INVITRO FORECASTING OF DRUGS THAT MAY INTERFERE WITH CODEINE BIOACTIVATION

被引：22

作者：

DAYER, P ^{[1
]}

DESMEULES, J ^{[1
]}

STRIBERNI, R ^{[1
]}

机构：

[1] UNIV HOSP GENEVA, PAIN CLIN, CH-1211 GENEVA 14, SWITZERLAND

来源：

EUROPEAN JOURNAL OF DRUG METABOLISM AND PHARMACOKINETICS | 1992年 / 17卷 / 02期

关键词：

CODEINE; MORPHINE; DRUG INTERACTIONS; CYTOCHROME P450 DB1; CYP2D6;

D O I：

10.1007/BF03188779

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The O-demethylation of codeine (methylmorphine) into morphine is mediated by the polymorphic cytochrome P450 DB1 (P450 IID6). By means of in vitro screening in human liver microsomes we have studied the effect on codeine bioactivation of several drugs used as analgesics or as adjuvants for pain control. In microsomes from an extensive metabolizer subject, paracetamol (acetaminophen) and NSAIDs (acetylsalicylic acid, diclofenac, indomethacin, piroxicam, and pirprofen), benzodiazepines (chlordiazepoxide, clonazepam, diazepam, flunitrazepam, and midazolam), and anticonvulsants (carbamazepine and phenytoin) did not alter the reaction. There was marked inhibition of in vitro morphine production by neuroleptics (chlorpromazine, haloperidol, levomepromazine, and thioridazine), metoclopramide, and tricyclic antidepressants (amitriptyline, clomipramine, desipramine, imipramine, and nortriptyline). Enzyme kinetics showed competitive inhibition by neuroleptics (chlorpromazine K(i) = 0.5-mu-M) and antidepressants (clomipramine K(i) = 6.8-mu-M), which are substrates of the polymorphic monooxygenase. Due to the low affinity of codeine for P450 DB1 (K(m) = 100-200-mu-M), its bioactivation in extensive metabolizers, and thus its analgesic efficacy, is liable to vary greatly when it is combined with any drug that has a high affinity for the polymorphic isozyme.

引用

页码：115 / 120

页数：6

共 26 条

[1] IMPORTANCE OF OXIDATIVE POLYMORPHISM AND LEVOMEPROMAZINE TREATMENT ON THE STEADY-STATE BLOOD-CONCENTRATIONS OF CLOMIPRAMINE AND ITS MAJOR METABOLITES [J].

BALANTGORGIA, AE ;

BALANT, LP ;

GENET, C ;

DAYER, P ;

AESCHLIMANN, JM ;

GARRONE, G .

EUROPEAN JOURNAL OF CLINICAL PHARMACOLOGY, 1986, 31 (04) :449-455

[2] EXPRESSION OF A HUMAN-LIVER CYTOCHROME-P-450 PROTEIN WITH TOLBUTAMIDE HYDROXYLASE-ACTIVITY IN SACCHAROMYCES-CEREVISIAE [J].

BRIAN, WR ;

SRIVASTAVA, PK ;

UMBENHAUER, DR ;

LLOYD, RS ;

GUENGERICH, FP .

BIOCHEMISTRY, 1989, 28 (12) :4993-4999

[3] CLINICAL-SIGNIFICANCE OF THE SPARTEINE-DEBRISOQUINE OXIDATION POLYMORPHISM [J].

BROSEN, K ;

GRAM, LF .

EUROPEAN JOURNAL OF CLINICAL PHARMACOLOGY, 1989, 36 (06) :537-547

[4] RECENT DEVELOPMENTS IN HEPATIC DRUG OXIDATION - IMPLICATIONS FOR CLINICAL PHARMACOKINETICS [J].

BROSEN, K .

CLINICAL PHARMACOKINETICS, 1990, 18 (03) :220-239

[5]

CHEN ZR, 1988, LANCET, V2, P914

[6]

Cochran W.G, 1957, STAT METHODS, V6th ed

[7] ENZYMATIC BASIS OF THE DEBRISOQUINE SPARTEINE-TYPE GENETIC-POLYMORPHISM OF DRUG OXIDATION - CHARACTERIZATION OF BUFURALOL 1'-HYDROXYLATION IN LIVER-MICROSOMES OF INVIVO PHENOTYPED CARRIERS OF THE GENETIC DEFICIENCY [J].

DAYER, P ;

KRONBACH, T ;

EICHELBAUM, M ;

MEYER, UA .

BIOCHEMICAL PHARMACOLOGY, 1987, 36 (23) :4145-4152

[8] DEXTROMETHORPHAN O-DEMETHYLATION IN LIVER-MICROSOMES AS A PROTOTYPE REACTION TO MONITOR CYTOCHROME-P-450 DB1 ACTIVITY [J].

DAYER, P ;

LEEMANN, T ;

STRIBERNI, R .

CLINICAL PHARMACOLOGY & THERAPEUTICS, 1989, 45 (01) :34-40

[9] BIOACTIVATION OF THE NARCOTIC DRUG CODEINE IN HUMAN-LIVER IS MEDIATED BY THE POLYMORPHIC MONOOXYGENASE CATALYZING DEBRISOQUINE 4-HYDROXYLATION (CYTOCHROME-P-450 DBL/BUFI) [J].

DAYER, P ;

DESMEULES, J ;

LEEMANN, T ;

STRIBERNI, R .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1988, 152 (01) :411-416

[10]

DAYER P, 1990, EUROPEAN CENSENSUS C, P33

← 1 2 3 →