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阿米卡星在新生儿中的药理学评估。

Pharmacological evaluation of amikacin in neonates.

作者信息

Howard J B, McCracken G H

出版信息

Antimicrob Agents Chemother. 1975 Jul;8(1):86-90. doi: 10.1128/AAC.8.1.86.

Abstract

The in vitro bacterial susceptibilities and pharmacokinetic properties of amikacin (BB-K8) were studied in newborn infants. Gram-negative bacteria and Staphylococcus aureus isolated from neonates were uniformly susceptible to 10 mug or less of amikacin per ml, and five Escherichia coli strains resistant to kanamycin were inhibited and killed by 5 mug or less of amikacin per ml. Mean peak serum concentrations of 17 to 20 mug/ml were observed 30 min after 7.5-mg/kg amikacin doses, and accumulation of drug in serum was not detected after repeated doses for 5 to 7 days. Intravenous infusion of amikacin over a 20-min period resulted in extremely low peak serum levels in four of eight infants studied. Serum half-life values were correlated inversely with postnatal age and renal clearances of amikacin. The volumes of drug distribution indicate that amikacin remains primarily in the extracellular fluid space of neonates. The lack of efficacy and safety data preclude the use of amikacin in neonates at this time.

摘要

在新生儿中研究了阿米卡星(BB-K8)的体外细菌敏感性和药代动力学特性。从新生儿中分离出的革兰氏阴性菌和金黄色葡萄球菌对每毫升10微克或更低剂量的阿米卡星均表现出一致的敏感性,并且5株对卡那霉素耐药的大肠杆菌菌株被每毫升5微克或更低剂量的阿米卡星抑制和杀灭。在给予7.5毫克/千克阿米卡星剂量后30分钟,观察到平均血清峰浓度为17至20微克/毫升,在重复给药5至7天后未检测到药物在血清中的蓄积。在研究的8名婴儿中有4名在20分钟内静脉输注阿米卡星后血清峰浓度极低。血清半衰期值与出生后年龄和阿米卡星的肾脏清除率呈负相关。药物分布容积表明阿米卡星主要保留在新生儿的细胞外液空间中。目前缺乏疗效和安全性数据,因此暂不推荐在新生儿中使用阿米卡星。

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Pharmacological evaluation of amikacin in neonates.阿米卡星在新生儿中的药理学评估。
Antimicrob Agents Chemother. 1975 Jul;8(1):86-90. doi: 10.1128/AAC.8.1.86.
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