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The nucleosome: a little variation goes a long way

机译:核小体:稍有变化就能走很长一段路

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Changes in the overall structure of chromatin are essential for the proper regulation of cellular processes, including gene activation and silencing, DNA repair, chromosome segregation during mitosis and meiosis, X chromosome inactivation in female mammals, and chromatin compaction during apoptosis. Such alterations of the chromatin template occur through at least 3 interrelated mechanisms: post-translational modifications of histones, ATP-dependent chromatin remodeling, and the incorporation (or replacement) of specialized histone variants into chromatin. Of these mechanisms, the exchange of variants into and out of chromatin is the least well understood. However, the exchange of conventional histones for variant histones has distinct and profound consequences within the cell. This review focuses on the growing number of mammalian histone variants, their particular biological functions and unique features, and how they may affect the structure of the nucleosome. We propose that a given nucleosome might not consist of heterotypic variants, but rather, that only specific histone variants come together to form a homotypic nucleosome, a hypothesis that we refer to as the nucleosome code. Such nucleosomes might in turn participate in marking specific chromatin domains that may contribute to epigenetic inheritance.
机译:染色质整体结构的变化对于正确调节细胞过程至关重要,包括基因激活和沉默,DNA修复,有丝分裂和减数分裂过程中的染色体分离,雌性哺乳动物的X染色体失活以及凋亡过程中的染色质紧实。染色质模板的这种改变是通过至少3种相互关联的机制发生的:组蛋白的翻译后修饰,ATP依赖的染色质重塑以及将专门的组蛋白变体掺入(或替代)染色质。在这些机制中,人们对变体进出染色质的了解最少。然而,将常规组蛋白交换为变异组蛋白在细胞内具有独特而深刻的后果。这篇综述的重点是越来越多的哺乳动物组蛋白变体,其特定的生物学功能和独特特征,以及它们如何影响核小体的结构。我们建议给定的核小体可能不由异型变体组成,而是只有特定的组蛋白变体一起形成同型核小体,这一假说我们称为核小体密码。此类核小体可能反过来参与标记可能有助于表观遗传的特定染色质结构域。

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