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Talking to chromatin: post-translational modulation of polycomb group function

机译:谈论染色质:多梳基团功能的翻译后调节

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Polycomb Group proteins are important epigenetic regulators of gene expression. Epigenetic control by polycomb Group proteins involves intrinsic as well as associated enzymatic activities. Polycomb target genes change with cellular context, lineage commitment and differentiation status, revealing dynamic regulation of polycomb function. It is currently unclear how this dynamic modulation is controlled and how signaling affects polycomb-mediated epigenetic processes at the molecular level. Experimental evidence on regulation of polycomb function by post-translational mechanisms is steadily emerging: Polycomb Group proteins are targeted for ubiquitylation, sumoylation and phosphorylation. In addition, specific Polycomb Group proteins modify other (chromatin) associated proteins via similar post-translational modifications. Such modifications affect protein function by affecting protein stability, protein-protein interactions and enzymatic activities. Here, we review current insights in covalent modification of Polycomb Group proteins in the context of protein function and present a tentative view of integrated signaling to chromatin in the context of phosphorylation. Clearly, the available literature reveals just the tip of the iceberg, and exact molecular mechanisms in, and the biological relevance of post-translational regulation of polycomb function await further elucidation. Our understanding of causes and consequences of post-translational modification of polycomb proteins will gain significantly from in vivo validation experiments. Impaired polycomb function has important repercussions for stem cell function, development and disease. Ultimately, increased understanding of signaling to chromatin and the mechanisms involved in epigenetic remodeling will contribute to the development of therapeutic interventions in cell fate decisions in development and disease.
机译:聚梳组蛋白是基因表达的重要表观遗传调控因子。聚梳组蛋白的表观遗传控制涉及内在以及相关的酶促活性。聚梳靶基因随细胞背景,谱系承诺和分化状态而变化,揭示了聚梳功能的动态调节。目前尚不清楚如何控制这种动态调节,以及信号如何在分子水平上影响多梳介导的表观遗传过程。通过翻译后机制调节聚梳功能的实验证据正在不断涌现:聚梳组蛋白的目标是泛素化,SUMO化和磷酸化。另外,特定的Polycomb Group蛋白通过类似的翻译后修饰来修饰其他(染色质)相关蛋白。这样的修饰通过影响蛋白质稳定性,蛋白质-蛋白质相互作用和酶活性来影响蛋白质功能。在这里,我们审查当前的见解在蛋白质功能的上下文中的共价修饰的Polycomb组蛋白,并提出了在磷酸化的背景下向染色质的整合信号的初步观点。显然,现有文献揭示了冰山一角,以及其中的确切分子机制,并且对多梳功能的翻译后调控的生物学相关性有待进一步阐明。通过体内验证实验,我们对多梳蛋白翻译后修饰的原因和后果的了解将非常重要。受损的多梳功能对干细胞功能,发育和疾病具有重要影响。最终,人们对染色质信号传导的更多理解以及表观遗传重塑所涉及的机制将有助于在发展和疾病中决定细胞命运的治疗性干预措施的发展。

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