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Systematic allelic analysis defines the interplay of key pathways in X chromosome inactivation

机译:系统等位基因分析定义了X染色体灭活中的关键途径的相互作用

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Xist RNA, the master regulator of X chromosome inactivation, acts in cis to induce chromosome-wide silencing. Whilst recent studies have defined candidate silencing factors, their relative contribution to repressing different genes, and their relationship with one another is poorly understood. Here we describe a systematic analysis of Xist-mediated allelic silencing in mouse embryonic stem cell-based models. Using a machine learning approach we identify distance to the Xist locus and prior gene expression levels as key determinants of silencing efficiency. We go on to show that Spen, recruited through the Xist A-repeat, plays a central role, being critical for silencing of all except a subset of weakly expressed genes. Polycomb, recruited through the Xist B/C-repeat, also plays a key role, favouring silencing of genes with pre-existing H3K27me3 chromatin. LBR and the Rbm15/m6A-methyltransferase complex make only minor contributions to gene silencing. Together our results provide a comprehensive model for Xist-mediated chromosome silencing.
机译:XIST RNA,X染色体灭活的主调节剂,在CIS诱导染色体沉默的沉默中。虽然最近的研究已经确定了候选人沉默因子,但他们对抑制不同基因的相对贡献,以及他们彼此的关系很差。在这里,我们描述了对小鼠胚胎干细胞的模型中XIST介导的等位基因沉默的系统分析。使用机器学习方法,我们将与XIST基因座的距离和先前基因表达水平识别为沉默效率的关键决定因素。我们继续展示斯普斯,通过XISE A-Repeat招聘,发挥着核心作用,除了弱表达基因的子集之外的沉默是至关重要的。通过XIST B / C重复招募的Polycomb也起到了关键作用,有利于将基因的沉默与预先存在的H3K27ME3染色质。 LBr和RBM15 / M6A-甲基转移酶复合物仅为基因沉默作出少量贡献。我们的结果在一起为XIST介导的染色体沉默提供了全面的模型。

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