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Analysis of the Topology of Vibrio cholerae NorM and Identification of Amino Acid Residues Involved in Norfloxacin Resistance▿ †

机译:霍乱弧菌NorM的拓扑分析和涉及诺氟沙星耐药性的氨基酸残基的鉴定▿†

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摘要

NorM, a putative efflux pump of Vibrio cholerae, is a member of the multidrug and toxic compound extrusion family of transporters. We demonstrate that NorM confers resistance to norfloxacin, ciprofloxacin, and ethidium bromide. Inactivation of norM rendered V. cholerae hypersensitive towards these fluoroquinolones. Multiple sequence alignment of members of its family identified several regions of high sequence conservation. The topology of NorM was determined using β-lactamase and chloramphenicol acetyltransferase fusions. The amino acid residues G184, K185, G187, P189, E190, G192, and G195 in the periplasmic loops and L381, R382, G383, Y384, K385, and D386 in the cytoplasmic loops, as well as all the acidic and cysteine residues of NorM, were mutated. Mutants G184V, G184W, K185I, P189S, E190K, and E190A lost the norfloxacin resistance-imparting phenotype characteristic of NorM. Mutants E124V, D155V, G187V, G187R, C196S, Y384H, Y384S, and Y384F exhibited partial resistance to norfloxacin. Mutants with replacements of G184 or G187 by A, K185 by R, and E190 by D retained the norfloxacin resistance phenotype of NorM. Analysis of the accumulation of norfloxacin in intact cells of Escherichia coli expressing NorM or its mutants in the presence or absence of carbonyl cyanide m-chlorophenylhydrazone supported the results obtained through susceptibility testing and argued in favor of NorM-mediated efflux as the determining factor in norfloxacin susceptibility in the genetically manipulated strains. Taken together, these results suggested that E124, D155, G184, K185, G187, P189, E190, C196, and Y384 are likely involved in NorM-dependent norfloxacin efflux. Except for D155, C196, and Y384, all of these residues are located in periplasmic loops.
机译:NorM是霍乱弧菌的推定外排泵,是多种药物和有毒化合物挤出转运蛋白家族的成员。我们证明NorM赋予对诺氟沙星,环丙沙星和溴化乙锭的抗性。 norM的失活使霍乱弧菌对这些氟喹诺酮类药物过敏。其家族成员的多序列比对鉴定了高序列保守性的几个区域。 NorM的拓扑结构是使用β-内酰胺酶和氯霉素乙酰转移酶融合物确定的。周质环中的氨基酸残基G184,K185,G187,P189,E190,G192和G195以及细胞质环中的L381,R382,G383,Y384,K385和D386以及所有的酸性和半胱氨酸残基NorM,被突变。突变体G184V,G184W,K185I,P189S,E190K和E190A失去了NorM赋予诺氟沙星抗性的表型特征。突变体E124V,D155V,G187V,G187R,C196S,Y384H,Y384S和Y384F对诺氟沙星表现出部分抗性。用A替换G184或G187,用R替换K185和用D替换E190的突变体保留了NorM的诺氟沙星抗性表型。在存在或不存在羰基氰化物间氯苯hydr的情况下,对表达NorM或其突变体的大肠杆菌完整细胞中诺氟沙星的积累进行的分析支持通过药敏测试获得的结果,并主张采用NorM介导的流出作为诺氟沙星的决定因素转基因菌株的易感性。综上所述,这些结果表明,E124,D155,G184,K185,G187,P189,E190,C196和Y384可能与NorM依赖性诺氟沙星外排有关。除D155,C196和Y384外,所有这些残基均位于周质环中。

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