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泛素结合型DNA修复酶HHR6A和HHR6B的表达表明其在精子发生和染色质修饰中发挥作用。

Expression of the ubiquitin-conjugating DNA repair enzymes HHR6A and B suggests a role in spermatogenesis and chromatin modification.

作者信息

Koken M H, Hoogerbrugge J W, Jasper-Dekker I, de Wit J, Willemsen R, Roest H P, Grootegoed J A, Hoeijmakers J H

机构信息

Department of Cell Biology and Genetics, Erasmus University, Rotterdam, The Netherlands.

出版信息

Dev Biol. 1996 Jan 10;173(1):119-32. doi: 10.1006/dbio.1996.0011.

Abstract

RAD6, a member of the expanding family of ubiquitin-conjugating (E2) enzymes, functions in the so-called "N-rule" protein breakdown pathway of Saccharomyces cerevisiae. In vitro, the protein can attach one or multiple ubiquitin (Ub) moieties to histones H2A and B and trigger their E3-dependent degradation. Rad6 mutants display a remarkably pleiotropic phenotype, implicating the protein in DNA damage-induced mutagenesis, postreplication repair, repression of retrotransposition, and sporulation. RAD6 transcription is strongly induced upon UV exposure and in meiosis, suggesting that it is part of a damage-induced response pathway and that it is involved in meiotic recombination. It is postulated that the protein exerts its functions by modulating chromatin structure. Previously, we have cloned two human homologs of this gene (designated HHR6A and HHR6B) and demonstrated that they partially complement the yeast defect. Here we present a detailed characterisation of their expression at the transcript and protein levels. Both HHR6 proteins, resolved by 2-dimensional immunoblot analysis, are expressed in all mammalian tissues and cell types examined, indicating that both genes are functional and constitutively expressed. Although the proteins are highly conserved, the UV induction present in yeast is not preserved, pointing to important differences in damage response between yeast and mammals. Absence of alterations in HHR6 transcripts or protein upon heat shock and during the cell cycle suggests that the proteins are not involved in stress response or cell cycle regulation. Elevated levels of HHR6 transcripts and proteins were found in testis. Enhanced HHR6 expression did not coincide with meiotic recombination but with the replacement of histones by transition proteins. Immunohistochemistry demonstrated that the HHR6 proteins are located in the nucleus, consistent with a functional link with chromatin. Electron microscopy combined with immunogold labeling revealed a preferential localisation of HHR6 in euchromatin areas, suggesting that the protein is associated with transcriptionally active regions. Our findings support the idea that both HHR6 genes have overlapping, constitutive functions related to chromatin conformation and that they have a specific role in spermatogenesis, involving Ub-mediated histone degradation.

摘要

RAD6是泛素结合(E2)酶不断扩大的家族中的一员,在酿酒酵母所谓的“N-规则”蛋白质降解途径中发挥作用。在体外,该蛋白质可将一个或多个泛素(Ub)部分连接到组蛋白H2A和B上,并触发其依赖E3的降解。Rad6突变体表现出明显的多效性表型,表明该蛋白质参与DNA损伤诱导的诱变、复制后修复、逆转座抑制和孢子形成。RAD6转录在紫外线照射和减数分裂时强烈诱导,表明它是损伤诱导反应途径的一部分,并且参与减数分裂重组。据推测,该蛋白质通过调节染色质结构发挥其功能。此前,我们已克隆了该基因(命名为HHR6A和HHR6B)的两个人类同源物,并证明它们部分弥补了酵母缺陷。在此,我们展示了它们在转录本和蛋白质水平上表达的详细特征描述。通过二维免疫印迹分析解析的两种HHR6蛋白质,在所检测的所有哺乳动物组织和细胞类型中均有表达,表明这两个基因具有功能且组成性表达。尽管这些蛋白质高度保守,但酵母中存在的紫外线诱导现象并未保留,这表明酵母和哺乳动物在损伤反应方面存在重要差异。热休克和细胞周期过程中HHR6转录本或蛋白质未发生改变,表明这些蛋白质不参与应激反应或细胞周期调控。在睾丸中发现HHR6转录本和蛋白质水平升高。HHR6表达增强与减数分裂重组不一致,而是与组蛋白被过渡蛋白取代有关。免疫组织化学表明,HHR6蛋白质位于细胞核中,这与它与染色质的功能联系一致。电子显微镜结合免疫金标记显示,HHR6优先定位于常染色质区域,表明该蛋白质与转录活跃区域相关。我们的研究结果支持这样一种观点,即两个HHR6基因具有与染色质构象相关的重叠组成性功能,并且它们在精子发生中具有特定作用,涉及Ub介导的组蛋白降解。

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