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Vol. 28, Issue 11, 1284-1290, November 2000
Department of Pharmacology, University of Maastricht, the
Netherlands (H.H.T.); and the Department of Biochemie Pharmacologique
et Metabolique, Université René Descartes, Paris, France
(J.-P.F., P.H.B.)
The oral anticoagulant acenocoumarol is given as a racemic mixture.
The (S)-enantiomer is rapidly cleared and is the reason why only (R)-acenocoumarol contributes to the
pharmacological effect. The objective of the study was to establish the
cytochrome P450 (CYP) enzymes catalyzing the hydroxylations of the
acenocoumarol enantiomers. Of various cDNA-expressed human CYPs, only
CYP2C9 hydroxylated (S)-acenocoumarol. Hydroxylation
occurred at the 6-, 7-, and 8-position with equal
Km values and a ratio of 0.9:1:0.1 for
Vmax. CYP2C9 also mediated the 6-, 7-, and
8-hydroxylations of (R)-acenocoumarol with
Km values three to four times and
Vmax values one-sixth times those of
(S)-acenocoumarol. (R)-Acenocoumarol was
also metabolized by CYP1A2 (6-hydroxylation) and CYP2C19 (6-, 7-, and
8-hydroxylation). In human liver microsomes one enzyme only catalyzed
(S)-acenocoumarol hydroxylations with
Km values < 1 µM. In most of the
samples tested the 7-hydroxylation of (R)-acenocoumarol was also catalyzed by one enzyme only. The 6-hydroxylation was catalyzed by at least two enzymes. Sulfaphenazole could completely inhibit in a competitive way the hydroxylations of
(S)-acenocoumarol and the 7-hydroxylation of
(R)-acenocoumarol. The 6-hydroxylation of
(R)-acenocoumarol could be partially inhibited by
sulfaphenazole, 40 to 50%, and by furafylline, 20 to 30%. Significant
mutual correlations were obtained between the hydroxylations of
(S)-acenocoumarol, the 7-hydroxylation of
(R)-acenocoumarol, the 7-hydroxylation of
(S)-warfarin, and the methylhydroxylation of
tolbutamide. The results demonstrate that
(S)-acenocoumarol is hydroxylated by a single enzyme,
namely CYP2C9. CYP2C9 is also the main enzyme in the 7-hydroxylation of
(R)-acenocoumarol. Other enzymes involved in
(R)-acenocoumarol hydroxylation reactions are CYP1A2 and
CYP2C19. Drug interactions must be expected, particularly for drugs
interfering with CYP2C9. Also, drugs interfering with CYP1A2 and
CYP2C19 may potentiate acenocoumarol anticoagulant therapy.
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