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螺旋-发夹-螺旋DNA糖基化酶超家族的结构、功能与进化:拼凑DNA碱基损伤修复机制的进化谜题

Structure, function and evolution of the Helix-hairpin-Helix DNA glycosylase superfamily: Piecing together the evolutionary puzzle of DNA base damage repair mechanisms.

作者信息

Trasviña-Arenas C H, Demir Merve, Lin Wen-Jen, David Sheila S

机构信息

Department of Chemistry, University of California, Davis, CA 95616, U.S.A..

Department of Chemistry, University of California, Davis, CA 95616, U.S.A.

出版信息

DNA Repair (Amst). 2021 Dec;108:103231. doi: 10.1016/j.dnarep.2021.103231. Epub 2021 Sep 25.

Abstract

The Base Excision Repair (BER) pathway is a highly conserved DNA repair system targeting chemical base modifications that arise from oxidation, deamination and alkylation reactions. BER features lesion-specific DNA glycosylases (DGs) which recognize and excise modified or inappropriate DNA bases to produce apurinic/apyrimidinic (AP) sites and coordinate AP-site hand-off to subsequent BER pathway enzymes. The DG superfamilies identified have evolved independently to cope with a wide variety of nucleobase chemical modifications. Most DG superfamilies recognize a distinct set of structurally related lesions. In contrast, the Helix-hairpin-Helix (HhH) DG superfamily has the remarkable ability to act upon structurally diverse sets of base modifications. The versatility in substrate recognition of the HhH-DG superfamily has been shaped by motif and domain acquisitions during evolution. In this paper, we review the structural features and catalytic mechanisms of the HhH-DG superfamily and draw a hypothetical reconstruction of the evolutionary path where these DGs developed diverse and unique enzymatic features.

摘要

碱基切除修复(BER)途径是一种高度保守的DNA修复系统,针对由氧化、脱氨和烷基化反应产生的化学碱基修饰。BER的特点是具有损伤特异性的DNA糖基化酶(DGs),它们识别并切除修饰的或不适当的DNA碱基,产生无嘌呤/无嘧啶(AP)位点,并将AP位点传递给后续的BER途径酶。已鉴定的DG超家族独立进化,以应对多种核碱基化学修饰。大多数DG超家族识别一组独特的结构相关损伤。相比之下,螺旋-发夹-螺旋(HhH)DG超家族具有作用于结构多样的碱基修饰的显著能力。HhH-DG超家族在底物识别方面的多功能性是由进化过程中的基序和结构域获得所塑造的。在本文中,我们综述了HhH-DG超家族的结构特征和催化机制,并对这些DGs发展出多样且独特酶学特征的进化路径进行了假设性重构。

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