Effect of various potential inhibitors, activators and inducers on the N-oxidation of isomeric aromatic diazines in vitro using rabbit liver microsomal preparations
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Altuntas, TG
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UNIV LONDON KINGS COLL,CHELSEA DEPT PHARM,LONDON SW3 6LX,ENGLANDUNIV LONDON KINGS COLL,CHELSEA DEPT PHARM,LONDON SW3 6LX,ENGLAND
Altuntas, TG
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]
Gorrod, JW
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UNIV LONDON KINGS COLL,CHELSEA DEPT PHARM,LONDON SW3 6LX,ENGLANDUNIV LONDON KINGS COLL,CHELSEA DEPT PHARM,LONDON SW3 6LX,ENGLAND
Gorrod, JW
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[1] UNIV LONDON KINGS COLL,CHELSEA DEPT PHARM,LONDON SW3 6LX,ENGLAND
1. The effects of various potential inhibitors, activators and inducers on the N-oxidation of isomeric aromatic diazines (pyrazine, pyrimidine and pyridazine) by rabbit liver microsomes have been studied. 2. 2,4-Dichloro-6-phenylphenoxyethylamine (DPEA), SKF 525-A and N-octylamine decreased N-oxide formation at 10(-4) M concentrations. 3. Methimazole and carbon monoxide inhibited the N-oxidation of all three substrates studied. 4. The inhibitory effects were generally exaggerated when hepatic microsomal preparations from phenobarbitone-pretreated animals were used as enzyme source. 5. When phenobarbitone or pyridine mere used as inducing agents, the N-oxidation of isomeric aromatic diazines showed considerable induction, whereas beta-naphthoflavone and Arochlor 1254 pretreatment had much weaker effects. 6. It is suggested that P4502E1 and/or 2B are the major subfamilies of P450 involved in the N-oxidation of isomeric diazines.
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页码:9 / 15
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Altuntas T. G., 1994, PHARM SCI COMMUN, V4, P117