Abstract

Deep abdominal vein thrombosis is extremely rare among thrombotic events secondary to the use of contraceptives. A case to illustrate the clinical utility of ethno-specific pharmacogenetic testing in warfarin management of a Hispanic patient is reported. A 37-year-old Hispanic Puerto Rican, non-gravid female with past medical history of abnormal uterine bleeding on hormonal contraceptive therapy was evaluated for abdominal pain. Physical exam was remarkable for unspecific diffuse abdominal tenderness, and general initial laboratory results—including coagulation parameters—were unremarkable. A contrast-enhanced computed tomography showed a massive thrombosis of the main portal, splenic, and superior mesenteric veins. On admission the patient was started on oral anticoagulation therapy with warfarin at 5 mg/day and low-molecular-weight heparin. The prediction of an effective warfarin dose of 7.5 mg/day, estimated by using a recently developed pharmacogenetic-guided algorithm for Caribbean Hispanics, coincided with the actual patient’s warfarin dose to reach the international normalized ratio target. We speculate that the slow rise in patient’s international normalized ratio observed on the initiation of warfarin therapy, the resulting high risk for thromboembolic events, and the required warfarin dose of 7.5 mg/day are attributable in some part to the presence of the NQO1*2 (g.559C>T, p.P187S) polymorphism, which seems to be significantly associated with resistance to warfarin in Hispanics. By adding genotyping results of this novel variant, the predictive model can inform clinicians better about the optimal warfarin dose in Caribbean Hispanics. The results highlight the potential for pharmacogenetic testing of warfarin to improve patient care.

Highlights

  • Warfarin (Coumadin) is an oral anticoagulant drug that inhibits the vitamin K–dependent clothing factors

  • A recently developed admixture-adjusted pharmacogenetic algorithm for Caribbean Hispanics is applied to a patient carrying a loss of function NQO1*2 (g.559C>T, p.P187S) polymorphism, which seems to be significantly associated with resistance to warfarin in this population

  • We introduced for the first time genetic information to guide the anticoagulation therapy in a Hispanic female with an atypical thrombosis

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Summary

Introduction

Warfarin (Coumadin) is an oral anticoagulant drug that inhibits the vitamin K–dependent clothing factors. The patient mentioned having been evaluated by gynecology service a month ago, and she was started on medroxyprogesterone acetate (Provera, Pfizer, New York, NY), she just used the medication for 10 days She underwent endometrial curettage procedure and biopsy with no further complications a week before starting with symptoms. The patient was initiated on oral warfarin at 5 mg/day following dose recommendations in clinical charts (nomograms) and current American College of Chest Physicians guidelines.[13,14] The baseline INR value on admission was 0.9 (Table 1). Following the pharmacogenetic-driven algorithm recommendations, the patient was prescribed warfarin at the dose of 7.5 mg/day for further prevention of thrombus formation. She was kept on this dose until discharge when she reported 2 continue INR values on therapeutic range. Period, the patient reported 2 bruises (one in the calves and the other in the thighs) on weeks 2 to 4, moderate palpitations and dark stools on week 3, chest pain on weeks 3 and 4 and weeks 11 and 12, as well as recurrent fatigue, weakness, anxiety, and discomfort

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