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伯氨喹在人体内的药代动力学:鉴定羧酸衍生物为主要血浆代谢物。

Pharmacokinetics of primaquine in man: identification of the carboxylic acid derivative as a major plasma metabolite.

作者信息

Mihaly G W, Ward S A, Edwards G, Orme M L, Breckenridge A M

出版信息

Br J Clin Pharmacol. 1984 Apr;17(4):441-6. doi: 10.1111/j.1365-2125.1984.tb02369.x.

Abstract

A method is described for the simultaneous determination of the carboxylic acid and N-acetyl-derivatives of primaquine, in plasma and urine. After oral administration of 45 mg primaquine, to five healthy volunteers, absorption was rapid, with peak primaquine levels of 153.3 +/- 23.5 ng/ml at 3 +/- 1 h, followed by an elimination half-life of 7.1 +/- 1.6 h, systemic clearance of 21.1 +/- 7.1 l/h, volume of distribution of 205 +/- 371 and cumulative urinary excretion of 1.3 +/- 0.9% of the dose. Primaquine underwent rapid conversion to the carboxylic acid metabolite of primaquine, which achieved peak levels of 1427 +/- 307 ng/ml at 7 +/- 4 h. Levels of this metabolite were sustained in excess of 1000 ng/ml for the 24 h study period, and no carboxyprimaquine was recovered in urine. N-acetyl primaquine was not detected in plasma or urine. Following [14C]-primaquine administration to one subject, plasma radioactivity levels rapidly exceeded primaquine concentrations. Plasma radioactivity was accounted for mainly as carboxyprimaquine . Though 64% of the dose was recovered over 143 h, as [14C]-radioactivity in urine, only 3.6% was due to primaquine. As neither carboxyprimaquine nor N- acetylprimaquine were detected in urine, the remaining radioactivity was due to unidentified metabolites.

摘要

本文描述了一种同时测定血浆和尿液中伯氨喹羧酸和N - 乙酰衍生物的方法。给5名健康志愿者口服45mg伯氨喹后,吸收迅速,在3±1小时达到伯氨喹峰值水平153.3±23.5ng/ml,随后消除半衰期为7.1±1.6小时,全身清除率为21.1±7.1l/h,分布容积为205±371,累积尿排泄量为剂量的1.3±0.9%。伯氨喹迅速转化为其羧酸代谢物,该代谢物在7±4小时达到峰值水平1427±307ng/ml。在24小时研究期间,该代谢物水平维持在1000ng/ml以上,尿液中未回收羧基伯氨喹。血浆和尿液中均未检测到N - 乙酰伯氨喹。给一名受试者服用[14C] - 伯氨喹后,血浆放射性水平迅速超过伯氨喹浓度。血浆放射性主要以羧基伯氨喹形式存在。尽管在143小时内64%的剂量以尿液中的[14C] - 放射性形式回收,但仅3.6%是由于伯氨喹。由于尿液中未检测到羧基伯氨喹和N - 乙酰伯氨喹,其余放射性归因于未鉴定的代谢物。

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