CAFFEINE METABOLISM BY HUMAN HEPATIC CYTOCHROMES P450 - CONTRIBUTIONS OF 1A2, 2E1 AND 3A ISOFORMS

被引：194

作者：

TASSANEEYAKUL, W

BIRKETT, DJ

MCMANUS, ME

TASSANEEYAKUL, W

VERONESE, ME

ANDERSSON, T

TUKEY, RH

MINERS, JO

机构：

[1] FLINDERS UNIV S AUSTRALIA, MED CTR, DEPT CLIN PHARMACOL, BEDFORD PK, SA 5042, AUSTRALIA

[2] UNIV QUEENSLAND, DEPT PHYSIOL & PHARMACOL, ST LUCIA, QLD 4072, AUSTRALIA

[3] UNIV CALIF SAN DIEGO, CTR CANC, DEPT PHARMACOL, LA JOLLA, CA 92093 USA

[4] ASTRA HASSLE AB, MOLNDAL, SWEDEN

来源：

BIOCHEMICAL PHARMACOLOGY | 1994年 / 47卷 / 10期

关键词：

CAFFEINE; CYTOCHROME P450; DRUG METABOLISM; HUMAN LIVER; SUBSTRATE PROBE;

D O I：

10.1016/0006-2952(94)90304-2

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Caffeine (CA) N1-, N3- and N7-demethylase, CA 8-hydroxylase and phenacetin O-deethylase activities were measured in microsomes from 18 separate human livers which had been characterized previously for a range of cytochrome P450 (CYP) isoform-specific activities and immunoreactive CYP protein contents. Correlations between the high affinity components of the three separate CA N-demethylations were highly significant (r = 0.77-0.91, P < 0.001) and each of the three high affinity CA N-demethylations correlated significantly (r = 0.64-0.93, P < 0.05-0.001) with the high affinity phenacetin O-deethylase, 2-acetylaminofluorene N-hydroxylation and 2-amino-1-methyl-6-phenylimidazo[4 ,5-b]pyridine (PhIP) and 2-amino-3-methylimidazo[4,5-f]quinoline (IQ) mutagenicity (all predominantly CYP1A2-mediated reactions). Consistent with these observations, cDNA-expressed human CYP1A2 catalyzed the N1-, N3- and N7-demethylation of CA and apparent K-m values were similar (0.24-0.28 mM) for ah three reactions and comparable to those observed previously with human liver microsomes. The low affinity components of CA N1- and N7-demethylation correlated significantly (r = 0.55-0.85, P < 0.05-0.001) with immunoreactive CYP2E1 content and the CYP2E1-specific activities 4-nitrophenol and chlorzoxazone hydroxylation. Diethyldithiocarbamate, a selective inhibitor of CYP2E1, inhibited the low affinity CA N1- and N7-demethylation, with IC50 values of 23 mu M and 11 mu M, respectively. The apparent K-m, values for CA N1- and N7-demethylation by cDNA-expressed CYP2E1 (namely 28 and 43 mM, respectively) were of a similar order to those calculated for the low affinity microsomal activities. Significant correlations (r = 0.87-0.97, P < 0.001) were observed between CA 8-hydroxylation and immunoreactive CYP3A content and the CYP3A-mediated reactions benzo(a)pyrene hydroxylation, omeprazole sulfoxidation and aflatoxin B1 mutagenesis. Effects of alpha-naphthoflavone, erythromycin, troleandomycin and nifedipine on microsomal CA 8-hydroxylation were generally consistent with CYP3A involvement. Taken together with previous data, the results indicate a major involvement of CYP1A2 in the high affinity component of all three human hepatic CA N-demethylations. In contrast, CYP2E1 appears to be the main enzyme involved in the low affinity components of CA N1- and N7-demethyIation while CA 8-hydroxylation is catalysed predominantly by a CYP3A isoform(s).

引用

页码：1767 / 1776

页数：10

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