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Endogenous DNA Double-Strand Breaks during DNA Transactions: Emerging Insights and Methods for Genome-Wide Profiling

机译:DNA交易过程中的内源性DNA双链断裂:全基因组分析的新兴见解和方法

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摘要

DNA double-strand breaks (DSBs) jeopardize genome integrity and can—when repaired unfaithfully—give rise to structural rearrangements associated with cancer. Exogenous agents such as ionizing radiation or chemotherapy can invoke DSBs, but a vast amount of breakage arises during vital endogenous DNA transactions, such as replication and transcription. Additionally, chromatin looping involved in 3D genome organization and gene regulation is increasingly recognized as a possible contributor to DSB events. In this review, we first discuss insights into the mechanisms of endogenous DSB formation, showcasing the trade-off between essential DNA transactions and the intrinsic challenges that these processes impose on genomic integrity. In the second part, we highlight emerging methods for genome-wide profiling of DSBs, and discuss future directions of research that will help advance our understanding of genome-wide DSB formation and repair.
机译:DNA双链断裂(DSB)危及基因组的完整性,如果不忠实地进行修复,可能会导致与癌症相关的结构重排。外源性试剂(例如电离辐射或化学疗法)可以调用DSB,但在重要的内源性DNA交易(例如复制和转录)过程中会发生大量破坏。另外,越来越多地认识到涉及3D基因组组织和基因调控的染色质环化可能是DSB事件的可能原因。在这篇综述中,我们首先讨论对内源性DSB形成机理的见解,展示必需的DNA交易与这些过程对基因组完整性造成的内在挑战之间的折衷。在第二部分中,我们重点介绍了用于全基因组DSB谱分析的新兴方法,并讨论了未来的研究方向,这将有助于增进我们对全基因组DSB形成和修复的理解。

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