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解旋酶 HELQ:适合 DSB 修复功能的分子特征。

Helicase HELQ: Molecular Characters Fit for DSB Repair Function.

机构信息

Beijing Key Laboratory of DNA Damage Response, College of Life Sciences, Capital Normal University, Beijing 100048, China.

出版信息

Int J Mol Sci. 2024 Aug 8;25(16):8634. doi: 10.3390/ijms25168634.

Abstract

The protein sequence and spatial structure of DNA helicase HELQ are highly conserved, spanning from archaea to humans. Aside from its helicase activity, which is based on DNA binding and translocation, it has also been recently reconfirmed that human HELQ possesses DNA-strand-annealing activity, similar to that of the archaeal HELQ homolog StoHjm. These biochemical functions play an important role in regulating various double-strand break (DSB) repair pathways, as well as multiple steps in different DSB repair processes. HELQ primarily facilitates repair in end-resection-dependent DSB repair pathways, such as homologous recombination (HR), single-strand annealing (SSA), microhomology-mediated end joining (MMEJ), as well as the sub-pathways' synthesis-dependent strand annealing (SDSA) and break-induced replication (BIR) within HR. The biochemical functions of HELQ are significant in end resection and its downstream pathways, such as strand invasion, DNA synthesis, and gene conversion. Different biochemical activities are required to support DSB repair at various stages. This review focuses on the functional studies of the biochemical roles of HELQ during different stages of diverse DSB repair pathways.

摘要

DNA 解旋酶 HELQ 的蛋白序列和空间结构高度保守,从古菌到人都有。除了基于 DNA 结合和易位的解旋酶活性外,最近还重新证实人类 HELQ 具有与古菌 HELQ 同源物 StoHjm 相似的 DNA 链退火活性。这些生化功能在调节各种双链断裂 (DSB) 修复途径以及不同 DSB 修复过程中的多个步骤方面发挥着重要作用。HELQ 主要促进末端切除依赖性 DSB 修复途径的修复,如同源重组 (HR)、单链退火 (SSA)、微同源介导的末端连接 (MMEJ) 以及 HR 内的合成依赖性链退火 (SDSA) 和断裂诱导复制 (BIR) 亚途径。HELQ 在末端切除及其下游途径(如链入侵、DNA 合成和基因转换)中的生化功能非常重要。不同的生化活性需要在不同的 DSB 修复阶段提供支持。这篇综述重点介绍了 HELQ 在不同 DSB 修复途径的不同阶段的生化作用的功能研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a98/11355030/4fc6197eb86d/ijms-25-08634-g001.jpg

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