Dose-dependent kinetics of diethylstilbestrol in the rat.

H Neumann
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Abstract

Diethylstilbestrol (DES) acts as a transplacental carcinogen with organotropic properties. The question is raised whether the pharmacokinetics of DES contribute to this effect. [3H] DES was administered to female Wistar rats orally, intravenously, and introperitoneally at doses ranging from 0.025 to 25 mg/kg. Radioactivity associated with erythrocytes and plasma proteins was measured and the pattern of unconjugated metabolites and glucuronides after column and thin-layer chromatography in blood determined. The different routes of administration resulted in different metabolite patterns. After iv injection, unconjugated, unpolar metabolites predomininated; after ip injection, glucuronides of unpolar metabolites; and after oral administration, unconjugated polar metabolites. The different compositions of the glucuronide fractions remained constant with time. The composition of the unconjugated metabolites changed with time after oral administration but not after iv injection. Blood levels of metabolites did not increase proportionally with dose. Overproportional increase was most prominent with the highest dose used. The observed effects are explained with intestinal metabolism and a liver first-pass effect.

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己烯雌酚在大鼠体内的剂量依赖性动力学。
己烯雌酚(DES)是一种具有器官性的胎盘转移致癌物。问题是DES的药代动力学是否促成了这种效果。[3H]雌性Wistar大鼠口服、静脉注射和腹腔注射DES,剂量范围为0.025 ~ 25mg /kg。测定了与红细胞和血浆蛋白相关的放射性,并测定了柱层和薄层色谱后血液中未结合代谢物和葡萄糖醛酸苷的模式。不同的给药途径导致不同的代谢模式。静脉注射后,以非偶联、非极性代谢物为主;注射IP后,非极性代谢产物葡糖苷;口服后,无偶联极性代谢物。葡萄糖醛酸酯组分的不同组成随时间保持不变。非偶联代谢物的组成在口服后随时间变化,而在静脉注射后无变化。血液中代谢物水平没有随剂量成比例增加。在使用最高剂量时,比例增加最为显著。观察到的效果可以用肠道代谢和肝脏首过效应来解释。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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