TY - JOUR
T1 - Identification of human liver cytochrome P450 isoforms mediating omeprazole metabolism
AU - ANDERSSON, TOMMY
AU - MINERS, JOHN O.
AU - VERONESE, MAURICE E.
AU - TASSANEEYAKUL, WICHITTRA
AU - TASSANEEYAKUL, WONGWIWAT
AU - MEYER, URS A.
AU - BIRKETT, DONALD J.
PY - 1993/12
Y1 - 1993/12
N2 - The in vitro metabolism of omeprazole was studied in human liver microsomes in order to define the metabolic pathways and identify the cytochrome P450 (CYP) isoforms responsible for the formation of the major omeprazole metabolites. The four major metabolites identified in vitro, in tentative order of importance, were hydroxyomeprazole, omeprazole sulphone, 5‐O‐desmethylomeprazole, and an unidentified compound termed metabolite X. Omeprazole pyridone was also detected but could not be quantitated. Incubation of hydroxyomeprazole and omeprazole sulphone with human microsomes resulted in both cases in formation of the hydroxysulphone. The kinetics of formation of the four primary metabolites studied were biphasic suggesting the involvement of multiple CYP isoforms in each case. Further studies used substrate concentrations at which the high affinity activities predominated. Formation of the major metabolite, hydroxyomeprazole, was significantly correlated with S‐mephenytoin hydroxylase and with benzo[a]pyrene metabolism and CYP3A content. Inhibition studies with isoform selective inhibitors also indicated a dominant role of S‐mephenytoin hydroxylase with some CYP3A contribution in the formation of hydroxyomeprazole. Correlation and inhibition data for the sulphone and metabolite X were consistent with a predominant role of the CYP3A subfamily in formation of these metabolites. Formation of 5‐O‐desmethylomeprazole was inhibited by both R, S‐mephenytoin and quinidine, indicating that both S‐mephenytoin hydroxylase and CYP2D6 may mediate this reaction in human liver microsomes and in vivo. The Vmax/Km (indicator of intrinsic clearance in vivo) for hydroxyomeprazole was four times greater than that for omeprazole sulphone. Consistent with findings in vivo, the results predict that omeprazole clearance in vivo would be reduced in poor metabolisers of mephenytoin due to reduction in the dominant partial metabolic clearance to hydroxyomeprazole. 1993 The British Pharmacological Society
AB - The in vitro metabolism of omeprazole was studied in human liver microsomes in order to define the metabolic pathways and identify the cytochrome P450 (CYP) isoforms responsible for the formation of the major omeprazole metabolites. The four major metabolites identified in vitro, in tentative order of importance, were hydroxyomeprazole, omeprazole sulphone, 5‐O‐desmethylomeprazole, and an unidentified compound termed metabolite X. Omeprazole pyridone was also detected but could not be quantitated. Incubation of hydroxyomeprazole and omeprazole sulphone with human microsomes resulted in both cases in formation of the hydroxysulphone. The kinetics of formation of the four primary metabolites studied were biphasic suggesting the involvement of multiple CYP isoforms in each case. Further studies used substrate concentrations at which the high affinity activities predominated. Formation of the major metabolite, hydroxyomeprazole, was significantly correlated with S‐mephenytoin hydroxylase and with benzo[a]pyrene metabolism and CYP3A content. Inhibition studies with isoform selective inhibitors also indicated a dominant role of S‐mephenytoin hydroxylase with some CYP3A contribution in the formation of hydroxyomeprazole. Correlation and inhibition data for the sulphone and metabolite X were consistent with a predominant role of the CYP3A subfamily in formation of these metabolites. Formation of 5‐O‐desmethylomeprazole was inhibited by both R, S‐mephenytoin and quinidine, indicating that both S‐mephenytoin hydroxylase and CYP2D6 may mediate this reaction in human liver microsomes and in vivo. The Vmax/Km (indicator of intrinsic clearance in vivo) for hydroxyomeprazole was four times greater than that for omeprazole sulphone. Consistent with findings in vivo, the results predict that omeprazole clearance in vivo would be reduced in poor metabolisers of mephenytoin due to reduction in the dominant partial metabolic clearance to hydroxyomeprazole. 1993 The British Pharmacological Society
KW - CYP isoforms
KW - human microsomal metabolism
KW - kinetics
KW - omeprazole
UR - http://www.scopus.com/inward/record.url?scp=0027145018&partnerID=8YFLogxK
U2 - 10.1111/j.1365-2125.1993.tb00410.x
DO - 10.1111/j.1365-2125.1993.tb00410.x
M3 - Article
C2 - 12959268
AN - SCOPUS:0027145018
SN - 0306-5251
VL - 36
SP - 521
EP - 530
JO - British Journal of Clinical Pharmacology
JF - British Journal of Clinical Pharmacology
IS - 6
ER -