Smeltzer B D, Schwartzman M S, Bertino J S
Department of Pharmacy Services, Mary Imogene Bassett Hospital, Cooperstown, New York 13326.
Antimicrob Agents Chemother. 1988 Feb;32(2):236-40. doi: 10.1128/AAC.32.2.236.
The pharmacokinetics of amikacin were investigated in five stable patients undergoing continuous ambulatory peritoneal dialysis (CAPD). Each patient was studied after the administration of 7.5 mg of amikacin per kg by both the intravenous (i.v.) and intraperitoneal (i.p.) route, allowing a 1-month washout period between doses. No differences in amikacin half-life, volume of distribution, total body clearance, or time-averaged peritoneal clearance were noted between the two routes of administration. After a 5-h dwell period, bioavailability as calculated by the area under the curve for i.p. amikacin was 53 +/- 14.0%. Amikacin pharmacokinetics parallel those of other aminoglycosides in CAPD patients when the drug is administered either i.v. or i.p. Single loading doses of amikacin administered i.v. to uninfected CAPD patients provided therapeutic serum and dialysate levels for many aerobic gram-negative organisms for up to 72 h. Because of the variability of absorption of i.p. administered amikacin, single i.p. doses are not recommended.
在5例接受持续性非卧床腹膜透析(CAPD)的稳定患者中研究了阿米卡星的药代动力学。每位患者经静脉(i.v.)和腹腔内(i.p.)途径给予每千克7.5mg阿米卡星后进行研究,两次给药之间有1个月的洗脱期。两种给药途径之间未观察到阿米卡星半衰期、分布容积、总体清除率或时间平均腹膜清除率的差异。在5小时的留腹期后,腹腔内给予阿米卡星的曲线下面积计算得出的生物利用度为53±14.0%。当药物经静脉或腹腔内给药时,CAPD患者中阿米卡星的药代动力学与其他氨基糖苷类药物相似。对未感染的CAPD患者静脉注射单次负荷剂量的阿米卡星,可为许多需氧革兰氏阴性菌提供长达72小时的治疗性血清和透析液水平。由于腹腔内给予阿米卡星吸收的变异性,不建议单次腹腔内给药。
