factor receptor signaling induces histone acetyltransferase domain-dependent nuclear translocation of p300/CREB-binding protein-associated factor and hGCN5 acetyltransferases.

机译:神经生长因子受体信号传导诱导组蛋白乙酰转移酶结构域依赖的p300 / CREB结合蛋白相关因子和hGCN5乙酰转移酶的核易位。

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摘要

The transcriptional coactivators, p300/CREB-binding protein-associated factor (PCAF) and hGCN5, are recruited to chromatin-remodeling complexes on enhancers of various gene promoters in response to growth factor stimulation. However, the molecular mechanisms by which surface receptor signals modulate the assembly of nuclear transcription complexes are not fully understood. Here we report that nerve growth factor receptor signaling induces nuclear translocation of PCAF and hGCN5 dependent upon the phosphorylation of Ser and Thr residues within their histone acetyltransferase domains, which requires activation of PI3K, Rsk2(pp90), and MSK-1. Neurotrophin stimulation induces p53(K320) acetylation by PCAF and transcriptionally activates p53-responsive enhancer elements within the p21(WAF/CIP1) promoter associated with G(1)/S arrest during neuronal differentiation. Most importantly, these findings represent the first evidence for signal-dependent nuclear translocation of PCAF and hGCN5 acetyltransferases and allude to a novel mechanism for ligand/receptor modulation of nuclear chromatin-remodeling complexes in neurons.
机译:转录共激活因子p300 / CREB结合蛋白相关因子(PCAF)和hGCN5被募集到各种基因启动子的增强子上的染色质重塑复合体,以响应生长因子的刺激。但是,尚不完全了解表面受体信号调节核转录复合物装配的分子机制。在这里我们报告神经生长因子受体信号传导诱导PCAF和hGCN5的核转位,取决于其组蛋白乙酰转移酶结构域内Ser和Thr残基的磷酸化,这需要激活PI3K,Rsk2(pp90)和MSK-1。 Neurotrophin刺激通过PCAF诱导p53(K320)乙酰化,并在神经元分化过程中转录激活与G(1)/ S阻滞相关的p21(WAF / CIP1)启动子内的p53反应增强子。最重要的是,这些发现代表了PCAF和hGCN5乙酰转移酶信号依赖性核易位的第一个证据,并暗示了神经元中核染色质重塑复合物的配体/受体调节的新机制。

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