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首页> 外文期刊>Frontiers in Microbiology >Characterization of Vibrio fluvialis qnrVC5 Gene in Native and Heterologous Hosts: Synergy of qnrVC5 with other Determinants in Conferring Quinolone Resistance
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Characterization of Vibrio fluvialis qnrVC5 Gene in Native and Heterologous Hosts: Synergy of qnrVC5 with other Determinants in Conferring Quinolone Resistance

机译:本地和异源宿主中<斜视> vibrio fluvialis QNRVC5 基因的表征:<斜体> QNRVC5 与其他决定因素的协同作用促进喹诺酮抗性

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摘要

Resistance of various pathogens toward quinolones has emerged as a serious threat to combat infections. Analysis of plethora of genes and resistance mechanisms associated with quinolone resistance reveals chromosome-borne and transferable determinants. qnr genes have been found to be responsible for transferable quinolone resistance. In the present work, a new allele qnrVC5 earlier reported in Vibrio fluvialis from this laboratory was characterized in detail for its sequence, genetic context and propensity to decrease the susceptibility for quinolones. The study has revealed persistence of qnrVC5 in clinical isolates of V. fluvialis from Kolkata region through the years 2002–2006. qnrVC5 existed in the form of a gene cassette with the open reading frame being flanked by an upstream promoter and a downstream V. cholerae repeat region suggestive of its superintegron origin. Sequence analysis of different qnrVC alleles showed that qnrVC5 was closely related to qnrVC2 and qnrVC4 and these alleles were associated with V. cholerae repeats. In contrast, qnrVC1, qnrVC3 , and qnrVC6 belonging to another group were associated with V. parahaemolyticus repeats. The gene manifested its activity in native V. fluvialis host as well as in Escherichia coli transformants harboring it by elevating the MIC toward various quinolones by twofold to eightfold. In combination with other quinolone resistance factors such as topoisomerase mutations and aac(6’)-Ib-cr gene, qnrVC5 gene product contributed toward higher quinolone resistance displayed by V. fluvialis isolates. Silencing of the gene using antisense peptide nucleic acid sensitized the V. fluvialis parent isolates toward ciprofloxacin. Recombinant QnrVC5 vividly demonstrated its role in conferring quinolone resistance. qnrVC5 gene, its synergistic effect and global dissemination should be perceived as a menace for quinolone-based therapies.
机译:各种病原体对喹诺酮的抵抗力被出现为对抗感染的严重威胁。与喹啉抗性相关的基因和抗性机​​制的分析显示染色体传播和可转移的决定簇。已发现QNR基因负责可转移的喹啉抗性。在目前的工作中,早些时候在来自该实验室的Vibrio Flyvialis中报道的新的等位基因QNRVC5的特征在于其序列,遗传背景和降低喹诺酮类敏感性的倾向。该研究透露了2002 - 2006年从加尔各答区的V.Fluvialis的临床分离株QNRVC5持续存在。 QNRVC5以基因盒的形式存在,具有上游启动子的开放读数框架和下游V.霍乱重复区域暗示其SuperIntegon起源。不同QNRVC等位基因的序列分析表明,QNRVC5与QNRVC2和QNRVC4密切相关,这些等位基因与V.霍乱重复相关。相反,属于另一组的QNRVC1,QNRVC3和QNRVC6与V. parahaemolyticus重复相关。该基因表现出其在天然V.Filvialis宿主中的活性以及通过双重升高到八十倍以通过将麦克风升高到各种喹诺酮来讨论它的大肠杆菌转化体。与其他喹啉酶突变和AAC(6') - IB-CR基因的其他喹啉抗性因子组合,QNRVC5基因产物有助于V.Fluvialis分离株显示的喹耳酮抗性。使用反义肽核酸沉默基因敏化V. flyvialis母体分离物朝向环丙沙星。重组QNRVC5生动地证明其在赋予喹诺酮抗性的作用。 QNRVC5基因,其协同效应和全球传播应被视为喹诺酮类疗法的威胁。

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