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Antimicrobial Susceptibility Breakpoints and First-Step parC Mutations in Streptococcus pneumoniae: Redefining Fluoroquinolone Resistance

机译:肺炎链球菌的抗生素敏感性起点和第一步parC突变:重新定义氟喹诺酮耐药性

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摘要

Clinical antimicrobial susceptibility breakpoints are used to predict the clinical outcome of antimicrobial treatment. In contrast, microbiologic breakpoints are used to identify isolates that may be categorized as susceptible when applying clinical breakpoints but harbor resistance mechanisms that result in their reduced susceptibility to the agent being tested. Currently, the National Committee for Clinical Laboratory Standards (NCCLS) guidelines utilize clinical breakpoints to characterize the activity of the fluoroquinolones against Streptococcus pneumoniae. To determine whether levofloxacin breakpoints can identify isolates that harbor recognized resistance mechanisms, we examined 115 S. pneumoniae isolates with a levofloxacin MIC of >2 μg/mL for first-step parC mutations. A total of 48 (59%) of 82 isolates with a levofloxacin MIC of 2 μg/mL, a level considered susceptible by NCCLS criteria, had a first-step mutation in parC. Whether surveillance programs that use levofloxacin data can effectively detect emerging resistance and whether fluoroquinolones can effectively treat infections caused by such isolates should be evaluated.
机译:临床抗菌药敏感性断点用于预测抗菌药治疗的临床结果。相比之下,微生物学断点用于鉴定在应用临床断点时可能被归类为易感菌株,但具有耐药机制,导致其对被测药物的敏感性降低。目前,美国国家临床实验室标准委员会(NCCLS)指南利用临床断点来表征氟喹诺酮类药物抗肺炎链球菌的活性。为了确定左氧氟沙星的断点是否可以鉴定出具有公认抗性机制的分离株,我们针对第一步parC突变检测了左氧氟沙星MIC> 2μg/ mL的115株肺炎链球菌。 82株分离出的左氧氟沙星MIC为2μg/ mL的菌落中有48株(59%)在parC中发生了第一步突变。应该评估使用左氧氟沙星数据的监视程序是否可以有效检测新出现的耐药性,以及氟喹诺酮类药物是否可以有效治疗此类分离物引起的感染。

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