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CYP2C9 genotype-guided warfarin prescribing enhances the efficacy and safety of anticoagulation: a prospective randomized controlled study.

机译:CYP2C9基因型指导的华法林处方可增强抗凝疗效和安全性:一项前瞻性随机对照研究。

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摘要

Warfarin anticoagulation effect is characterized by marked variability, some of which has been attributed to CYP2C9 polymorphisms. This study prospectively examines whether a priori knowledge of CYP2C9 genotype may improve warfarin therapy. Patients were randomly assigned to receive warfarin by a validated algorithm ("control", 96 patients) or CYP2C9 genotype-adjusted algorithms ("study", 95 patients). The first therapeutic international normalized ratio and stable anticoagulation were reached 2.73 and 18.1 days earlier in the study group, respectively (P<0.001). The faster rate of initial anticoagulation was driven by a 28% higher daily dose in the study group (P<0.001). Study group patients spent more time within the therapeutic range (80.4 vs 63.4%, respectively, P<0.001) and experienced less minor bleeding (3.2 vs 12.5%, P<0.02, respectively). In conclusion, CYP2C9 genotype-guided warfarin therapy is more efficient and safer than the "average-dose" protocol. Future research should focus on construction of algorithms that incorporate other polymorphisms (VKORC1), host factors, and environmental influences.
机译:华法林抗凝作用的特征在于明显的变异性,其中一些归因于CYP2C9多态性。这项研究前瞻性检查了CYP2C9基因型的先验知识是否可以改善华法林治疗。通过验证的算法(“对照组”,96例患者)或经CYP2C9基因型调整的算法(“研究”,95例患者)将患者随机分配接受华法林治疗。在研究组中,第一个治疗国际标准化比率和稳定的抗凝治疗分别提前了2.73天和18.1天(P <0.001)。在研究组中,日剂量增加28%驱使初始抗凝的速度更快(P <0.001)。研究组患者在治疗范围内花费的时间更多(分别为80.4和63.4%,P <0.001),较少的轻微出血(分别为3.2和12.5%,P <0.02)。总之,CYP2C9基因型指导的华法林治疗比“平均剂量”方案更有效,更安全。未来的研究应着重于构建包含其他多态性(VKORC1),宿主因素和环境影响的算法。

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