Clinical Application of Pharmacogenetic-Based Warfarin-Dosing Algorithm in Patients of Han Nationality after Rheumatic Valve Replacement: A Randomized and Controlled Trial

MingSong Wang; XiLong Lang; ShiTao Cui; Ke Fei; LiangJian Zou; Jia Cao; LiangXu Wang; ShengHui Zhang; XinTian Wu; YiLing Wang; Qiang Ji

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Clinical Application of Pharmacogenetic-Based Warfarin-Dosing Algorithm in Patients of Han Nationality after Rheumatic Valve Replacement: A Randomized and Controlled Trial

机译：基于药物遗传学的华法林剂量算法在风湿性瓣膜置换术后汉族患者中的临床应用：一项随机对照试验

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Background The polymorphisms of VKORC1 and CYP2C9 play increasingly important roles in the inter-individual variability in warfarin dose. This study aimed to evaluate the feasibility of clinical application of pharmacogenetic-based warfarin-dosing algorithm in patients of Han nationality with rheumatic heart disease after valve replacement in a randomized and controlled trial. Methods One hundred and one consecutive patients of Han nationality with rheumatic heart disease undergoing valve surgery were enrolled and randomly assigned to an experimental group (n=50, based on CYP2C9 and VKORC1 genotypes, pharmacogenetic-based “predicted warfarin dose” for 3 days and then was adjusted to INR until stable warfarin maintenance dose) or a control group (n=51, 2.5mg/d for 3 days and then was adjusted to INR until stable warfarin maintenance dose). All included patients were followed for 50 days after initiation of warfarin therapy. The primary end-point was the time to reach a stable warfarin maintenance dose. Results During the follow-up, 84.0% patients in the experimental group and 58.8% patients in the control group received warfarin maintenance dose. Compared with control group, patients in the experimental group had shorter mean time elapse from initiation of warfarin therapy until warfarin maintenance dose (27.5±1.8 d versus 34.7±1.8 d, pConclusion: Based on CYP2C9 and VKORC1 genotypes, the pharmacogenetic-based warfarin-dosing algorithm may shorten the time elapse from initiation of warfarin therapy until warfarin maintenance dose. It is feasible for the clinical application of the pharmacogenetic-based warfarin-dosing algorithm in patients of Han nationality with rheumatic heart disease after valve replacement.

机译：背景VKORC1和CYP2C9的多态性在华法林剂量的个体间差异中起越来越重要的作用。这项研究旨在通过随机对照试验评估基于药物遗传学的华法林剂量算法在汉族风湿性心脏病患者瓣膜置换后临床应用的可行性。方法选取连续接受瓣膜手术的汉族风湿性心脏病病人110例，随机分为实验组（n = 50，基于CYP2C9和VKORC1基因型，基于药物遗传学的“华法林预测剂量”），并进行实验。然后将其调整为INR，直至达到稳定的华法林维持剂量）或对照组（n = 51，2.5mg / d，持续3天，然后调整为INR，直到达到稳定的华法林维持剂量）。开始华法林治疗后，对所有纳入的患者进行随访50天。主要终点是达到稳定的华法林维持剂量的时间。结果随访期间，实验组84.0％的患者和对照组中58.8％的患者接受了华法林维持剂量。与对照组相比，实验组患者从开始华法林治疗到华法林维持剂量的平均时间较短（27.5±1.8 d对34.7±1.8 d，p）。结论：基于CYP2C9和VKORC1基因型，基于药物遗传学的华法林-给药算法可以缩短从开始使用华法林治疗到维持华法林剂量的时间，这对于在汉族患有风湿性心脏病的患者更换瓣膜后使用基于药理遗传学的华法林给药算法是可行的。

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《International Journal of Medical Sciences 》 |2012年第6期| 共8页
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MingSong Wang; XiLong Lang; ShiTao Cui; Ke Fei; LiangJian Zou; Jia Cao; LiangXu Wang; ShengHui Zhang; XinTian Wu; YiLing Wang; Qiang Ji;
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Clinical Application of Pharmacogenetic-Based Warfarin-Dosing Algorithm in Patients of Han Nationality after Rheumatic Valve Replacement: A Randomized and Controlled Trial

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