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DNA 修复和去甲基化因子胸腺嘧啶 DNA 糖基化酶可逆地使染色质浓缩。

Reversible chromatin condensation by the DNA repair and demethylation factor thymine DNA glycosylase.

机构信息

Department of Chemistry, Texas A&M University, College Station, TX 77843, USA.

出版信息

Nucleic Acids Res. 2021 Mar 18;49(5):2450-2459. doi: 10.1093/nar/gkab040.

Abstract

Chromatin structures (and modulators thereof) play a central role in genome organization and function. Herein, we report that thymine DNA glycosylase (TDG), an essential enzyme involved in DNA repair and demethylation, has the capacity to alter chromatin structure directly through its physical interactions with DNA. Using chemically defined nucleosome arrays, we demonstrate that TDG induces decompaction of individual chromatin fibers upon binding and promotes self-association of nucleosome arrays into higher-order oligomeric structures (i.e. condensation). Chromatin condensation is mediated by TDG's disordered polycationic N-terminal domain, whereas its C-terminal domain antagonizes this process. Furthermore, we demonstrate that TDG-mediated chromatin condensation is reversible by growth arrest and DNA damage 45 alpha (GADD45a), implying that TDG cooperates with its binding partners to dynamically control chromatin architecture. Finally, we show that chromatin condensation by TDG is sensitive to the methylation status of the underlying DNA. This new paradigm for TDG has specific implications for associated processes, such as DNA repair, DNA demethylation, and transcription, and general implications for the role of DNA modification 'readers' in controlling chromatin organization.

摘要

染色质结构(及其调节剂)在基因组组织和功能中起着核心作用。在此,我们报告称,胸腺嘧啶 DNA 糖基化酶(TDG)是一种参与 DNA 修复和去甲基化的必需酶,它能够通过与 DNA 的物理相互作用直接改变染色质结构。我们使用化学定义的核小体阵列,证明 TDG 在结合后会导致单个染色质纤维解压缩,并促进核小体阵列自组装成更高阶的寡聚结构(即浓缩)。染色质浓缩是由 TDG 的无规多阳离子 N 端结构域介导的,而其 C 端结构域则拮抗该过程。此外,我们证明 TDG 介导的染色质浓缩可通过生长停滞和 DNA 损伤 45 阿尔法(GADD45a)逆转,这意味着 TDG 与其结合伙伴合作,以动态控制染色质结构。最后,我们表明 TDG 引起的染色质浓缩对基础 DNA 的甲基化状态敏感。这种 TDG 的新范式对相关过程具有特定意义,例如 DNA 修复、DNA 去甲基化和转录,并且对 DNA 修饰“读取器”在控制染色质组织中的作用具有普遍意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2549/7969020/98f37d328869/gkab040fig1.jpg

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