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Developmentally regulated alterations in Polycomb repressive complex 1 proteins on the inactive X chromosome

机译:X染色体上无活性的Polycomb阻遏复合物1蛋白的发育调控变化

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摘要

Polycomb group (PcG) proteins belonging to the polycomb (Pc) repressive complexes 1 and 2 (PRC1 and PRC2) maintain homeotic gene silencing. In Drosophila, PRC2 methylates histone H3 on lysine 27, and this epigenetic mark facilitates recruitment of PRC1. Mouse PRC2 (mPRC2) has been implicated in X inactivation, as mPRC2 proteins transiently accumulate on the inactive X chromosome (Xi) at the onset of X inactivation to methylate histone H3 lysine 27 (H3-K27). In this study, we demonstrate that mPRC1 proteins localize to the Xi, and that different mPRC1 proteins accumulate on the Xi during initiation and maintenance of X inactivation in embryonic cells. The Xi accumulation of mPRC1 proteins requires Xist RNA and is not solely regulated by the presence of H3-K27 methylation, as not all cells that exhibit this epigenetic mark on the Xi show Xi enrichment of mPRC1 proteins. Our results implicate mPRC1 in X inactivation and suggest that the regulated assembly of PcG protein complexes on the Xi contributes to this multistep process.
机译:属于polycomb(Pc)阻遏复合物1和2(PRC1和PRC2)的polycomb group(PcG)蛋白保持同源基因沉默。在果蝇中,PRC2使赖氨酸27上的组蛋白H3甲基化,该表观遗传标记促进了PRC1的募集。小鼠PRC2(mPRC2)已与X失活有关,因为在X失活开始时mPRC2蛋白会短暂地积聚在非活性X染色体(Xi)上,从而甲基化组蛋白H3赖氨酸27(H3-K27)。在这项研究中,我们证明了mPRC1蛋白位于Xi,而在胚胎细胞X失活的起始和维持过程中,不同的mPRC1蛋白在Xi上积累。 mPRC1蛋白的Xi积累需要Xist RNA,并且不仅受H3-K27甲基化的存在调控,因为并非所有在Xi上显示此后生标记的细胞都显示Xi富集了mPRC1蛋白。我们的结果暗示mPRC1处于X灭活状态,并暗示Xi上PcG蛋白复合物的受调控组装有助于此多步过程。

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