Mechanism of DNA damage tolerance.

World journal of biological chemistry Pub Date : 2015-08-26 DOI:10.4331/wjbc.v6.i3.48

Xin Bi

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引用次数: 39

Abstract

DNA damage may compromise genome integrity and lead to cell death. Cells have evolved a variety of processes to respond to DNA damage including damage repair and tolerance mechanisms, as well as damage checkpoints. The DNA damage tolerance (DDT) pathway promotes the bypass of single-stranded DNA lesions encountered by DNA polymerases during DNA replication. This prevents the stalling of DNA replication. Two mechanistically distinct DDT branches have been characterized. One is translesion synthesis (TLS) in which a replicative DNA polymerase is temporarily replaced by a specialized TLS polymerase that has the ability to replicate across DNA lesions. TLS is mechanistically simple and straightforward, but it is intrinsically error-prone. The other is the error-free template switching (TS) mechanism in which the stalled nascent strand switches from the damaged template to the undamaged newly synthesized sister strand for extension past the lesion. Error-free TS is a complex but preferable process for bypassing DNA lesions. However, our current understanding of this pathway is sketchy. An increasing number of factors are being found to participate or regulate this important mechanism, which is the focus of this editorial.

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DNA损伤耐受机制。

DNA损伤可能损害基因组完整性并导致细胞死亡。细胞已经进化出多种过程来应对DNA损伤，包括损伤修复和耐受机制，以及损伤检查点。DNA损伤耐受(DDT)途径促进DNA聚合酶在DNA复制过程中绕过单链DNA损伤。这可以防止DNA复制的停滞。两个机械上不同的滴滴涕分支已被表征。一种是翻译合成(TLS)，其中复制性DNA聚合酶暂时被具有跨DNA损伤复制能力的特殊TLS聚合酶所取代。TLS在机制上是简单和直接的，但它本质上容易出错。另一种是无错误模板切换(TS)机制，在这种机制中，停滞的新生链从受损的模板切换到未受损的新合成的姊妹链，以延长通过病变。无差错TS是一种复杂但优选的绕过DNA病变的方法。然而，我们目前对这一途径的理解是粗略的。越来越多的因素正在被发现参与或调节这一重要机制，这是本文的重点。

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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World journal of biological chemistry

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