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抗菌药物药代动力学参数与动物模型治疗效果的相关性。

Correlation of antimicrobial pharmacokinetic parameters with therapeutic efficacy in an animal model.

作者信息

Vogelman B, Gudmundsson S, Leggett J, Turnidge J, Ebert S, Craig W A

机构信息

Medical Service, William S. Middleton Memorial Veterans Hospital, Madison, Wisconsin 53705.

出版信息

J Infect Dis. 1988 Oct;158(4):831-47. doi: 10.1093/infdis/158.4.831.

Abstract

Current antimicrobial dosing regimens are designed to maintain active drug levels for most of the dosing interval and are based on 40-y-old observations. With use of numerous multiple-dosing regimens in an animal model, this study is the first to successfully minimize the interdependence between pharmacokinetic parameters and thereby determine, by stepwise multivariate regression analysis, that the time that serum levels exceeded the minimum inhibitory concentration (MIC) was the most significant parameter determining efficacy for beta-lactams and erythromycin against various pathogens, whereas the log area under the curve was the major parameter for aminoglycosides. Optimal dosing intervals were no greater than the time that serum levels exceeded the MIC plus the duration of the postantibiotic effect. Careful application of these concepts should allow other investigators to use more optimally dosed regimens than those previously used in preclinical trials and to design studies to improve on current dosing regimens for humans.

摘要

当前的抗菌药物给药方案旨在使大部分给药间隔内药物保持有效水平,且基于40年前的观察结果。在动物模型中使用多种多剂量给药方案后,本研究首次成功地将药代动力学参数之间的相互依赖性降至最低,从而通过逐步多元回归分析确定,血清水平超过最低抑菌浓度(MIC)的时间是β-内酰胺类药物和红霉素针对各种病原体的疗效的最显著决定参数,而曲线下面积对数是氨基糖苷类药物的主要参数。最佳给药间隔不超过血清水平超过MIC的时间加上抗生素后效应的持续时间。谨慎应用这些概念应能使其他研究人员采用比先前在临床前试验中使用的方案更优化的给药方案,并设计研究以改进当前的人类给药方案。

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