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STRATEGIES FOR EQUITABLE PHARMACOGENOMIC-GUIDED WARFARIN DOSING AMONG EUROPEAN AND AFRICAN AMERICAN INDIVIDUALS IN A CLINICAL POPULATION

机译:在欧洲和非洲人群中以药代动力学指导的华法林剂量的策略

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摘要

The blood thinner warfarin has a narrow therapeutic range and high inter- and intra-patient variability in therapeutic doses. Several studies have shown that pharmacogenomic variants help predict stable warfarin dosing. However, retrospective and randomized controlled trials that employ dosing algorithms incorporating pharmacogenomic variants under perform in African Americans. This study sought to determine if: 1) including additional variants associated with warfarin dose in African Americans, 2) predicting within single ancestry groups rather than a combined population, or 3) using percentage African ancestry rather than observed race, would improve warfarin dosing algorithms in African Americans. Using BioVU, the Vanderbilt University Medical Center biobank linked to electronic medical records, we compared 25 modeling strategies to existing algorithms using a cohort of 2,181 warfarin users (1,928 whites, 253 blacks). We found that approaches incorporating additional variants increased model accuracy, but not in clinically significant ways. Race stratification increased model fidelity for African Americans, but the improvement was small and not likely to be clinically significant. Use of percent African ancestry improved model fit in the context of race misclassification.
机译:血液稀释剂华法令具有较窄的治疗范围,且治疗剂量之间的患者间和患者内差异很大。几项研究表明,药物基因组学变异有助于预测稳定的华法林剂量。但是,回顾性和随机对照试验采用了结合了药物基因组变异体的给药算法,在非洲裔美国人中正在进行。这项研究试图确定:1)在非裔美国人中包括与华法林剂量有关的其他变体,2)在单个祖先组而不是在合并的人群中进行预测,或3)使用非洲祖先百分比而不是所观察到的种族,是否会改善华法林的给药算法在非洲裔美国人中。使用BioVU(范德比尔特大学医学中心与电子病历链接的生物库),我们使用2,181名华法林使用者(1,928名白人,253名黑人)对25种建模策略与现有算法进行了比较。我们发现,结合其他变体的方法可以提高模型的准确性,但在临床上却不重要。种族分层提高了非裔美国人的模型保真度,但是这种改善很小,而且在临床上不太可能具有重大意义。在种族分类错误的情况下,使用非洲血统百分比改善了模型拟合。

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