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Clinically relevant chromosomally encoded multidrug resistance efflux pumps in bacteria.细菌中具有临床相关性的染色体编码多药耐药外排泵
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猪布鲁氏菌中两个介导抗菌抗性的RND系统之间的相互作用

Interplay between two RND systems mediating antimicrobial resistance in Brucella suis.

作者信息

Martin Fernando A, Posadas Diana M, Carrica Mariela C, Cravero Silvio L, O'Callaghan David, Zorreguieta Angeles

机构信息

Fundación Instituto Leloir, IIBBA CONICET and FCEyN, Universidad de Buenos Aires, Patricias Argentinas 435, (C1405BWE) Buenos Aires, Argentina.

出版信息

J Bacteriol. 2009 Apr;191(8):2530-40. doi: 10.1128/JB.01198-08. Epub 2009 Feb 6.

DOI:10.1128/JB.01198-08
PMID:19201794
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2668434/
Abstract

The RND-type efflux pumps are responsible for the multidrug resistance phenotype observed in many clinically relevant species. Also, RND pumps have been implicated in physiological processes, with roles in the virulence mechanisms of several pathogenic bacteria. We have previously shown that the BepC outer membrane factor of Brucella suis is involved in the efflux of diverse drugs, probably as part of a tripartite complex with an inner membrane translocase. In the present work, we characterize two membrane fusion protein-RND translocases of B. suis encoded by the bepDE and bepFG loci. MIC assays showed that the B. suis DeltabepE mutant was more sensitive to deoxycholate (DOC), ethidium bromide, and crystal violet. Furthermore, multicopy bepDE increased resistance to DOC and crystal violet and also to other drugs, including ampicillin, norfloxacin, ciprofloxacin, tetracycline, and doxycycline. In contrast to the DeltabepE mutant, the resistance profile of B. suis remained unaltered when the other RND gene (bepG) was deleted. However, the DeltabepE DeltabepG double mutant showed a more severe phenotype than the DeltabepE mutant, indicating that BepFG also contributes to drug resistance. An open reading frame (bepR) coding for a putative regulatory protein of the TetR family was found upstream of the bepDE locus. BepR strongly repressed the activity of the bepDE promoter, but DOC released the repression mediated by BepR. A clear induction of the bepFG promoter activity was observed only in the BepDE-defective mutant, indicating a regulatory interplay between the two RND efflux pumps. Although only the BepFG-defective mutant showed a moderate attenuation in model cells, the activities of both bepDE and bepFG promoters were induced in the intracellular environment of HeLa cells. Our results show that B. suis harbors two functional RND efflux pumps that may contribute to virulence.

摘要

RND型外排泵与许多临床相关菌种中观察到的多药耐药表型有关。此外,RND泵还参与生理过程,在几种病原菌的毒力机制中发挥作用。我们之前已经表明,猪布鲁氏菌的BepC外膜因子参与多种药物的外排,可能是与内膜转运酶形成三方复合物的一部分。在本研究中,我们对由bepDE和bepFG基因座编码的猪布鲁氏菌的两种膜融合蛋白-RND转运酶进行了表征。最低抑菌浓度(MIC)测定表明,猪布鲁氏菌DeltabepE突变体对脱氧胆酸盐(DOC)、溴化乙锭和结晶紫更敏感。此外,多拷贝的bepDE增加了对DOC、结晶紫以及其他药物(包括氨苄青霉素、诺氟沙星、环丙沙星、四环素和强力霉素)的耐药性。与DeltabepE突变体不同,当另一个RND基因(bepG)缺失时,猪布鲁氏菌的耐药谱保持不变。然而,DeltabepE DeltabepG双突变体表现出比DeltabepE突变体更严重的表型,表明BepFG也有助于耐药性。在bepDE基因座上游发现了一个编码假定的TetR家族调节蛋白的开放阅读框(bepR)。BepR强烈抑制bepDE启动子的活性,但DOC解除了BepR介导的抑制作用。仅在BepDE缺陷型突变体中观察到bepFG启动子活性的明显诱导,表明两个RND外排泵之间存在调节相互作用。虽然只有BepFG缺陷型突变体在模型细胞中表现出中度减毒,但bepDE和bepFG启动子的活性在HeLa细胞的细胞内环境中均被诱导。我们的结果表明,猪布鲁氏菌含有两个功能性RND外排泵,可能有助于其毒力。