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Mammalian DNA ligases; roles in maintaining genome integrity

DNA连接酶 dna连接酶 DNA修复 生物 DNA钳 DNA修复蛋白XRCC4 DNA复制 核苷酸切除修复 DNA去甲基化 体外重组 DNA聚合酶mu DNA DDB1型 分子生物学 泛素连接酶 生物化学 细菌圆形染色体 泛素 DNA甲基化 基因 分子克隆 互补DNA 核糖核酸 基因表达 逆转录酶
作者
Annahita Sallmyr,Seema Khattri Bhandari,Tasmin Naila,Alan E. Tomkinson
出处
期刊:Journal of Molecular Biology [Elsevier]
卷期号:: 168276-168276
标识
DOI:10.1016/j.jmb.2023.168276
摘要

The joining of breaks in the DNA phosphodiester backbone is essential for genome integrity. Breaks are generated during normal processes such as DNA replication, cytosine demethylation during differentiation, gene rearrangement in the immune system and germ cell development. In addition, they are generated either directly by a DNA damaging agent or indirectly due to damage excision during repair. Breaks are joined by a DNA ligase that catalyzes phosphodiester bond formation at DNA nicks with 3’ hydroxyl and 5’ phosphate termini. Three human genes encode ATP-dependent DNA ligases. These enzymes have a conserved catalytic core consisting of three subdomains that encircle nicked duplex DNA during ligation. The DNA ligases are targeted to different nuclear DNA transactions by specific protein-protein interactions. Both DNA ligase IIIα and DNA ligase IV form stable complexes with DNA repair proteins, XRCC1 and XRCC4, respectively. There is functional redundancy between DNA ligase I and DNA ligase IIIα in DNA replication, excision repair and single-strand break repair. Although DNA ligase IV is a core component of the major double-strand break repair pathway, non-homologous end joining, the other enzymes participate in minor, alternative double-strand break repair pathways. In contrast to the nucleus, only DNA ligase IIIα is present in mitochondria and is essential for maintaining the mitochondrial genome. Human immunodeficiency syndromes caused by mutations in either LIG1 or LIG4 have been described. Preclinical studies with DNA ligase inhibitors have identified potentially targetable abnormalities in cancer cells and evidence that DNA ligases are potential targets for cancer therapy.

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