Endogenous base damage as a driver of genomic instability in homologous recombination-deficient cancers

IF 3 3区 生物学 Q2 GENETICS & HEREDITY
Lindsey N. Aubuchon , Priyanka Verma
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引用次数: 0

Abstract

Homologous recombination (HR) is a high-fidelity DNA double-strand break (DSB) repair pathway. Both familial and somatic loss of function mutation(s) in various HR genes predispose to a variety of cancer types, underscoring the importance of error-free repair of DSBs in human physiology. While environmental sources of DSBs have been known, more recent studies have begun to uncover the role of endogenous base damage in leading to these breaks. Base damage repair intermediates often consist of single-strand breaks, which if left unrepaired, can lead to DSBs as the replication fork encounters these lesions. This review summarizes various sources of endogenous base damage and how these lesions are repaired. We highlight how conversion of base repair intermediates, particularly those with 5′or 3′ blocked ends, to DSBs can be a predominant source of genomic instability in HR-deficient cancers. We also discuss how endogenous base damage and ensuing DSBs can be exploited to enhance the efficacy of Poly (ADP-ribose) polymerase inhibitors (PARPi), that are widely used in the clinics for the regimen of HR-deficient cancers.

内源性碱基损伤是同源重组缺陷型癌症基因组不稳定的驱动因素。
同源重组(HR)是一种高保真 DNA 双链断裂(DSB)修复途径。各种 HR 基因的家族性和体细胞功能缺失突变易导致多种类型的癌症,凸显了 DSB 的无差错修复在人类生理学中的重要性。虽然人们已经知道 DSB 的环境来源,但最近的研究已开始揭示内源性碱基损伤在导致这些断裂中的作用。碱基损伤修复中间体通常由单链断裂组成,如果不对其进行修复,当复制叉遇到这些病变时就会导致 DSB。本综述总结了内源性碱基损伤的各种来源以及这些损伤是如何修复的。我们强调了碱基修复中间体,尤其是那些5'或3'末端被阻断的中间体,如何转化为DSB,成为HR缺陷癌症基因组不稳定的主要来源。我们还讨论了如何利用内源性碱基损伤和随之而来的 DSB 来提高聚(ADP-核糖)聚合酶抑制剂(PARPi)的疗效,这种抑制剂在临床上被广泛用于治疗 HR 缺陷型癌症。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
DNA Repair
DNA Repair 生物-毒理学
CiteScore
7.60
自引率
5.30%
发文量
91
审稿时长
59 days
期刊介绍: DNA Repair provides a forum for the comprehensive coverage of DNA repair and cellular responses to DNA damage. The journal publishes original observations on genetic, cellular, biochemical, structural and molecular aspects of DNA repair, mutagenesis, cell cycle regulation, apoptosis and other biological responses in cells exposed to genomic insult, as well as their relationship to human disease. DNA Repair publishes full-length research articles, brief reports on research, and reviews. The journal welcomes articles describing databases, methods and new technologies supporting research on DNA repair and responses to DNA damage. Letters to the Editor, hot topics and classics in DNA repair, historical reflections, book reviews and meeting reports also will be considered for publication.
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