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Linker histone variants control chromatin dynamics during early embryogenesis

机译:接头组蛋白变异控制早期胚胎发生过程中的染色质动力学

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摘要

Complex transitions in chromatin structure produce changes in genome function during development in metazoa. Linker histones, the last component of nucleosomes to be assembled into chromatin, comprise considerably divergent subtypes as compared with core histones. In all metazoa studied, their composition changes dramatically during early embryogenesis concomitant with zygotic gene activation, leading to distinct functional changes that are still poorly understood. Here, we show that early embryonic linker histone B4, which is maternally expressed, is functionally different from somatic histone H1 in influencing chromatin structure and dynamics. We developed a chromatin assembly system with nucleosome assembly protein-1 as a linker histone chaperone. This assay system revealed that maternal histone B4 allows chromatin to be remodeled by ATP-dependent chromatin remodeling factor, whereas somatic histone H1 prevents this remodeling. Structural analysis shows that histone B4 does not significantly restrict the accessibility of linker DNA. These findings define the functional significance of developmental changes in linker histone variants. We propose a model that holds that maternally expressed linker histones are key molecules specifying nuclear dynamics with respect to embryonic totipotency.
机译:染色质结构的复杂转变会在后生动物发育期间产生基因组功能的变化。与核心组蛋白相比,接头组蛋白是要组装成染色质的核小体的最后一个成分,其亚型明显不同。在所有研究的后生动物中,它们的组成在早期胚胎发生过程中伴随着合子基因激活而发生了巨大变化,导致明显的功能变化,人们对此仍然知之甚少。在这里,我们显示母本表达的早期胚胎连接蛋白组蛋白B4在影响染色质结构和动力学方面与体细胞组蛋白H1在功能上有所不同。我们开发了核仁组装蛋白-1作为连接蛋白组蛋白伴侣的染色质组装系统。该测定系统显示,母体组蛋白B4允许染色质被ATP依赖的染色质重塑因子重塑,而体细胞组蛋白H1阻止了这种重塑。结构分析表明,组蛋白B4不会显着限制接头DNA的可及性。这些发现确定了接头组蛋白变体中发育变化的功能意义。我们提出一个模型,该模型认为母体表达的连接子组蛋白是指定关于胚胎全能性的核动力学的关键分子。

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