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Non-B DNA Secondary Structures and Their Resolution by RecQ Helicases

机译:非B DNA二级结构及其RecQ解旋酶的解析。

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摘要

In addition to the canonical B-form structure first described by Watson and Crick, DNA can adopt a number of alternative structures. These non-B-form DNA secondary structures form spontaneously on tracts of repeat sequences that are abundant in genomes. In addition, structured forms of DNA with intrastrand pairing may arise on single-stranded DNA produced transiently during various cellular processes. Such secondary structures have a range of biological functions but also induce genetic instability. Increasing evidence suggests that genomic instabilities induced by non-B DNA secondary structures result in predisposition to diseases. Secondary DNA structures also represent a new class of molecular targets for DNA-interactive compounds that might be useful for targeting telomeres and transcriptional control. The equilibrium between the duplex DNA and formation of multistranded non-B-form structures is partly dependent upon the helicases that unwind (resolve) these alternate DNA structures. With special focus on tetraplex, triplex, and cruciform, this paper summarizes the incidence of non-B DNA structures and their association with genomic instability and emphasizes the roles of RecQ-like DNA helicases in genome maintenance by resolution of DNA secondary structures. In future, RecQ helicases are anticipated to be additional molecular targets for cancer chemotherapeutics.
机译:除了Watson和Crick首先描述的规范B型结构外,DNA还可采用许多其他结构。这些非B型DNA二级结构是在基因组中丰富的重复序列片段上自发形成的。另外,在各种细胞过程中瞬时产生的单链DNA上可能会出现具有链内配对的结构化形式的DNA。这样的二级结构具有一定范围的生物学功能,但也引起遗传不稳定。越来越多的证据表明,由非B DNA二级结构诱导的基因组不稳定性会导致疾病易感性。二级DNA结构也代表了与DNA相互作用的化合物的新型分子靶标,可能对靶向端粒和转录控制有用。双链DNA与多链非B型结构形成之间的平衡部分取决于解旋(解析)这些替代DNA结构的解旋酶。本文特别关注四重体,三重体和十字形,总结了非B DNA结构的发生及其与基因组不稳定性的关系,并通过解析DNA二级结构强调了RecQ样DNA解旋酶在基因组维护中的作用。将来,RecQ解旋酶有望成为癌症化学治疗的其他分子靶标。

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