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大鼠体内两种含半胱胺的2-(氯乙基)亚硝基脲的主要尿液代谢产物。

Main urinary metabolites of two cysteamine-containing 2-(chloroethyl) nitrosoureas in rats.

作者信息

Godeneche D, Labarre P, Moreau M F, Madelmont J C, Rapp M, Papon J, Veyre A

机构信息

Institut National de la Santé et de la Recherche Médicale, INSERM U71, BP 184, Clermont-Ferrand, France.

出版信息

Drug Metab Dispos. 1993 Jan-Feb;21(1):93-9.

PMID:8095233
Abstract

Urine is the major route of excretion of N'-(2-chloroethyl)-N-[2-(methylsulfinyl)ethyl]-N'-nitrosourea (CMSOEN2), N'-(2-chloroethyl)-N-[2-(methylsulfonyl)ethyl]-N'-nitrosourea (CMSO2EN2), and their metabolites in the rat. Labeling the two compounds with 14C in three different positions facilitated their metabolic study in animals. The 14C-ethyl species were chosen in order to investigate the presence of unchanged compounds and that of the denitrosated forms. With the same 14C label position, we showed that isolated metabolites derived from this part of the molecule were degradation products of alkylated glutathione and/or cysteine. They are common to both CMSOEN2 and CMSO2EN2, namely thiodiacetic acid and its sulfoxide, the sum of which represents about half of urinary radioactivity. N-acetyl carboxymethylcysteine and N-acetyl hydroxyethylcysteine, accounting for approximately 6% to 7% of the eliminated 14C radioactivity, were also characterized. However, four minor metabolites corresponding to less than 10% of the excreted radioactivity remained unidentified. With the [14C]cysteamine and [14C]carbonyl labels related to the isocyanate moiety behavior, we indirectly showed that more than 60% to 70% of the excreted metabolites were carbamoylation products of endogenous substrates. A small amount of free amines, 2-methylsulfinylethylamine and/or 2-methylsulfonylethylamine, representing 15%-16% of the eliminated radioactivity, was also detected. The total data confirm the predominant function of glutathione and/or cysteine in the detoxifying system of the chloroethyl moieties and reveal the unexpected but important role played by carbamoylation reactions in the metabolic fate of the drug isocyanate moieties.

摘要

尿液是大鼠体内N'-(2-氯乙基)-N-[2-(甲基亚磺酰基)乙基]-N'-亚硝基脲(CMSOEN2)、N'-(2-氯乙基)-N-[2-(甲基磺酰基)乙基]-N'-亚硝基脲(CMSO2EN2)及其代谢产物的主要排泄途径。将这两种化合物在三个不同位置用14C标记有助于在动物体内进行它们的代谢研究。选择14C-乙基形式是为了研究未变化的化合物和脱亚硝基形式的存在情况。在相同的14C标记位置,我们表明源自该分子这一部分的分离代谢产物是烷基化谷胱甘肽和/或半胱氨酸的降解产物。它们是CMSOEN2和CMSO2EN2共有的,即硫代二乙酸及其亚砜,其总和约占尿液放射性的一半。还鉴定出了占消除的14C放射性约6%至7%的N-乙酰羧甲基半胱氨酸和N-乙酰羟乙基半胱氨酸。然而,四种占排泄放射性不到10%的次要代谢产物仍未鉴定出来。通过与异氰酸酯部分行为相关的[14C]半胱胺和[14C]羰基标记,我们间接表明超过60%至70%的排泄代谢产物是内源性底物的氨基甲酰化产物。还检测到少量游离胺、2-甲基亚磺酰基乙胺和/或2-甲基磺酰基乙胺,占消除放射性的15%-16%。总体数据证实了谷胱甘肽和/或半胱氨酸在氯乙基部分解毒系统中的主要作用,并揭示了氨基甲酰化反应在药物异氰酸酯部分代谢命运中所起的意外但重要的作用。

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