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首页> 外文期刊>Clinical and translational science. >VKORC1 and Novel CYP2C9 Variation Predict Warfarin Response in Alaska Native and American Indian People
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VKORC1 and Novel CYP2C9 Variation Predict Warfarin Response in Alaska Native and American Indian People

机译:VKORC1和新型CYP2C9变异预测阿拉斯加本地和美洲印度人的华法林应对

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Alaska Native and American Indian (AN/AI) people have unique pharmacogene variation that may affect warfarin disposition and therapeutic response. We performed targeted genotyping for cytochrome P450 (CYP)2C9, vitamin K epoxide oxidase reductase complex subunit 1 (VKORC1), CYP4F2, CYP4F11, and gamma-glutamyl carboxylase (GGCX) variants in AN/AI people receiving warfarin. The primary outcome was stable warfarin dose, defined as one dose, and associated international normalized ratio within the target range, at least 6 months after starting therapy, with two matching doses at least 2 weeks apart. Genotype-phenotype relationships were assessed by multivariate regression analysis, adjusted for self-reported heritage, age, gender, and concurrent statin use. VKORC1 genotype explained 34% of dose variability, with VKORC1 -1639G>A and 1173C>T associated with a 1.7 mg/day (P = 1.4e-05) dose reduction. Additionally, CYP2C9 N218I was suggestively significant (P = 0.077), with heterozygotes requiring 1.1 mg/day less than reference individuals. Self-reported heritage was significantly associated with dose, largely driven by differences in the diagnostic VKORC1 allele frequencies among AN/AI people.
机译:阿拉斯加本土和美洲印第安人(AN / AI)人们具有独特的药物转基因变异,可能会影响华法林的性格和治疗反应。我们对接受华法林的人们进行了靶向基因分型(CYP)2C9,维生素K环氧化物氧化酶还原酶复合亚基1(VKORC1),CYP4F2,CYP4F11和γ-谷氨酸羧酸酯(GGCX)变体。主要结果是稳定的华法林剂量,定义为一种剂量,并在起始治疗后至少6个月内的目标范围内的相关国际标准化比例,两种匹配至少2周。通过多元回归分析评估基因型 - 表型关系,调整为自我报告的遗产,年龄,性别和并发他汀类药物使用。 VKORC1基因型解释了34%的剂量变异性,VKORC1 -1639G> A和1173C> T.与1.7mg /天(P = 1.4E-05)剂量还原相关。另外,CYP2C9 N218I略微显着(P = 0.077),杂合子需要比参考个体少1.1mg /天。自我报告的遗产与剂量显着相关,主要是由人类诊断vkorc1等位基因频率的差异驱动。

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