首页> 美国卫生研究院文献>The Journal of Veterinary Medical Science >Fluoroquinolone Resistance Mechanism of Clinical Isolates and SelectedMutants of Pasteurella multocida from Bovine Respiratory Disease inChina
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Fluoroquinolone Resistance Mechanism of Clinical Isolates and SelectedMutants of Pasteurella multocida from Bovine Respiratory Disease inChina

机译:临床分离株的氟喹诺酮耐药机制及选择牛呼吸道疾病多杀性巴氏杆菌的突变体。中国

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摘要

The minimum inhibitory concentrations (MICs), mutation prevention concentrations (MPCs) and contribution of quinolone resistance-determining region (QRDR) mutations to fluoroquinolone (ciprofloxacin, enrofloxacin and orbifloxacin) susceptibility in 23 Pasteurella multocida (Pm) isolates were investigated. Fluoroquinolone-susceptible isolates (MICs ≤0.25 µg/ml, 9 isolates) had no QRDR mutations, and their respective MPCs were low. Fluoroquinolone-intermediate isolates (MICs=0.5 µg/ml, 14 isolates) had QRDR mutations (Asp87 to Asn or Ala84 to Pro in gyrA), and their respective MPCs were high (4–32 µg/ml). First-step mutants (n=5) and laboratory-derived highly resistant fluoroquinolone mutants (n=5) also had QRDR mutations. The MICs of fluoroquinolones for mutant-derived strains were decreased in the presence of efflux inhibitors. The results indicated that the fluoroquinolone resistance of Pm is mainly due to multiple target gene mutations in gyrA and parC and the overexpression of efflux pump genes.
机译:研究了23种多杀巴斯德氏菌(Ps)菌株中的最小抑制浓度(MIC),预防突变浓度(MPC)和喹诺酮耐药性决定区域(QRDR)突变对氟喹诺酮(环丙沙星,恩诺沙星和奥比沙星)的敏感性。氟喹诺酮敏感性分离株(MIC≤0.25µg / ml,9个分离株)无QRDR突变,其各自的MPC较低。氟喹诺酮中间体分离株(MICs = 0.5 µg / ml,14个分离株)具有QRDR突变(gyrA中从Asp87到Asn或从Ala84到Pro),它们各自的MPCs高(4–32 µg / ml)。第一步突变体(n = 5)和实验室衍生的高抗性氟喹诺酮突变体(n = 5)也具有QRDR突变。在存在外排抑制剂的情况下,突变体菌株的氟喹诺酮类药物的MIC降低。结果表明,Pm对氟喹诺酮类药物的耐药性主要归因于gyrA和parC中的多个靶基因突变以及外排泵基因的过表达。

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