细胞色素P450同工酶CYP2C9和维生素K环氧化物还原酶复合体亚基1的基因型共同决定华法林稳定剂量:一项前瞻性研究。
Genotypes of the cytochrome p450 isoform, CYP2C9, and the vitamin K epoxide reductase complex subunit 1 conjointly determine stable warfarin dose: a prospective study.
作者信息
Carlquist John F, Horne Benjamin D, Muhlestein Joseph B, Lappé Donald L, Whiting Bryant M, Kolek Matthew J, Clarke Jessica L, James Brent C, Anderson Jeffrey L
机构信息
Department of Medicine, Division of Cardiology, University of Utah School of Medicine, Cardiovascular Department, LDS Hospital, Salt Lake City, Utah, USA.
出版信息
J Thromb Thrombolysis. 2006 Dec;22(3):191-7. doi: 10.1007/s11239-006-9030-7.
BACKGROUND
Warfarin has a narrow therapeutic range and wide inter-individual dosing requirements that may be related to functional variants of genes affecting warfarin metabolism (i.e., CYP2C9) and activity (i.e., vitamin K epoxide reductase complex subunit 1-VKORC1). We hypothesized that variants in these two genes explain a substantial proportion of variability in stable warfarin dose and could be used as a basis for improved dosing algorithms.
METHODS
Consecutive consenting outpatients (n = 213) with stable INR (2-3) for >1 month were enrolled. Buccal DNA was extracted using a Qiagen mini-column and CYP2C92 and VKORC1 genotyping performed by the Taqman 3' nuclease assay. Sequencing for CYP2C93, genotyping was done using Big Dye v3.1 terminator chemistry Dose by genotype was assessed by linear regression.
RESULTS
Weekly warfarin dose averaged 30.8 +/- 13.9 mg/week; average INR was 2.42 +/- 0.72. CYP2C9*2/*3 genotype distribution was: CC/AA (wild-type [WT]) = 71.4%, CT/AA = 18.3%, CC/AC = 9.4%, and CT/AC = 1%; VKORC1 genotypes were CC (WT) = 36.6%, CT = 50.7%, and TT = 12.7%. Warfarin doses (mg/week) varied by genotype: for CYP2C9, 33.3 mg/week for WT (CC/AA), 27.2 mg/week for CT/AA (P = 0.04 vs. WT), 23.0 mg/week for CC/AC (P = 0.003), and 6.0 mg/week for CT/AC (P < 0.001), representing dose reductions of 18-31% for single and 82% for double variant carriers; for VKORC1: 38.4 mg/week for WT (CC), 28.6 mg/week for CT (P < 0.001 vs. WT), 20.95 mg/week for TT (P < 0.001). In multiple linear regression, genotype was the dominant predictor of warfarin dose (P = 2.4 x 10(-15)); weak predictors were age, weight, and sex. Genotype-based modeling explained 33% of dose-variance, compared with 12% for clinical variables alone.
CONCLUSION
In this large prospective study of warfarin genetic dose-determinants, carriage of a single or double CYP2C9 variant, reduced warfarin dose 18-72%, and of a VKORC1 variant by 65%. Genotype-based modeling explained almost one-half of dose-variance. A quantitative dosing algorithm incorporating genotypes for 2C9 and VKORC1 could substantially improve initial warfarin dose-selection and reduce related complications.
背景
华法林的治疗窗较窄,个体间给药剂量需求差异较大,这可能与影响华法林代谢的基因(如CYP2C9)功能变异以及活性(如维生素K环氧化物还原酶复合体亚基1-VKORC1)有关。我们推测这两个基因的变异可解释稳定华法林剂量变异性的很大一部分,并可作为改进给药算法的基础。
方法
纳入连续的同意参与研究的门诊患者(n = 213),其国际标准化比值(INR)稳定在2 - 3且持续超过1个月。使用Qiagen微型柱提取颊黏膜DNA,并通过Taqman 3'核酸酶测定法进行CYP2C92和VKORC1基因分型。对CYP2C93进行测序,使用Big Dye v3.1终止剂化学法进行基因分型。通过线性回归评估不同基因型的剂量。
结果
每周华法林平均剂量为30.8±13.9mg/周;平均INR为2.42±0.72。CYP2C9*2/*3基因型分布为:CC/AA(野生型[WT])= 71.4%,CT/AA = 18.3%,CC/AC = 9.4%,CT/AC = 1%;VKORC1基因型为CC(WT)= 36.6%,CT = 50.7%,TT = 12.7%。华法林剂量(mg/周)因基因型而异:对于CYP2C9,野生型(CC/AA)为33.3mg/周,CT/AA为27.2mg/周(与野生型相比P = 0.04),CC/AC为23.0mg/周(P = 0.003),CT/AC为6.0mg/周(P < 0.001),单变异携带者剂量降低18 - 31%,双变异携带者剂量降低82%;对于VKORC1:野生型(CC)为38.4mg/周,CT为28.6mg/周(与野生型相比P < 0.001),TT为20.95mg/周(P < 0.001)。在多元线性回归中,基因型是华法林剂量的主要预测因素(P = 2.4×10⁻¹⁵);年龄、体重和性别是较弱的预测因素。基于基因型的模型解释了33%的剂量变异性,而仅临床变量解释了12%。
结论
在这项关于华法林基因剂量决定因素的大型前瞻性研究中,携带单个或双个CYP2C9变异可使华法林剂量降低18 - 72%,携带VKORC1变异可使剂量降低65%。基于基因型的模型解释了近一半的剂量变异性。纳入CYP2C9和VKORC1基因型的定量给药算法可显著改善华法林初始剂量选择并减少相关并发症。
Zotero 插件