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Alteration of postantibiotic effect during one dosing interval of tobramycin simulated in an in vitro pharmacokinetic model.

机译:在体外药代动力学模型中模拟的妥​​布霉素一个给药间隔期间抗生素后效应的变化。

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摘要

The kinetics of the postantibiotic effect (PAE) during one dosing interval of tobramycin against Staphylococcus aureus and Pseudomonas aeruginosa was investigated. We determined the PAE at different time points during this dosing interval of 12 h in an in vitro pharmacokinetic model simulating human pharmacokinetics in which the half-life of tobramycin was adjusted to 2.4 +/- 0.2 h. Using an enzymatic method to inactivate tobramycin, we determined PAEs in samples extracted from the model at 1, 5, 8, and 12 h, corresponding with tobramycin concentrations of 20, 5, 2, and 1 times the MIC for the test organism. The PAE decreased significantly from 2.5 h at 1 h to 0 h at 12 h. No change in MIC was observed for the strains during the experiments. We conclude that the PAE decreases with decreasing tobramycin concentrations during a 12-h dosing interval and completely disappears after the concentration has reached the MIC for the test organism. On the basis of these observations, the emphasis that is placed on the PAE in discussions about the optimal dosing interval in aminoglycoside therapy is questionable.
机译:研究了妥布霉素对金黄色葡萄球菌和铜绿假单胞菌的一个给药间隔期间的抗生素后效应(PAE)的动力学。我们在模拟人药代动力学的体外药代动力学模型中,在此给药间隔12小时的不同时间点确定了PAE,其中妥布霉素的半衰期调整为2.4 +/- 0.2 h。使用酶促方法使妥布霉素失活,我们在1、5、8、12 h时确定了从模型中提取的样品中的PAEs,对应于妥布霉素的20、5、2和1倍于被测微生物的MIC浓度。 PAE从1小时的2.5小时显着降低到12小时的0小时。在实验期间,未观察到菌株的MIC变化。我们得出结论,在12小时的给药间隔内,PAE随着妥布霉素浓度的降低而降低,并在浓度达到测试生物的MIC后完全消失。基于这些观察,在关于氨基糖苷治疗的最佳给药间隔的讨论中对PAE的强调是有​​疑问的。

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