抗凝血药物遗传学。

Anders Rane, Jonatan D Lindh
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引用次数: 19

摘要

华法林、阿昔诺可豆酚和苯丙酚是世界上主要的抗凝血药物。由于其治疗指数低、不良反应严重、应用广泛,且具有不同的动力学和药物遗传依赖性,因此探索在常规INR测量之外预测剂量的进一步可能性具有重要意义。在这里,我们详细描述了这些药物对动力学的相对药理学影响,遗传风险群体的群体分布,以及影响剂量需求和不良反应风险的临床特征的新数据。在开始治疗之前和之后不久的遗传信息的有用性也进行了讨论。目前对这些问题的重新关注不仅是因为新的遗传知识和基因分型设施,而且还因为严重不良反应的发生率很高。这些措施在抗凝治疗患者护理中的应用是重要的,等待新的治疗原则的引入,这可能需要很长时间。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Pharmacogenetics of anticoagulants.

Warfarin, acenocoumarol, and phenprocoumon are among the major anticoagulant drugs worldwide. Because of their low therapeutic index and serious adverse reactions (ADRs), their wide use, and their varying kinetics and pharmacogenetic dependence, it is of great importance to explore further possibilities to forecast the dose beyond conventional INR measurements. Here, we describe particulars of the relative pharmacogenetic influence on the kinetics of these agents, the population distribution of genetics risk groups, and novel data on clinical features with influence on dose requirement and ADR risk. The usefulness of genetic information prior to and soon after start of therapy is also discussed. The current renewed focus on these issues is caused not only because of new genetic knowledge and genotyping facilities but also because of the high rate of serious ADRs. Application of these measures in the care of patients with anticoagulant therapy is important awaiting new therapeutic principles to be introduced, which may take long time still.

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