CYP4F2 genetic variant alters required warfarin dose

Michael D. Caldwell(Marshfield Clinic), Tarif Awad, Julie A. Johnson(University of Florida), Brian F. Gage(Washington University in St. Louis), Mat Falkowski, Paul J. Gardina, Jason Hubbard, Yaron Turpaz, Taimour Langaee(University of Florida), Charles Eby(Washington University in St. Louis), Cristi R. King(Washington University in St. Louis), Amy Brower(Third Wave Systems (United States)), John R. Schmelzer(Marshfield Clinic), Ingrid Glurich(Marshfield Clinic), Humberto Vidaillet, Steven H. Yale(Marshfield Clinic), Kai Qi Zhang(Marshfield Clinic), Richard L. Berg(Marshfield Clinic), James K. Burmester(Marshfield Clinic)
Blood
February 4, 2008
Cited by 522Open Access
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Abstract

Warfarin is an effective, commonly prescribed anticoagulant used to treat and prevent thrombotic events. Because of historically high rates of drug-associated adverse events, warfarin remains underprescribed. Further, interindividual variability in therapeutic dose mandates frequent monitoring until target anticoagulation is achieved. Genetic polymorphisms involved in warfarin metabolism and sensitivity have been implicated in variability of dose. Here, we describe a novel variant that influences warfarin requirements. To identify additional genetic variants that contribute to warfarin requirements, screening of DNA variants in additional genes that code for drug-metabolizing enzymes and drug transport proteins was undertaken using the Affymetrix drug-metabolizing enzymes and transporters panel. A DNA variant (rs2108622; V433M) in cytochrome P450 4F2 (CYP4F2) was associated with warfarin dose in 3 independent white cohorts of patients stabilized on warfarin representing diverse geographic regions in the United States and accounted for a difference in warfarin dose of approximately 1 mg/day between CC and TT subjects. Genetic variation of CYP4F2 was associated with a clinically relevant effect on warfarin requirement.


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