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Impact of netilmicin regimens on the activities of ceftazidime-netilmicin combinations against Pseudomonas aeruginosa in an in vitro pharmacokinetic model.

机译:在体外药代动力学模型中,奈替米星方案对头孢他啶-奈替米星组合抗铜绿假单胞菌活性的影响。

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摘要

The antibacterial activities of ceftazidime and netilmicin were studied in a two-compartment in vitro model. Pseudomonas aeruginosa cultures were exposed to changing drug concentrations that mimic human pharmacokinetics. Netilmicin alone reduced the numbers of organisms in cultures of the susceptible strains by more than 99% within 4 h; however, regrowth occurred after 8 h. Although ceftazidime alone killed more slowly than netilmicin, only one of the five strains regrew within 28 h. When both drugs were combined, rapid initial killing occurred without subsequent regrowth. Studied after 24 h in combination with ceftazidime, netilmicin was as effective when given as a single daily dose as when administered in three daily doses that provided 50% more aminoglycoside per day. Decreased bacterial susceptibility was seen after ceftazidime exposure for one strain and after netilmicin exposure for all originally netilmicin-susceptible strains. No such reduction in susceptibility was observed during exposure to the combination. The results of standard in vitro checkerboard tests for synergism were predictive of the initial (4 to 8 h) but not the final (24 to 28 h) assessment of drug interaction in the pharmacokinetic model.
机译:在两室体外模型中研究了头孢他啶和奈替米星的抗菌活性。铜绿假单胞菌培养物暴露于模仿人药代动力学的变化的药物浓度。仅用奈替米星就可以在4小时内将易感菌株培养物中的生物体数量减少99%以上;然而,再生长发生在8小时后。尽管仅头孢他啶的杀灭作用比奈替米星慢,但五种菌株中只有一种在28小时内恢复。当两种药物联合使用时,快速的最初杀伤发生而没有随后的再生。与头孢他啶联用24小时后研究,奈替米星作为单日剂量给药与以三日剂量给药(每天提供50%更多的氨基糖苷)给药一样有效。暴露于头孢他啶的一种菌株后以及所有初始耐替尼米星敏感菌株的奈替米星暴露后,细菌的敏感性均降低。暴露于该组合期间未观察到磁化率的这种降低。协同作用的标准体外棋盘格测试结果可预测药代动力学模型中药物相互作用的初始评估(4至8小时),而非最终评估(24至28小时)。

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