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真核生物中聚集性 DNA 损伤修复:与突变和细胞存活的相关性。

Clustered DNA lesion repair in eukaryotes: relevance to mutagenesis and cell survival.

机构信息

Institut Curie, Bât. 110, Centre Universitaire, 91405 Orsay, France.

出版信息

Mutat Res. 2011 Jun 3;711(1-2):123-33. doi: 10.1016/j.mrfmmm.2010.12.010. Epub 2010 Dec 24.

Abstract

A clustered DNA lesion, also known as a multiply damaged site, is defined as ≥ 2 damages in the DNA within 1-2 helical turns. Only ionizing radiation and certain chemicals introduce DNA damage in the genome in this non-random way. What is now clear is that the lethality of a damaging agent is not just related to the types of DNA lesions introduced, but also to how the damage is distributed in the DNA. Clustered DNA lesions were first hypothesized to exist in the 1990s, and work has progressed where these complex lesions have been characterized and measured in irradiated as well as in non-irradiated cells. A clustered lesion can consist of single as well as double strand breaks, base damage and abasic sites, and the damages can be situated on the same strand or opposing strands. They include tandem lesions, double strand break (DSB) clusters and non-DSB clusters, and base excision repair as well as the DSB repair pathways can be required to remove these complex lesions. Due to the plethora of oxidative damage induced by ionizing radiation, and the repair proteins involved in their removal from the DNA, it has been necessary to study how repair systems handle these lesions using synthetic DNA damage. This review focuses on the repair process and mutagenic consequences of clustered lesions in yeast and mammalian cells. By examining the studies on synthetic clustered lesions, and the effects of low vs high LET radiation on mammalian cells or tissues, it is possible to extrapolate the potential biological relevance of these clustered lesions to the killing of tumor cells by radiotherapy and chemotherapy, and to the risk of cancer in non-tumor cells, and this will be discussed.

摘要

一个簇状 DNA 损伤,也称为多处损伤部位,定义为在 1-2 个螺旋圈的 DNA 内有≥2 处损伤。只有电离辐射和某些化学物质以这种非随机的方式在基因组中引入 DNA 损伤。现在清楚的是,一种损伤剂的致死性不仅与引入的 DNA 损伤类型有关,还与损伤在 DNA 中的分布方式有关。簇状 DNA 损伤最初是在 20 世纪 90 年代假设存在的,并且已经在辐照和未辐照的细胞中对这些复杂损伤进行了特征描述和测量。一个簇状损伤可以由单链和双链断裂、碱基损伤和无碱基位点组成,并且损伤可以位于同一链或相反链上。它们包括串联损伤、双链断裂(DSB)簇和非 DSB 簇,碱基切除修复以及 DSB 修复途径都可能需要去除这些复杂损伤。由于电离辐射诱导的大量氧化损伤,以及涉及从 DNA 中去除这些损伤的修复蛋白,因此有必要使用合成 DNA 损伤来研究修复系统如何处理这些损伤。本综述重点介绍了酵母和哺乳动物细胞中簇状损伤的修复过程和诱变后果。通过检查合成簇状损伤的研究,以及低 LET 与高 LET 辐射对哺乳动物细胞或组织的影响,可以推断出这些簇状损伤对放射治疗和化学疗法杀死肿瘤细胞的潜在生物学相关性,以及对非肿瘤细胞癌症风险的相关性,这将在本文中进行讨论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ae60/3101299/ecece80eb3b6/nihms267108f1.jpg

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