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NAR Breakthrough Article A dimeric state for PRC2

机译:NAR突破性文章PRC2的二聚状态

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摘要

Polycomb repressive complex-2 (PRC2) is a histone methyltransferase required for epigenetic silencing during development and cancer. Long non-coding RNAs (lncRNAs) can recruit PRC2 to chromatin. Previous studies identified PRC2 subunits in a complex with the apparent molecular weight of a dimer, which might be accounted for by the incorporation of additional protein subunits or RNA rather than PRC2 dimerization. Here we show that reconstituted human PRC2 is in fact a dimer, using multiple independent approaches including analytical size exclusion chromatography (SEC), SEC combined with multi-angle light scattering and co-immunoprecipitation of differentially tagged subunits. Even though it contains at least two RNA-binding subunits, each PRC2 dimer binds only one RNA molecule. Yet, multiple PRC2 dimers bind a single RNA molecule cooperatively. These observations suggest a model in which the first RNA binding event promotes the recruitment of multiple PRC2 complexes to chromatin, thereby nucleating repression.
机译:聚梳抑制复合物2(PRC2)是组蛋白甲基转移酶,是发育和癌症过程中表观遗传沉默所必需的。长的非编码RNA(lncRNA)可以募集PRC2到染色质。先前的研究在与二聚体表观分子量的复合物中鉴定出PRC2亚基,这可能是由于掺入了其他蛋白质亚基或RNA而不是PRC2二聚体所致。在这里,我们显示重构的人PRC2实际上是一个二聚体,使用多种独立方法,包括分析尺寸排阻色谱(SEC),SEC与多角度光散射结合和差异标记亚基的共免疫沉淀。即使它包含至少两个RNA结合亚基,每个PRC2二聚体仅结合一个RNA分子。但是,多个PRC2二聚体可协同结合单个RNA分子。这些观察结果提出了一种模型,其中第一个RNA结合事件促进了多个PRC2复合物向染色质的募集,从而使抑制成核。

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