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基因变异,尤其是 CYP2C9 和 VKORC1,对华法林药理学的影响。

Effect of genetic variants, especially CYP2C9 and VKORC1, on the pharmacology of warfarin.

机构信息

Section of Cardiology, Heart & Vascular Center, Lebanon, New Hampshire 03756, USA.

出版信息

Semin Thromb Hemost. 2012 Nov;38(8):893-904. doi: 10.1055/s-0032-1328891. Epub 2012 Oct 6.

Abstract

The genes encoding the cytochrome P450 2C9 enzyme (CYP2C9) and vitamin K-epoxide reductase complex unit 1 (VKORC1) are major determinants of anticoagulant response to warfarin. Together with patient demographics and clinical information, they account for approximately one-half of the warfarin dose variance in individuals of European descent. Recent prospective and randomized controlled trial data support pharmacogenetic guidance with their use in warfarin dose initiation and titration. Benefits from pharmacogenetics-guided warfarin dosing have been reported to extend beyond the period of initial dosing, with supportive data indicating benefits to at least 3 months. The genetic effects of VKORC1 and CYP2C9 in African and Asian populations are concordant with those in individuals of European ancestry; however, frequency distribution of allelic variants can vary considerably between major populations. Future randomized controlled trials in multiethnic settings using population-specific dosing algorithms will allow us to further ascertain the generalizability and cost-effectiveness of pharmacogenetics-guided warfarin therapy. Additional genome-wide association studies may help us to improve and refine dosing algorithms and potentially identify novel biological pathways.

摘要

细胞色素 P450 2C9 酶(CYP2C9)和维生素 K 环氧化物还原酶复合物亚单位 1(VKORC1)的基因是华法林抗凝反应的主要决定因素。这些基因与患者的人口统计学和临床信息一起,可解释欧洲血统个体中约一半的华法林剂量差异。最近的前瞻性和随机对照试验数据支持在华法林剂量起始和滴定中使用药物遗传学指导。药物遗传学指导华法林剂量的获益不仅局限于初始剂量阶段,有支持性数据表明至少 3 个月的获益。VKORC1 和 CYP2C9 的遗传效应在非洲和亚洲人群与欧洲血统个体中一致;然而,等位基因变异的频率分布在主要人群之间差异很大。在使用人群特异性剂量算法的多民族环境中进行未来的随机对照试验,将使我们能够进一步确定药物遗传学指导的华法林治疗的普遍性和成本效益。全基因组关联研究可能有助于我们改进和完善剂量算法,并可能确定新的生物学途径。

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