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Xist Deletional Analysis Reveals an Interdependency between Xist RNA and Polycomb Complexes for Spreading along the Inactive X

机译:XIST删除分析显示XIST RNA和Polycomb复合物之间的相互依存性,用于沿着无效X传播

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摘要

During X-inactivation, Xist RNA spreads along an entire chromosome to establish silencing. However, the mechanism and functional RNA elements involved in spreading remain undefined. By performing a comprehensive endogenous Xist deletion screen, we identify Repeat B as crucial for spreading Xist and maintaining Polycomb repressive complexes 1 and 2 (PRC1/PRC2) along the inactive X (Xi). Unexpectedly, spreading of these three factors is inextricably linked. Deleting Repeat B or its direct binding partner, HNRNPK, compromises recruitment of PRC1 and PRC2. In turn, ablating PRC1 or PRC2 impairs Xist spreading. Therefore, Xist and Polycomb complexes require each other to propagate along the Xi, suggesting a positive feedback mechanism between RNA initiator and protein effectors. Perturbing Xist/Polycomb spreading causes failure of de novo Xi silencing, with partial compensatory downregulation of the active X, and also disrupts topological Xi reconfiguration. Thus, Repeat B is a multifunctional element that integrates interdependent Xist/Polycomb spreading, silencing, and changes in chromosome architecture.
机译:在X-inactivation期间,XIST RNA沿整个染色体传播以建立沉默。然而,展开的机制和功能RNA元件仍未确定。通过进行全面的内源性XIST缺失筛网,我们将重复B识别为沿着无效X(XI)展开XIST和维持多元组压制复合物1和2(PRC1 / PRC2)的至关重要。出乎意料地,传播这三个因素是密不可分的。删除重复B或其直接装订合作伙伴,HNRNPK,妥协招聘PRC1和PRC2。反过来,消融的PRC1或PRC2损害了XIST扩散。因此,XIST和Polycomb复合物彼此沿XI繁殖,表明RNA引发剂和蛋白质效应之间的阳性反馈机制。扰动XIST / Polycomb扩展导致De Novo Xi Sulencing的失败,有源X的部分补偿下调,并且还破坏了拓扑XI重新配置。因此,重复B是一个多功能元素,其集成相互依存的XISC / POLYCOMB扩展,沉默和染色体体系结构的变化。

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