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Aims: To examine the effect of ticlopidine administration on the activities CYP2C19 and CYP3 A in vivo using omeprazole as a model substrate.

Methods: A single dose of 40 mg omeprazole was administered orally with or without ticlopidine (300 mg daily for 6 days) to six Japanese extensive metabolisers with respect to CYP2C19. Blood samples were taken for the measurement of plasma concentrations of omeprazole, 5-hydroxyomeprazole and omeprazole sulphone.

Results: Ticlopidine administration increased omeprazole Cmax (1978 /- 859/3442 /- 569 (control phase/ticlopidine phase, nM)) and decreased the oral clearance of omeprazole (CL/F; 25.70 /- 16.17/10.76 /- 1.16 (control phase/ticlopidine phase, 1 h-1)) significantly. The 5-hydroxyomeprazole to omeprazole AUC ratio (0.817 /- 0.448/0.236 /- 0.053 (control phase/ticlopidine phase)) and the 5-hydroxyomeprazole to omeprazole sulphone AUC ratio (1.114 /- 0.782/0.256 /- 0.051 (control phase/ticlopidine phase)) were decreased significantly after ticlopidine administration. The decrease in omeprazole CL/F and the 5-hydroxyomeprazole to omeprazole AUC ratio correlated significantly with their respective absolute values when the drug was given alone. The decrease in CL/F following ticlopidine administration correlated with that in the 5-hydroxyomeprazole to omeprazole AUC ratio.

Conclusions: These findings suggest that ticlopidine inhibited the in vivo activity of CYP2C19, but not, or to a lesser extent CYP3 A4, and that the magnitude of inhibition by ticlopidine is related to the in vivo activity of CYP2C19 before inhibition.

(C) 1999 Blackwell Science Ltd.