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Stable isotope methodology in the pharmacokinetic studies of androgenic steroids in humans.

作者信息

Shinohara Y, Baba S

机构信息

Tokyo College of Pharmacy, Japan.

出版信息

Steroids. 1990 Apr;55(4):170-6. doi: 10.1016/0039-128x(90)90106-l.

DOI:10.1016/0039-128x(90)90106-l
PMID:2187285
Abstract

The use of stable isotopically labeled steroids combined with gas chromatography/mass spectrometry (GC/MS) has found a broad application in pharmacologic studies. Initially, stable isotopically labeled steroids served as the ideal analytic internal standard for GC/MS analysis; however, their in vivo use has expanded and has proven to be a powerful pharmacokinetic tool. We have successfully used stable isotope methodology to study the pharmacokinetic/bioavailability of androgens. The primary advantage of the technique is that endogenous and exogenous steroids with the same basic structure can be differentiated by using stable isotopically labeled analogs. The method was used to examine the pharmacokinetics of testosterone and testosterone propionate, and to clarify the influence of endogenous testosterone. Another advantage of the isotope methods is that steroidal drugs can be administered concomitantly in two formulations (e.g., solution and solid dosage). A single set of blood samples serves to describe the time course of the formulations being compared. This stable isotope coadministration technique was used to estimate the relative bioavailability of 17 alpha-methyltestosterone.

摘要

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