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Histone H1 Subtypes Differentially Modulate Chromatin Condensation without Preventing ATP-Dependent Remodeling by SWI/SNF or NURF

机译:组蛋白H1亚型在不阻止SWI / SNF或NURF ATP依赖重塑的情况下差异调节染色质凝结

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摘要

Although ubiquitously present in chromatin, the function of the linker histone subtypes is partly unknown and contradictory studies on their properties have been published. To explore whether the various H1 subtypes have a differential role in the organization and dynamics of chromatin we have incorporated all of the somatic human H1 subtypes into minichromosomes and compared their influence on nucleosome spacing, chromatin compaction and ATP-dependent remodeling. H1 subtypes exhibit different affinities for chromatin and different abilities to promote chromatin condensation, as studied with the Atomic Force Microscope. According to this criterion, H1 subtypes can be classified as weak condensers (H1.1 and H1.2), intermediate condensers (H1.3) and strong condensers (H1.0, H1.4, H1.5 and H1x). The variable C-terminal domain is required for nucleosome spacing by H1.4 and is likely responsible for the chromatin condensation properties of the various subtypes, as shown using chimeras between H1.4 and H1.2. In contrast to previous reports with isolated nucleosomes or linear nucleosomal arrays, linker histones at a ratio of one per nucleosome do not preclude remodeling of minichromosomes by yeast SWI/SNF or Drosophila NURF. We hypothesize that the linker histone subtypes are differential organizers of chromatin, rather than general repressors.
机译:尽管普遍存在于染色质中,但是连接子组蛋白亚型的功能尚不明确,有关其性质的矛盾研究已经发表。为了探索各种H1亚型在染色质的组织和动力学中是否具有不同的作用,我们将所有人体H1亚型整合到了微染色体中,并比较了它们对核小体间距,染色质紧实度和ATP依赖性重塑的影响。根据原子力显微镜研究,H1亚型对染色质表现出不同的亲和力,并具有不同的促进染色质凝聚的能力。根据此标准,H1亚型可分为弱冷凝器(H1.1和H1.2),中间冷凝器(H1.3)和强冷凝器(H1.0,H1.4,H1.5和H1x)。可变的C末端结构域对于H1.4的核小体间隔是必需的,并且可能负责各种亚型的染色质缩合特性,如使用H1.4和H1.2之间的嵌合体所示。与先前关于分离的核小体或线性核小体阵列的报道相比,每个核小体比例为一个的接头组蛋白不排除酵母SWI / SNF或果蝇NURF对微染色体的重塑。我们假设接头组蛋白亚型是染色质的差异组织者,而不是一般的阻遏物。

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