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Phosphorylation-regulated binding of RNA polymerase II to fibrous polymers of low-complexity domains

机译:磷酸化调节RNA聚合酶II与低复杂度结构域的纤维状聚合物的结合

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The low-complexity (LC) domains of the products of the fused in sarcoma (FUS), Ewings sarcoma (EWS), and TAF15 genes are translocated onto a variety of different DNA-binding domains and thereby assist in driving the formation of cancerous cells. In the context of the translocated fusion proteins, these LC sequences function as transcriptional activation domains. Here, we show that polymeric fibers formed from these LC domains directly bind the C-terminal domain (CTD) of RNA polymerase II in a manner reversible by phosphorylation of the iterated, heptad repeats of the CTD. Mutational analysis indicates that the degree of binding between the CTD and the LC domain polymers correlates with the strength of transcriptional activation. These studies offer a simple means of conceptualizing how RNA polymerase II is recruited to active genes in its unphosphorylated state and released for elongation following phosphorylation of the CTD. PaperFlick
机译:肉瘤融合(FUS),尤因氏肉瘤(EWS)和TAF15基因的产物的低复杂度(LC)结构域易位到各种不同的DNA结合结构域中,从而有助于推动癌细胞的形成。在易位融合蛋白的情况下,这些LC序列起转录激活域的作用。在这里,我们显示了由这些LC结构域形成的聚合纤维直接结合RNA聚合酶II的C端结构域(CTD),其方式可通过CTD的七倍体重复序列的磷酸化来逆转。突变分析表明,CTD和LC域聚合物之间的结合程度与转录激活的强度相关。这些研究提供了一种简单的方法,可以概念化如何将RNA聚合酶II募集到处于未磷酸化状态的活性基因中,并在CTD磷酸化后释放以延伸。 PaperFlick

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