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Impact of GGCX STX1B and FPGS Polymorphisms on Warfarin Dose Requirements in European‐Americans and Egyptians

机译:GGCXSTX1B和FPGS多态性对欧美人和埃及人中华法林剂量需求的影响

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摘要

Genotype‐based algorithms that include VKORC1 and CYP2C9 genotypes are less predictive of warfarin dose variability in Africans as opposed to Europeans. Polymorphisms in GGCX, FPGS, or STX1B are associated with warfarin dose requirements in African‐Americans. We sought to determine if they influenced warfarin dose in European‐Americans, and another African population, specifically Egyptians. We genotyped 529 adults (n = 325 European‐Americans, 204 Egyptians) on a stable warfarin dose for GGCX rs12714145 and rs10654848, FPGS rs7856096, and STX1B rs4889606. Rs12714145, rs10654848, and rs7856096 were not associated with warfarin dose, whereas STX1B rs4889606 was a significant determinant in univariate analysis (P < 0.0001) in both cohorts. However, STX1B rs4889606 was in high linkage disequilibrium with VKORC1‐1639 G>A, and was no longer significant after including VKORC1‐1639 G>A in the regression model. Based on these data, the polymorphisms do not appear to influence, in a clinically important way, warfarin dose requirements in European‐Americans and Egyptians.
机译:与欧洲人相比,包括VKORC1和CYP2C9基因型的基于基因型的算法对华法林剂量变异性的预测较少。 GGCX,FPGS或STX1B中的多态性与非裔美国人的华法林剂量需求有关。我们试图确定它们是否影响了欧美人和另一非洲人口(特别是埃及人)中的华法林剂量。我们以稳定的华法林剂量对529名成人(n = 325名欧洲裔美国人,204名埃及人)进行了基因分型,分别用于GGCX rs12714145和rs10654848,FPGS rs7856096和STX1B rs4889606。 Rs12714145,rs10654848和rs7856096与华法林剂量无关,而STX1B rs4889606在这两个队列的单变量分析中是重要的决定因素(P <0.0001)。但是,STX1B rs4889606与VKORC1-1639 G> A处于高度连锁不平衡状态,在将VKORC1-1639 G> A包含在回归模型中之后不再显着。根据这些数据,多态性似乎并没有以临床上重要的方式影响欧美人和埃及人的华法林剂量需求。

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