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Optimizing therapy with antibacterial agents: use of pharmacokinetic-pharmacodynamic principles in pediatrics.

机译:使用抗菌药物优化治疗:在儿科中使用药代动力学-药效学原理。

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摘要

The appropriate dosage of antibacterial agents is essential in achieving both clinical and microbiologic success in the treatment of infections in children. By using in vitro experimental data and animal model outcome data, the pharmacokinetic-pharmacodynamic (PK-PD) parameters predictive of antibacterial effect have been elucidated. For time-dependent drugs such as beta-lactams, the PK-PD parameter of interest is the percentage of time in a dosage interval for which drug concentrations remain above the minimum inhibitory concentration (MIC) of the infecting organism. For concentration-dependent drugs such as aminoglycosides, the PK-PD parameter of interest is the ratio of the area under the plasma concentration-time curve to the MIC. Recent studies using data on clinical and microbiologic outcomes from infected adults and children, combined with data on drug exposure, have confirmed the importance of these parameters and provided estimates of the PK-PD goals of therapy for various antibacterial agents. Application of these PK-PD principles allows rational dosage regimen selection, both for serious infections in critically ill children and for non-life-threatening community-acquired infections.
机译:适当剂量的抗菌剂对于在治疗儿童感染方面取得临床和微生物学成功均至关重要。通过使用体外实验数据和动物模型结果数据,已阐明了预测抗菌作用的药代动力学-药效学(PK-PD)参数。对于时间依赖性药物(例如β-内酰胺类),感兴趣的PK-PD参数是剂量间隔中药物浓度保持在感染生物体最低抑制浓度(MIC)以上的时间百分比。对于浓度依赖性药物(例如氨基糖苷),感兴趣的PK-PD参数是血浆浓度-时间曲线下面积与MIC的比值。最近的研究使用了来自受感染的成人和儿童的临床和微生物结局数据,以及有关药物暴露的数据,证实了这些参数的重要性,并提供了各种抗菌药物治疗的PK-PD目标的估计值。这些PK-PD原理的应用允许合理选择剂量方案,既可以用于重症儿童的严重感染,也可以用于非危及生命的社区获得性感染。

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