ROLE OF P450IID6, THE TARGET OF THE SPARTEINE-DEBRISOQUIN OXIDATION POLYMORPHISM, IN THE METABOLISM OF IMIPRAMINE

被引：122

作者：

BROSEN, K ^{[1
]}

ZEUGIN, T ^{[1
]}

MEYER, UA ^{[1
]}

机构：

[1] UNIV BASEL,BIOCTR,CH-4056 BASEL,SWITZERLAND

来源：

CLINICAL PHARMACOLOGY & THERAPEUTICS | 1991年 / 49卷 / 06期

关键词：

D O I：

10.1038/clpt.1991.77

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The formation of three oxidative metabolites of imipramine, N-desmethylimipramine (desipramine), 2-hydroxyimipramine, and 10-hydroxyimipramine was studied in microsomes of an extensive metabolizer liver (KDL 26) and of a poor metabolizer liver (KDL 31) and in a homogenate of COS-1 cells in which the P450IID6 complementary deoxyribonucleic acid had been expressed. The following data support the role of P450IID6 in the 2-hydroxylation of imipramine: (1) The formation of 2-hydroxyimipramine was reduced to less than 20% of the control value when microsomes were incubated with serum containing inhibitory antibodies against P450IID6 (anti-LKM1), whereas no effect was seen with regard to formation of desipramine and 10-hydroxyimiprainine, (2) quinidine and levomepromazine were potent competitive inhibitors of 2-hydroxylation of imipramine (k(i) almost-equal-to 70 nmol/L, and k(i) almost-equal-to 1-mu-mol/L, respectively) but had no effect on N-demethylation and 10-hydroxylation, and (3) in the COS-1 cell, homogenate, 10-hydroxyimipramine, 2-hydroxyimipramine, and desipramine were formed at rates of 48, 164, and 256 pmol per hour per milligram of homogenate protein, respectively. The P450 isozymes that are responsible for N-demethylation and 10-hydroxylation of imipramine have not yet been identified.

引用

页码：609 / 617

页数：9

共 31 条

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