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N-乙基-N-甲基苯胺体外N-氧化立体选择性的种属差异。

Species differences in the stereoselectivity of N-oxygenation of N-ethyl-N-methylaniline in vitro.

作者信息

Hadley M R, Oldham H G, Camilleri P, Damani L A, Hutt A J

机构信息

SmithKline Beecham Pharmaceuticals, Tonbridge, Kent, England.

出版信息

Chirality. 1996;8(6):430-40. doi: 10.1002/(SICI)1520-636X(1996)8:6<430::AID-CHIR4>3.0.CO;2-G.

Abstract

The prochiral tertiary amine N-ethyl-N-methylaniline (EMA) is known to be stereoselectively N-oxygenated in the presence of hepatic microsomal preparations. This biotransformation is thought to be mediated predominantly by the flavin-containing monooxygenase (FMO) enzyme system. In order to characterise this reaction further, the in vitro metabolism of EMA in the presence of hepatic microsomal preparations derived from a number of laboratory species has been examined. EMA N-oxide formation was stereoselective with respect to the (-)-S-enantiomer in the presence of microsomal preparations from all species examined, with the degree of selectivity decreasing in the order of rabbit > rat approximately LACA mouse approximately DBA/2Ha mouse > guinea-pig > dog. The enantiomeric composition of the metabolically derived EMA N-oxide appeared to be determined solely by the differential rate of formation of the two enantiomers as opposed to any differences in affinities for the substrate in its pro-R and pro-S conformations. The use of enzyme inhibitors, activators and inducers indicated that EMA N-oxide formation was predominantly mediated by FMO in the presence of rabbit hepatic microsomes and that these agents did not generally affect the stereochemical outcome of the biotransformation.

摘要

已知前手性叔胺N-乙基-N-甲基苯胺(EMA)在肝微粒体制剂存在下会发生立体选择性N-氧化。这种生物转化被认为主要由含黄素单加氧酶(FMO)酶系统介导。为了进一步表征该反应,研究了在源自多种实验动物的肝微粒体制剂存在下EMA的体外代谢。在所有受试动物的微粒体制剂存在下,EMA N-氧化物的形成对(-)-S-对映体具有立体选择性,选择性程度按以下顺序降低:兔>大鼠>近交系LACA小鼠>近交系DBA/2Ha小鼠>豚鼠>狗。代谢生成的EMA N-氧化物的对映体组成似乎仅由两种对映体形成的差异速率决定,而非其前R和前S构象对底物亲和力的任何差异。酶抑制剂、激活剂和诱导剂的使用表明,在兔肝微粒体存在下,EMA N-氧化物的形成主要由FMO介导,并且这些试剂通常不影响生物转化的立体化学结果。

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