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血红蛋白介导的烯胺代谢及单电子氧化的可能参与。

Haemoprotein-mediated metabolism of enamines and the possible involvement of one-electron oxidations.

作者信息

Sayre L M, Engelhart D A, Nadkarni D V, Babu M K, Klein M E, McCoy G

机构信息

Department of Chemistry, Case Western Reserve University, Cleveland, OH 44106, USA.

出版信息

Xenobiotica. 1995 Jul;25(7):769-75. doi: 10.3109/00498259509061892.

DOI:10.3109/00498259509061892
PMID:7483673
Abstract
  1. Microsomal metabolism of 1-benzylpiperidine (1-BP), its cis-2,6-dimethyl (cis-2,6-DMBP), 4,4-dimethyl (4,4-DMBP), and alpha, alpha-dimethyl (alpha, alpha-DMBP) analogues, and phencyclidine (PCP) has been studied to assess the involvement of P450 oxidation of the enamine tautomers of the initial endocyclic iminium metabolites. 2. The selective prevention by cyanide of the metabolite production of 1-benzyl-3-piperidone but not 1-benzyl-3-piperidinol from 1-BP is consistent with the enamine as the source of the 3-one metabolite. 3. The parent amines and particularly the independently prepared iminium species induced a pattern of metabolism-dependent irreversible inactivation of P450 benz-phetamine demethylase activity, consistent with involvement of enamine C-3 oxidation in the inactivation process. 4. Substrate activity of the endocyclic enamines and alpha-aminoketones (presumably the enol-enamine tautomers) for horseradish peroxidase under conditions where simple aliphatic amines display no activity is consistent with metabolic one-electron oxidations of the enamines.
摘要
  1. 已对1-苄基哌啶(1-BP)、其顺式-2,6-二甲基(顺式-2,6-DMBP)、4,4-二甲基(4,4-DMBP)和α,α-二甲基(α,α-DMBP)类似物以及苯环己哌啶(PCP)的微粒体代谢进行了研究,以评估初始内环亚胺代谢物的烯胺互变异构体的P450氧化作用。2. 氰化物对1-BP生成1-苄基-3-哌啶酮而非1-苄基-3-哌啶醇代谢物的选择性抑制作用,与烯胺作为3-酮代谢物的来源一致。3. 母体胺类,尤其是独立制备的亚胺物种,诱导了一种与P450苄非他明脱甲基酶活性代谢依赖性不可逆失活相关的模式,这与烯胺C-3氧化参与失活过程一致。4. 在简单脂肪族胺无活性的条件下,内环烯胺和α-氨基酮(可能是烯醇-烯胺互变异构体)对辣根过氧化物酶的底物活性与烯胺的代谢单电子氧化作用一致。

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