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[采用持续静脉输注法对小诺米星进行的药代动力学研究]

[Pharmacokinetic studies of micronomicin using a continuous intravenous infusion method].

作者信息

Yamasaku F

出版信息

Jpn J Antibiot. 1983 Nov;36(11):3283-90.

PMID:6674541
Abstract

The basic pharmacokinetics of micronomicin (MCR) were studied in 4 healthy adult volunteers. MCR 60 and 120 mg were intravenously administered in 30 and 60 minutes at constant rates by means of continuous infusion apparatus. The same dosages were also tested by intramuscular route. The concentrations of MCR in serum and urine were determined by HPLC and analyzed following the two-compartment open model after intravenous treatment and following the one-compartment open model after intramuscular treatment. When MCR was given by intramuscular route, the mean serum concentration of 4 subjects reached a peak of 3.98 micrograms/ml at 30 minutes after a dose of 60 mg and 6.7 micrograms/ml at 30 minutes after that of 120 mg. The peak concentration was achieved at the end of intravenous infusion and was dose-related, since it was 6.1 and 10.5 micrograms/ml after a 30-minute infusion of 60 and 120 mg, respectively, and 4.85 and 9.43 micrograms/ml after a 60-minute infusion of 60 and 120 mg, respectively. At 8 hours, concentrations dropped to less than 0.1 microgram/ml and to 0.2 microgram/ml or less after 60 and 120 mg, respectively, regardless of the route and rate of administration. The mean urinary recovery up to 8 hours ranged 84 to 92% of the dose. There were no appreciable differences in pharmacokinetic parameters among 4 modes of intravenous infusion, with a T1/2(beta) of 1.43 approximately 2.02 hours. In the case of intramuscular treatment, parameters analyzed following the one-compartment open model were on similar levels to corresponding values found after intravenous treatment and the T1/2 was 1.39 hours after 60 mg and 1.43 hours after 120 mg.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在4名健康成年志愿者中研究了小诺米星(MCR)的基本药代动力学。通过连续输注装置,以恒定速率在30分钟和60分钟内静脉注射60毫克和120毫克MCR。相同剂量也通过肌肉注射途径进行测试。静脉注射后,采用二室开放模型,肌肉注射后,采用一室开放模型,通过高效液相色谱法测定血清和尿液中MCR的浓度并进行分析。当通过肌肉注射途径给予MCR时,4名受试者的平均血清浓度在给予60毫克剂量后30分钟达到峰值3.98微克/毫升,在给予120毫克剂量后30分钟达到6.7微克/毫升。静脉输注结束时达到峰值浓度,且与剂量相关,因为在分别输注60毫克和120毫克30分钟后,峰值浓度分别为6.1和10.5微克/毫升,在分别输注60毫克和120毫克60分钟后,峰值浓度分别为4.85和9.43微克/毫升。8小时时,无论给药途径和速率如何,浓度分别降至低于0.1微克/毫升(60毫克剂量后)和0.2微克/毫升或更低(120毫克剂量后)。至8小时的平均尿回收率为剂量的84%至92%。4种静脉输注方式的药代动力学参数无明显差异,T1/2(β)为1.43至2.02小时。在肌肉注射治疗的情况下,采用一室开放模型分析的参数与静脉注射治疗后相应值处于相似水平,60毫克后T1/2为1.39小时,120毫克后T1/2为1.43小时。(摘要截断于250字)

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