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Novel SNP in CYP2C9 is associated with changes in warfarin clearance and CYP2C9 expression levels in African Americans

机译:CYP2C9中的新型SNP与非裔美国人中华法林清除率和CYP2C9表达水平的变化有关

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摘要

Warfarin is a widely used anticoagulant whose active S-enantiomer is primarily metabolized by the CYP2C9 enzyme. The CYP2C9*2 and CYP2C9*3 alleles are associated with lower warfarin dose requirement and decreased enzyme activity. In contrast, we previously identified a novel SNP (rs7089580 A>T) in CYP2C9 that is associated with higher warfarin dose requirement in African Americans. In this study, we examine the effect of rs7089580 on warfarin pharmacokinetics and CYP2C9 expression in 63 African American patients and 32 African American liver tissues, respectively. We found oral clearance of S-warfarin to be higher among carriers of the minor rs7089580 allele (T) compared to wild type homozygotes (3.73±1.46 ml/min vs. 2.95±1.39 ml/min, p=0.04). CYP2C9 mRNA expression in liver tissue was also higher among A/T and T/T genotypes compared to A/A (p<0.02). Our findings indicate that rs7089580 is associated with higher S-warfarin clearance and CYP2C9 expression and may help explain the higher dose requirement of warfarin in African Americans. Furthermore, rs7089580 is in complete linkage disequilibrium with the promoter SNP rs12251841 in African Americans which may provide a biologically plausible explanation for the observed effect on CYP2C9 expression levels. Given the many clinically relevant substrates of CYP2C9, identifying polymorphisms that affect expression levels and metabolism across ethnicities is essential for individualization of doses with a narrow therapeutic index.
机译:华法林是一种广泛使用的抗凝剂,其活性S对映体主要通过CYP2C9酶代谢。 CYP2C9 * 2和CYP2C9 * 3等位基因与较低的华法林剂量要求和降低的酶活性有关。相反,我们先前在CYP2C9中鉴定了一种新的SNP(rs7089580 A> T),这与非洲裔美国人中较高的华法林剂量需求有关。在这项研究中,我们研究了rs7089580对华法林药代动力学和CYP2C9表达分别在63位非裔美国人和32位非裔美国人肝组织中的作用。我们发现未成年人rs7089580等位基因(T)的携带者中S-华法林的口服清除率比野生型纯合子高(3.73±1.46 ml / min对2.95±1.39 ml / min,p = 0.04)。与A / A相比,A / T和T / T基因型的肝组织中CYP2C9 mRNA的表达也较高(p <0.02)。我们的发现表明rs7089580与更高的S-华法林清除率和CYP2C9表达有关,并可能有助于解释非洲裔美国人对华法林的更高剂量需求。此外,在非洲裔美国人中,rs7089580与启动子SNP rs12251841处于完全连锁不平衡状态,这可能为观察到的对CYP2C9表达水平的影响提供生物学上合理的解释。考虑到CYP2C9的许多临床相关底物,鉴定影响多族裔表达水平和代谢的多态性对于个体化具有较窄治疗指数的剂量至关重要。

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