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专注于 DNA 糖基化酶——一组具有高潜力的受严格调控的酶,可作为抗癌药物靶点。

Focus on DNA Glycosylases-A Set of Tightly Regulated Enzymes with a High Potential as Anticancer Drug Targets.

机构信息

Institut de Biologie Structurale (IBS), University Grenoble Alpes, CEA, CNRS, F-38000 Grenoble, France.

出版信息

Int J Mol Sci. 2020 Dec 3;21(23):9226. doi: 10.3390/ijms21239226.

Abstract

Cancer is the second leading cause of death with tens of millions of people diagnosed with cancer every year around the world. Most radio- and chemotherapies aim to eliminate cancer cells, notably by causing severe damage to the DNA. However, efficient repair of such damage represents a common mechanism of resistance to initially effective cytotoxic agents. Thus, development of new generation anticancer drugs that target DNA repair pathways, and more particularly the base excision repair (BER) pathway that is responsible for removal of damaged bases, is of growing interest. The BER pathway is initiated by a set of enzymes known as DNA glycosylases. Unlike several downstream BER enzymes, DNA glycosylases have so far received little attention and the development of specific inhibitors of these enzymes has been lagging. Yet, dysregulation of DNA glycosylases is also known to play a central role in numerous cancers and at different stages of the disease, and thus inhibiting DNA glycosylases is now considered a valid strategy to eliminate cancer cells. This review provides a detailed overview of the activities of DNA glycosylases in normal and cancer cells, their modes of regulation, and their potential as anticancer drug targets.

摘要

癌症是全球每年导致数千万人被诊断出癌症的第二大死亡原因。大多数放化疗旨在消除癌细胞,特别是通过对 DNA 造成严重损伤。然而,这种损伤的有效修复是对最初有效的细胞毒性药物产生耐药性的常见机制。因此,开发靶向 DNA 修复途径的新一代抗癌药物,特别是负责清除受损碱基的碱基切除修复 (BER) 途径,越来越受到关注。BER 途径由一组称为 DNA 糖苷酶的酶启动。与几种下游 BER 酶不同,迄今为止,DNA 糖苷酶受到的关注较少,这些酶的特异性抑制剂的开发一直滞后。然而,DNA 糖苷酶的失调也已知在许多癌症中和疾病的不同阶段发挥核心作用,因此抑制 DNA 糖苷酶被认为是消除癌细胞的有效策略。本文综述了 DNA 糖苷酶在正常和癌细胞中的活性、调节方式及其作为抗癌药物靶点的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4509/7730500/2834817b6455/ijms-21-09226-g001.jpg

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