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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Pharmacogenetic relevance of CYP4F2 V433M polymorphism on acenocoumarol therapy.
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Pharmacogenetic relevance of CYP4F2 V433M polymorphism on acenocoumarol therapy.

机译:CYP4F2 V433M多态性与乙酰香豆酚治疗的药物遗传学相关性。

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VKORC1 and CYP2C9 polymorphisms are used to predict the safe dose of oral anticoagulant therapy. A new variant of CYP4F2 (V433M) has recently been related to the required warfarin dose. We evaluated its influence in earliest response to acenocoumarol in 100 selected men who started anticoagulation (3 mg for 3 consecutive days). V433M genotype exerted a gene dosage-dependent effect on the decrease of factors II, VII, IX, and X in the earliest response to acenocoumarol, with homozygous 433V subjects being the most sensitive. Similarly, after the initiation of therapy, international normalized ratio also experienced a gene dosage-dependent effect (P = .015), and 433V subjects needed 4 mg/week less than 433M carriers to achieve a steady anticoagulation (P = .043). Multivariate linear regression analysis revealed a significant contribution of V433M polymorphism to variability of both early international normalized ratio value (R(2) = 0.14) and dose requirements (R(2) = 0.19). Our data underline the relevant role of CYP4F2 V433M polymorphism in the pharmacogenetics of coumarin anticoagulants.
机译:VKORC1和CYP2C9多态性用于预测口服抗凝治疗的安全剂量。 CYP4F2(V433M)的新变体最近与所需的华法林剂量有关。我们在100名开始抗凝治疗的男性(连续3天服用3毫克)中评估了其对乙酰香豆酚最早反应的影响。 V433M基因型在对乙酰香豆酚的最早反应中对II,VII,IX和X因子的减少发挥了基因剂量依赖性作用,其中纯合性433V受试者最敏感。同样,开始治疗后,国际标准化比率也经历了基因剂量依赖性效应(P = .015),并且433V受试者需要比433M携带者少4 mg /周的剂量才能实现稳定的抗凝(P = .043)。多元线性回归分析显示V433M多态性对早期国际标准化比率值(R(2)= 0.14)和剂量要求(R(2)= 0.19)的变异性有重大贡献。我们的数据强调了CYP4F2 V433M多态性在香豆素抗凝剂的药物遗传学中的相关作用。

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