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Identification of small molecules that inhibit the histone chaperone Asf1 and its chromatin function

机译:鉴定抑制组蛋白伴侣Asf1及其染色质功能的小分子

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摘要

The eukaryotic genome is packed into chromatin, which is important for the genomic integrity and gene regulation. Chromatin structures are maintained through assembly and disassembly of nucleosomes catalyzed by histone chaperones. Asf1 (anti-silencing function 1) is a highly conserved histone chaperone that mediates histone transfer on/off DNA and promotes histone H3 lysine 56 acetylation at globular core domain of histone H3. To elucidate the role of Asf1 in the modulation of chromatin structure, we screened and identified small molecules that inhibit Asf1 and H3K56 acetylation without affecting other histone modifications. These pyrimidine-2,4,6-trione derivative molecules inhibited the nucleosome assembly mediated by Asf1 in vitro, and reduced the H3K56 acetylation in HeLa cells. Furthermore, production of HSV viral particles was reduced by these compounds. As Asf1 is implicated in genome integrity, cell proliferation, and cancer, current Asf1 inhibitor molecules may offer an opportunity for the therapeutic development for treatment of diseases. [BMB Reports 2015; 48(12): 685-690]
机译:真核生物基因组被装入染色质中,这对于基因组完整性和基因调控很重要。染色质结构是通过组蛋白伴侣蛋白催化的核小体的组装和拆卸来维持的。 Asf1(抗沉默功能1)是高度保守的组蛋白分子伴侣,可介导组蛋白转移DNA的作用,并促进组蛋白H3球状核心结构域的组蛋白H3赖氨酸56乙酰化。为了阐明Asf1在染色质结构调节中的作用,我们筛选并鉴定了抑制Asf1和H3K56乙酰化而不影响其他组蛋白修饰的小分子。这些嘧啶2,4,6-三酮衍生物分子在体外抑制了Asf1介导的核小体装配,并减少了HeLa细胞中的H3K56乙酰化。此外,这些化合物减少了HSV病毒颗粒的产生。由于Asf1与基因组完整性,细胞增殖和癌症有关,目前的Asf1抑制剂分子可能为疾病的治疗开发提供机会。 [BMB报告2015; 48(12):685-690]

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