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探测聚合酶θ解旋酶样结构域的结构与功能。

Probing the structure and function of polymerase θ helicase-like domain.

机构信息

Department of Microbiology and Molecular Genetics, University of Vermont, 89 Beaumont Ave, Burlington, VT 05405, USA.

Department of Epigenetics & Molecular Carcinogenesis, The University of Texas MD Anderson Center, Houston, TX 77230, USA.

出版信息

DNA Repair (Amst). 2022 Aug;116:103358. doi: 10.1016/j.dnarep.2022.103358. Epub 2022 Jun 14.

Abstract

DNA Polymerase θ is the key actuator of the recently identified double-strand break repair pathway, theta-mediated end joining (TMEJ). It is the only known polymerase to have a 3-domain architecture containing an independently functional family A DNA polymerase tethered by a long central region to an N-terminal helicase-like domain (HLD). Full-length polymerase θ and the isolated HLD hydrolyze ATP in the presence of DNA, but no processive DNA duplex unwinding has been observed. Based on sequence and structure conservation, the HLD is classified as a member of helicase superfamily II and, more specifically, the Ski2-like family. The specific subdomain composition and organization most closely resemble that of archaeal DNA repair helicases Hel308 and Hjm. The underlying structural basis as to why the HLD is not able to processively unwind duplex DNA, despite its similarity to bona fide helicases, remains elusive. Activities of the HLD include ATP hydrolysis, protein displacement, and annealing of complementary DNA. These observations have led to speculation about the role of the HLD within the context of double-strand break repair via TMEJ, such as removal of single-stranded DNA binding proteins like RPA and RAD51 and microhomology alignment. This review summarizes the structural classification and organization of the polymerase θ HLD and its homologs and explores emerging data on its biochemical activities. We conclude with a simple, speculative model for the HLD's role in TMEJ.

摘要

DNA 聚合酶θ是最近发现的双链断裂修复途径——θ介导的末端连接(TMEJ)的关键执行者。它是唯一已知的具有 3 个结构域的聚合酶,包含一个独立功能的家族 A DNA 聚合酶,通过一个长的中心区域与 N 端的解旋酶样结构域(HLD)相连。全长聚合酶θ和分离的 HLD 在 DNA 存在的情况下水解 ATP,但没有观察到连续的 DNA 双链解旋。根据序列和结构的保守性,HLD 被归类为 II 型超家族的解旋酶,更具体地说是 Ski2 样家族。HLD 的特定亚结构域组成和组织最类似于古细菌 DNA 修复解旋酶 Hel308 和 Hjm。尽管 HLD 与真正的解旋酶相似,但它为什么不能连续地解旋双链 DNA 的潜在结构基础仍然难以捉摸。HLD 的活性包括 ATP 水解、蛋白质位移和互补 DNA 的退火。这些观察结果导致人们推测 HLD 在通过 TMEJ 进行双链断裂修复中的作用,例如去除单链 DNA 结合蛋白如 RPA 和 RAD51 以及微同源性对齐。本综述总结了聚合酶θ HLD 及其同源物的结构分类和组织,并探讨了其生化活性的最新数据。我们以 HLD 在 TMEJ 中的作用的一个简单的、推测性的模型结束。

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Probing the structure and function of polymerase θ helicase-like domain.探测聚合酶θ解旋酶样结构域的结构与功能。
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Annu Rev Genet. 2022 Nov 30;56:207-228. doi: 10.1146/annurev-genet-072920-041046. Epub 2022 Aug 26.

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