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淋病奈瑟菌核苷酸切除修复系统的遗传特征。

Genetic characterization of the nucleotide excision repair system of Neisseria gonorrhoeae.

机构信息

Department of Microbiology-Immunology, Northwestern University Feinberg School of Medicine, Chicago, IL 60611, USA.

出版信息

J Bacteriol. 2010 Feb;192(3):665-73. doi: 10.1128/JB.01018-09. Epub 2009 Nov 20.

Abstract

Nucleotide excision repair (NER) is universally used to recognize and remove many types of DNA damage. In eubacteria, the NER system typically consists of UvrA, UvrB, UvrC, the UvrD helicase, DNA polymerase I, and ligase. In addition, when DNA damage blocks transcription, transcription-repair coupling factor (TRCF), the product of the mfd gene, recruits the Uvr complex to repair the damage. Previous work using selected mutants and assays have indicated that pathogenic Neisseria spp. carry a functional NER system. In order to comprehensively examine the role of NER in Neisseria gonorrhoeae DNA recombination and repair processes, the predicted NER genes (uvrA, uvrB, uvrC, uvrD, and mfd) were each disrupted by a transposon insertion, and the uvrB and uvrD mutants were complemented with a copy of each gene in an ectopic locus. Each uvr mutant strain was highly sensitive to UV irradiation and also showed sensitivity to hydrogen peroxide killing, confirming that all of the NER genes in N. gonorrhoeae are functional. The effect of RecA expression on UV survival was minor in uvr mutants but much larger in the mfd mutant. All of the NER mutants demonstrated wild-type levels of pilin antigenic variation and DNA transformation. However, the uvrD mutant exhibited higher frequencies of PilC-mediated pilus phase variation and spontaneous mutation, a finding consistent with a role for UvrD in mismatch repair. We conclude that NER functions are conserved in N. gonorrhoeae and are important for the DNA repair capabilities of this strict human pathogen.

摘要

核苷酸切除修复 (NER) 是普遍用于识别和去除多种类型的 DNA 损伤的方法。在真细菌中,NER 系统通常由 UvrA、UvrB、UvrC、UvrD 解旋酶、DNA 聚合酶 I 和连接酶组成。此外,当 DNA 损伤阻断转录时,转录修复偶联因子 (TRCF),即 mfd 基因的产物,会招募 Uvr 复合物来修复损伤。以前使用选择性突变体和测定法的工作表明,致病性奈瑟氏菌属携带功能正常的 NER 系统。为了全面研究 NER 在淋病奈瑟氏菌 DNA 重组和修复过程中的作用,预测的 NER 基因 (uvrA、uvrB、uvrC、uvrD 和 mfd) 均通过转座子插入而被破坏,并且 uvrB 和 uvrD 突变体用每个基因的一个拷贝在异位基因座进行了互补。每个 uvr 突变菌株对 UV 照射高度敏感,并且对过氧化氢杀伤也敏感,这证实了淋病奈瑟氏菌中的所有 NER 基因都是功能正常的。RecA 表达对 uvr 突变体中 UV 生存的影响较小,但对 mfd 突变体的影响要大得多。所有的 NER 突变体均表现出野生型的菌毛抗原变异和 DNA 转化水平。然而,uvrD 突变体表现出更高频率的 PilC 介导的菌毛相变异和自发突变,这一发现与 UvrD 在错配修复中的作用一致。我们得出结论,NER 功能在淋病奈瑟氏菌中是保守的,并且对这种严格的人体病原体的 DNA 修复能力很重要。

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