首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >The nuclear matrix protein CIZ1 facilitates localization of Xist RNA to the inactive X-chromosome territory
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The nuclear matrix protein CIZ1 facilitates localization of Xist RNA to the inactive X-chromosome territory

机译:核基质蛋白CIZ1促进XIST RNA定位到无活性的X-染色体区域

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The nuclear matrix protein Cip1-interacting zinc finger protein 1 (CIZ1) promotes DNA replication in association with cyclins and has been linked to adult and pediatric cancers. Here we show that CIZ1 is highly enriched on the inactive X chromosome (Xi) in mouse and human female cells and is retained by interaction with the RNA-dependent nuclear matrix. CIZ1 is recruited to Xi in response to expression of X inactive-specific transcript (Xist) RNA during the earliest stages of X inactivation in embryonic stem cells and is dependent on the C-terminal nuclear matrix anchor domain of CIZ1 and the E repeats of Xist. CIZ1-null mice, although viable, display fully penetrant female-specific lymphoproliferative disorder. Interestingly, in mouse embryonic fibroblast cells derived from CIZ1-null embryos, Xist RNA localization is disrupted, being highly dispersed through the nucleoplasm rather than focal. Focal localization is reinstated following re-expression of CIZ1. Focal localization of Xist RNA is also disrupted in activated B and T cells isolated from CIZ1-null animals, suggesting a possible explanation for female-specific lymphoproliferative disorder. Together, these findings suggest that CIZ1 has an essential role in anchoring Xist to the nuclear matrix in specific somatic lineages.
机译:核基质蛋白CIP1 - 相互作用的锌指蛋白1(CIZ1)促进与细胞周期司相关的DNA复制,并与成人和儿科癌症相关联。在这里,我们表明CIZ1高度富集在小鼠和人氏母细胞中的无活性X染色体(XI)上,并通过与RNA依赖性核基质的相互作用而保留。 CIZ1响应于胃肠干细胞X失活阶段的最早阶段的X无活性特异性转录物(XIST)RNA的表达,依赖于C末端核基质锚固结构域和XIST的Xist 。 Ciz1-null小鼠,虽然可行,显示出完全渗透的女性特异性淋巴抑制性疾病。有趣的是,在衍生自Ciz1-Null胚胎的小鼠胚胎成纤维细胞中,XIST RNA定位被破坏,高度分散通过核状而不是焦点。在重新表达CIZ1之后恢复焦点定位。 XIST RNA的焦点定位也破坏了从Ciz1-Null动物分离的活化的B和T细胞中断,表明对女特异性淋巴抑制性疾病的可能解释。这些研究结果表明CIZ1在锚定XIST在特定的体制谱系中的核基质中具有重要作用。

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