Kimura Rina, Miyashita Kotaro, Kokubo Yoshihiro, Akaiwa Yasuhisa, Otsubo Ryoichi, Nagatsuka Kazuyuki, Otsuki Toshiho, Okayama Akira, Minematsu Kazuo, Naritomi Hiroaki, Honda Shigenori, Tomoike Hitonobu, Miyata Toshiyuki
Research Institute, Japan.
Thromb Res. 2007;120(2):181-6. doi: 10.1016/j.thromres.2006.09.007. Epub 2006 Oct 17.
The dose required for the anticoagulant effect of warfarin exhibits large inter-individual variations. This study sought to determine the contribution of four genes, vitamin K epoxide reductase (VKORC1), gamma-glutamyl carboxylase (GGCX), calumenin (CALU), and cytochrome P450 2C9 (CYP2C9) to the warfarin maintenance dose required in Japanese patients following ischemic stroke. We recruited 93 patients on stable anticoagulation with a target International Normalized Ratio (INR) of 1.6-2.6. We genotyped eleven representative single nucleotide polymorphisms (SNPs) in the three genes involved in vitamin K cycle and the 42613A>C SNP in CYP2C9, known as CYP2C93, and then examined an association of these genotypes with warfarin maintenance doses (mean+/-SD=2.96+/-1.06 mg/day). We found an association of effective warfarin dose with the -1639G>A (p=0.004) and 3730G>A genotypes (p=0.006) in VKORC1, the 8016G>A genotype in GGCX (p=0.022), and the 42613A>C genotype in CYP2C9 (p=0.015). The model using the multiple regression analysis including age, sex, weight, and three genetic polymorphisms accounted for 33.3% of total variations in warfarin dose. The contribution to inter-individual variation in warfarin dose was 5.9% for VKORC1 -1639G>A, 5.2% for CYP2C9 42613A>C, and 4.6% for GGCX 8016G>A. In addition to polymorphisms in VKORC1 and CYP2C9, we identified GGCX 8016G>A, resulting in the missense mutation R325Q, as a genetic determinant of warfarin maintenance dose in Japanese patients.
华法林产生抗凝作用所需的剂量存在很大的个体差异。本研究旨在确定维生素K环氧化物还原酶(VKORC1)、γ-谷氨酰羧化酶(GGCX)、钙网蛋白(CALU)和细胞色素P450 2C9(CYP2C9)这四个基因对日本缺血性中风患者所需华法林维持剂量的影响。我们招募了93名接受稳定抗凝治疗的患者,目标国际标准化比值(INR)为1.6 - 2.6。我们对参与维生素K循环的三个基因中的11个代表性单核苷酸多态性(SNP)以及CYP2C9中已知的42613A>C SNP(称为CYP2C9*3)进行了基因分型,然后检查这些基因型与华法林维持剂量(平均值±标准差 = 2.96±1.06毫克/天)之间的关联。我们发现有效华法林剂量与VKORC1中的 - 1639G>A(p = 0.004)和3730G>A基因型(p = 0.006)、GGCX中的8016G>A基因型(p = 0.022)以及CYP2C9中的42613A>C基因型(p = 0.015)存在关联。使用包括年龄、性别、体重和三种基因多态性的多元回归分析模型解释了华法林剂量总变异的33.3%。VKORC1 - 1639G>A对华法林剂量个体间变异的贡献为5.9%,CYP2C9 42613A>C为5.2%,GGCX 8016G>A为4.6%。除了VKORC1和CYP2C9中的多态性外,我们还确定GGCX 8016G>A(导致错义突变R325Q)是日本患者华法林维持剂量的遗传决定因素。
