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司来吉兰主要代谢产物的药代动力学及生物等效性:口服司来吉兰后的去甲基司来吉兰、甲基苯丙胺和苯丙胺

Pharmacokinetics and bioequivalence of the main metabolites of selegiline: desmethylselegiline, methamphetamine and amphetamine after oral administration of selegiline.

作者信息

Mascher H J, Kikuta C, Millendorfer A, Schiel H, Ludwig G

机构信息

Pharm-analyt Laboratory GmbH, Baden, Austria.

出版信息

Int J Clin Pharmacol Ther. 1997 Jan;35(1):9-13.

PMID:9021435
Abstract

A bioavailability study of 2 different selegiline preparations were conducted in 20 healthy volunteers to test the bioequivalence. Almost no bioavailability study of selegiline has been published. As plasma levels of selegiline are very low and the elimination half-life is very short being about 9 minutes, therefore, a very sensitive and selective method for determining the 3 main metabolites desmethylselegiline (DMS), methamphetamine (MA) and amphetamine (A) was developed. After application of a single oral dose of 5 mg selegiline the Cmax values of DMS reached 5-6 ng/ml, of MA 6-7 ng/ml and of A about 2 ng/ml. The AUC infinity values were with DMS about 11 ng/ml x h +/- 4.5, with MA about 130 g/ml x h +/- 50 and with A about 50 ng/ml x h +/- 15. The 90% confidence interval was with logarithmic transformed AUC infinity values 92-107% with DMS, 89-107% with MA, and 84-104% with A. The logarithmic transformed Cmax values showed a 90% confidence interval of 92-127% with DMS, 91-101% with MA, and 90-103% with A. All relevant pharmacokinetic parameters showed bioequivalence with all 3 metabolites (DMS, MA, and A).

摘要

在20名健康志愿者中进行了2种不同司来吉兰制剂的生物利用度研究,以测试生物等效性。几乎没有关于司来吉兰生物利用度研究的报道发表。由于司来吉兰的血浆水平非常低,消除半衰期很短,约为9分钟,因此开发了一种非常灵敏和特异的方法来测定3种主要代谢物去甲基司来吉兰(DMS)、甲基苯丙胺(MA)和苯丙胺(A)。单次口服5mg司来吉兰后,DMS的Cmax值达到5-6ng/ml,MA为6-7ng/ml,A约为2ng/ml。DMS的AUC∞值约为11ng/ml·h±4.5,MA约为130ng/ml·h±50,A约为50ng/ml·h±15。对数转换后的AUC∞值的90%置信区间,DMS为92-107%,MA为89-107%,A为84-104%。对数转换后的Cmax值显示,DMS的90%置信区间为92-127%,MA为91-101%,A为90-103%。所有相关的药代动力学参数显示,3种代谢物(DMS、MA和A)均具有生物等效性。

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