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华法林剂量算法中遗传因素和非遗传因素的应用。

Use of genetic and nongenetic factors in warfarin dosing algorithms.

作者信息

Wu Alan H B

机构信息

University of California, San Francisco, Department of Laboratory Medicine, Clinical Chemistry Laboratory, San Francisco General Hospital, 1001 Potrero Avenue, San Francisco, CA 94110, USA.

出版信息

Pharmacogenomics. 2007 Jul;8(7):851-61. doi: 10.2217/14622416.8.7.851.

Abstract

Despite the fact that warfarin has been used as an anticoagulant for many years, the safety profile for this drug has been poor. Inappropriate dosing continues to contribute to significant morbidity and mortality due to thrombotic disease and bleeding. Therefore, there is a need for the development, characterization and implementation of dosing algorithms using a patient's demographic information and genotype. Recently, polymorphisms in two genes, cytochrome P450 2C9 and vitamin K epoxide reductase complex 1, have been shown to affect warfarin's pharmacogenomics and pharmacodynamics, respectively. Adding genotypes to a dosing algorithm may enable better prediction of initial warfarin dosing than use of demographic data alone. An advisory committee of the US FDA voted on November 14, 2005, to require manufacturers of warfarin to relabel their product, indicating that genotyping is recommended prior to drug administration. The exact date when this recommendation will be enacted remains to be determined. Successful implementation of pharmacogenomics into clinical practice requires genotyping results that can be translated directly into clinical decisions. The development of a warfarin dosing algorithm that includes genotyping may be the means to achieve this goal.

摘要

尽管华法林作为一种抗凝剂已使用多年,但该药物的安全性一直不佳。由于血栓形成性疾病和出血,剂量不当持续导致显著的发病率和死亡率。因此,需要利用患者的人口统计学信息和基因型来开发、表征和实施给药算法。最近研究表明,细胞色素P450 2C9和维生素K环氧化物还原酶复合体1这两个基因的多态性分别影响华法林的药物基因组学和药效学。在给药算法中加入基因型可能比仅使用人口统计学数据能更好地预测华法林的初始剂量。美国食品药品监督管理局(FDA)的一个咨询委员会于2005年11月14日投票,要求华法林制造商重新标注其产品,表明建议在给药前进行基因分型。该建议的确切实施日期仍有待确定。将药物基因组学成功应用于临床实践需要能够直接转化为临床决策的基因分型结果。开发包含基因分型的华法林给药算法可能是实现这一目标的手段。

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