首页> 外文期刊>Journal of Medical Microbiology: An Official Journal of the Pathological Society of Great Britain and Ireland >Effect of 1-(1-naphthylmethyl)-piperazine on antimicrobial agent susceptibility in multidrug-resistant isogenic and veterinary Escherichia coli field strains
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Effect of 1-(1-naphthylmethyl)-piperazine on antimicrobial agent susceptibility in multidrug-resistant isogenic and veterinary Escherichia coli field strains

机译:1-(1-萘甲基)-哌嗪对多药耐药的同基因和兽医大肠杆菌菌株中抗菌剂敏感性的影响

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The objective of this study was to evaluate the interaction of the efflux pump inhibitor 1-(1-naphthylmethyl)-piperazine (NMP) when combined with different families of antimicrobial agents against isogenic strains and multidrug-resistant (MDR) Escherichia coli field strains isolated from animals. Laboratory isogenic strains of E. coli with different levels of expression of efflux pumps were used as quality controls. Ten MDR E. coli strains were collected from healthy animals in a cross-sectional study in four commercial dairy farms. The MICs of florfenicol, ciprofloxacin, tetracycline and ampicillin were determined by a serial microdilution method in Luria–Bertani broth in the presence or absence of NMP. NMP used with ampicillin exerted no effect on the isogenic or field strains. In most of the field MDRE. coli strains and in an acrAB-overexpressing (AG112) isogenic strain, the MICs of florfenicol, ciprofloxacin and tetracycline decreased at least fourfold when the antimicrobial was combined with the highest NMP concentrations. In the wild-type strain (AG100), there were no decreases of more than twice the MIC, whilst in strain AG100A, an efflux pump-deficient strain, the MIC did not change, regardless of the concentration of NMP used with these three antimicrobials. Thus, ampicillin was not affected by the efflux pump mechanism, whereas ciprofloxacin, tetracycline and florfenicol were shown to be substrates of efflux pumps, with a consequent significant reduction in MICs. Resistance could not be completely reversed in the E. coli field strains by NMP, probably because other resistance mechanisms were also present. However, in strain AG112, the MIC results demonstrated that NMP expressed an important synergistic activity with florfenicol. The reduction in florfenicol MIC value was sufficient to reverse antimicrobial resistance completely for AG112.
机译:这项研究的目的是评估外排泵抑制剂1-(1-萘甲基)-哌嗪(NMP)与不同家族的抗同种菌株和耐多药(MDR)大肠杆菌田间菌株结合使用时的相互作用来自动物。将具有不同水平外排泵表达水平的大肠杆菌实验室同基因菌株用作质量控制。在四个商业奶牛场的横断面研究中,从健康动物中收集了十种MDR大肠杆菌菌株。在存在或不存在NMP的情况下,通过连续微量稀释法在Luria-Bertani肉汤中测定氟苯尼考,环丙沙星,四环素和氨苄青霉素的MIC。与氨苄青霉素一起使用的NMP对等基因或野外菌株没有影响。在大多数领域,MDRE。大肠杆菌菌株和acrAB过表达(AG112)等基因菌株中,当抗菌药物与最高NMP浓度组合使用时,氟苯尼考,环丙沙星和四环素的MIC降低至少四倍。在野生型菌株(AG100)中,MIC的降低没有超过两倍,而在外排泵缺陷型菌株AG100A中,MIC不变,而与这三种抗微生物剂使用的NMP的浓度无关。因此,氨苄西林不受外排泵机制的影响,而环丙沙星,四环素和氟苯尼考被证明是外排泵的底物,因此MIC显着降低。 NMP无法在大肠杆菌田间菌株中完全逆转耐药性,这可能是因为还存在其他耐药机制。然而,在菌株AG112中,MIC结果表明NMP与氟苯尼考具有重要的协同作用。氟苯尼考MIC值的降低足以完全逆转AG112的抗药性。

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