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形成和修复源于常见内源性损伤的链间 DNA 交联。

Formation and Repair of an Interstrand DNA Cross-Link Arising from a Common Endogenous Lesion.

机构信息

University of Missouri Department of Chemistry 125 Chemistry Building Columbia, Missouri 65211, United States.

Department of Chemistry University of California-Riverside Riverside, California 92521-0403, United States.

出版信息

J Am Chem Soc. 2021 Sep 22;143(37):15344-15357. doi: 10.1021/jacs.1c06926. Epub 2021 Sep 13.

Abstract

Interstrand DNA cross-links (ICLs) are cytotoxic because they block the strand separation required for read-out and replication of the genetic information in duplex DNA. The unavoidable formation of ICLs in cellular DNA may contribute to aging, neurodegeneration, and cancer. Here, we describe the formation and properties of a structurally complex ICL derived from an apurinic/apyrimidinic (AP) site, which is one of the most common endogenous lesions in cellular DNA. The results characterize a cross-link arising from aza-Michael addition of the -amino group of a guanine residue to the electrophilic sugar remnant generated by spermine-mediated strand cleavage at an AP site in duplex DNA. An α,β-unsaturated iminium ion is the critical intermediate involved in ICL formation. Studies employing the bacteriophage φ29 polymerase provided evidence that this ICL can block critical DNA transactions that require strand separation. The results of biochemical studies suggest that this complex strand break/ICL might be repaired by a simple mechanism in which the 3'-exonuclease action of the enzyme apurinic/apyrimidinic endonuclease (APE1) unhooks the cross-link to initiate repair via the single-strand break repair pathway.

摘要

链间 DNA 交联(ICLs)是细胞毒性的,因为它们阻止了双链 DNA 中遗传信息读取和复制所需的链分离。细胞 DNA 中不可避免地形成 ICL 可能导致衰老、神经退行性变和癌症。在这里,我们描述了一种源自无嘌呤/无嘧啶(AP)位点的结构复杂的 ICL 的形成和特性,AP 位点是细胞 DNA 中最常见的内源性损伤之一。结果表征了一种交联,它是由腺嘌呤残基的 -氨基与 spermine 介导的双链 DNA 中 AP 位点处的糖残基产生的亲电物质发生氮杂迈克尔加成反应而形成的。α,β-不饱和亚氨基离子是形成 ICL 所涉及的关键中间体。噬菌体 φ29 聚合酶的研究提供了证据,证明这种 ICL 可以阻止需要链分离的关键 DNA 交易。生化研究的结果表明,这种复杂的链断裂/ICL 可能通过一种简单的机制进行修复,其中酶脱嘌呤/嘧啶内切核酸酶 1(APE1)的 3'-核酸外切酶作用将交联物解开,通过单链断裂修复途径开始修复。

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