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Genetic complementation analysis showed distinct contributions of the N-terminal tail of H2A.Z to epigenetic regulations

机译:遗传互补分析显示H2A.Z N末端尾巴对表观遗传调控的独特贡献

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H2A.Z is one of the most evolutionally conserved histone variants. In vertebrates, this histone variant has two isoforms, H2A.Z.1 and H2A.Z.2, each of which is coded by an individual gene. H2A.Z is involved in multiple epigenetic regulations, and in humans, it also has relevance to carcinogenesis. In this study, we used the H2A.Z DKO cells, in which both H2A.Z isoform genes could be inducibly knocked out, for the functional analysis of H2A.Z by a genetic complementation assay, as the first example of its kind in vertebrates. Ectopically expressed wild-type H2A.Z and two N-terminal mutants, a nonacetylable H2A.Z mutant and a chimera in which the N-terminal tail of H2A.Z.1 was replaced with that of the canonical H2A, complemented the mitotic defects of H2A.Z DKO cells similarly, suggesting that both acetylation and distinctive sequence of the N-terminal tail of H2A.Z are not required for mitotic progression. In contrast, each one of these three forms of H2A.Z complemented the transcriptional defects of H2A.Z DKO cells differently. These results suggest that the N-terminal tail of vertebrate H2A.Z makes distinctively different contributions to these epigenetic events. Our results also imply that this genetic complementation system is a novel and useful tool for the functional analysis of H2A.Z.
机译:H2A.Z是进化最保守的组蛋白变体之一。在脊椎动物中,该组蛋白变异体具有两个同工型,H2A.Z.1和H2A.Z.2,每个同工型由一个单独的基因编码。 H2A.Z与多种表观遗传调控有关,在人类中,它也与致癌作用有关。在这项研究中,我们使用H2A.Z DKO细胞(其中两个H2A.Z亚型基因均可被诱导敲除),通过遗传互补分析对H2A.Z进行功能分析,作为脊椎动物中此类的首例。异位表达的野生型H2A.Z和两个N末端突变体,一个不可乙酰化的H2A.Z突变体和一个嵌合体,其中将H2A.Z.1的N末端尾部替换为规范H2A的尾部,从而补充了有丝分裂缺陷H2A.Z DKO细胞具有类似的特征,表明有丝分裂进程既不需要乙酰化,又不需要H2A.Z N末端尾巴的独特序列。相反,这三种形式的H2A.Z中的每一种都不同地补充了H2A.Z DKO细胞的转录缺陷。这些结果表明,脊椎动物H2A.Z的N末端尾巴对这些表观遗传事件做出了截然不同的贡献。我们的结果还暗示,这种遗传互补系统是H2A.Z功能分析的一种新颖且有用的工具。

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