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卡马西平致畸性小鼠模型中卡马西平代谢的特征分析。

Characterization of carbamazepine metabolism in a mouse model of carbamazepine teratogenicity.

作者信息

Amore B M, Kalhorn T F, Skiles G L, Hunter A P, Bennett G D, Finnell R H, Nelson S D, Slattery J T

机构信息

Department of Pharmaceutics, School of Pharmacy, University of Washington, Seattle 98195-7610, USA.

出版信息

Drug Metab Dispos. 1997 Aug;25(8):953-62.

PMID:9280403
Abstract

The disposition of carbamazepine (CBZ) was investigated in the SWV mouse. A 14C-CBZ dose was administered to CBZ pretreated mice, and the distribution of radiolabeled material was determined. Twenty-four hours after the 14C-CBZ dose, 92.5% of the dose was accounted for in urine (56%), in the visera and carcass (22%), in feces (11%), and expired as 14CO2 (2%). CBZ metabolites present in hydrolyzed urine were also identified using a combination of spectroscopic techniques. CBZ, CBZ-10,11-epoxide (CBZE), 2- and 3-hydroxy-CBZ, methylsulfonyl-CBZ, and glucuronides of CBZ and CBZE accounted for 64% of total urinary radioactivity (0-24 hr) in CBZ pretreated mice. Minor metabolites of CBZ included novel cysteine and N-acetylcysteine conjugates of CBZ, as well as a methylsulfonyl conjugate of CBZE not previously reported. The urinary excretion of these thioether conjugates was increased in CBZ/phenobarbital pretreated mice and decreased in CBZ/stiripentol pretreated mice in comparison with CBZ-only treated mice. Preliminary studies of the effects of phenobarbital and stiripentol on the urinary abundance of these metabolites are consistent with the modulation of teratogenicity in the SWV mouse by the same pretreatments. These data suggest the formation of thioether metabolites of CBZ may be related to CBZ teratogenicity in the SWV mouse.

摘要

在SWV小鼠中研究了卡马西平(CBZ)的处置情况。给预先用CBZ处理过的小鼠给予14C-CBZ剂量,然后测定放射性标记物质的分布。给予14C-CBZ剂量24小时后,该剂量的92.5%出现在尿液中(56%)、内脏和尸体中(22%)、粪便中(11%),并以14CO2形式呼出(2%)。还使用多种光谱技术鉴定了水解尿液中存在的CBZ代谢物。CBZ、CBZ-10,11-环氧化物(CBZE)、2-和3-羟基-CBZ、甲基磺酰基-CBZ以及CBZ和CBZE的葡糖醛酸苷占预先用CBZ处理过的小鼠总尿放射性(0 - 24小时)的64%。CBZ的次要代谢物包括CBZ新的半胱氨酸和N-乙酰半胱氨酸共轭物,以及一种先前未报道的CBZE甲基磺酰共轭物。与仅用CBZ处理的小鼠相比,预先用CBZ/苯巴比妥处理的小鼠中这些硫醚共轭物的尿排泄增加,而预先用CBZ/司替戊醇处理的小鼠中则减少。关于苯巴比妥和司替戊醇对这些代谢物尿丰度影响的初步研究与相同预处理对SWV小鼠致畸性的调节一致。这些数据表明CBZ硫醚代谢物的形成可能与SWV小鼠中CBZ的致畸性有关。

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