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CYP2C19基因多态性与首发缺血性卒中氯吡格雷二级预防复发风险的关联研究
引用本文:曾涛,肖旋浩,徐邦牢,雷秀霞,李泽,周进,黄翚,潘小平.CYP2C19基因多态性与首发缺血性卒中氯吡格雷二级预防复发风险的关联研究[J].中国卒中杂志,2018,13(9):908-914.
作者姓名:曾涛  肖旋浩  徐邦牢  雷秀霞  李泽  周进  黄翚  潘小平
作者单位:1510180.广州市第一人民医院神经内科;2.广州市第一人民医院检验科
基金项目:广州市科技计划项目(2016201604030) 广东省自然科学基金项目(2014A030310093) 广东省医学科学技术研究基金(A2017249)
摘    要:目的探讨CYP2C19基因多态性与规律服用氯吡格雷预防缺血性卒中二级复发风险之间的关系。方法入组首次缺血性卒中的326例汉族患者,采用DNA微阵列芯片法检测CYP2C19基因多态性,随访患者缺血性卒中复发情况,分析规律服用氯吡格雷的患者卒中复发与CYP2C19基因多态性的关系。结果对入组患者经过1~37个月平均(14.44±5.07)个月]的随访,共139例规律服用氯吡格雷,其中29(20.86%)例出现卒中复发。中代谢型和慢代谢型患者的复发风险较快代谢型升高,比值比(odds ratio,OR)分别为3.0595%可信区间(confidence interval,CI)1.11~8.43,P=0.025]和9.17(95%CI2.39~35.16,P0.001]。携带*2(G681A)A等位基因患者的卒中复发风险是携带G等位基因患者的2.63倍(P0.001)。携带*2突变杂合子和纯合子患者卒中复发风险分别是野生型的2.82倍(P=0.026)和9.69倍(P0.001)。携带有1个失功能(loss of function,LOF)等位基因者卒中复发的风险是未携带者的3.02倍,(95%CI 1.13~8.05,P=0.030),携带2个LOF等位基因者卒中复发的风险是未携带者的11.01倍(95%CI 2.67~45.24,P0.001)。多因素Logistic回归分析提示携带LOF等位基因是卒中复发的独立危险因素。结论规律服用氯吡格雷进行二级预防的首发缺血性卒中患者,中慢代谢型患者的卒中复发风险较快代谢型升高,携带CYP2C19 LOF等位基因是首发缺血性卒中患者卒中复发的独立危险因素。

关 键 词:基因多态性  氯吡格雷  首发缺血性卒中  复发  
收稿时间:2017-11-09

Association of CYP2C19 Gene Polymorphisms with Risk of Recurrent Stroke in First-ever Ischemic Stroke Patients with Clopidogrel for Secondary Prevention
ZENG Tao,XIAO Xuan-Hao,XU Bang-Lao,LEI Xiu-Xia,LI Ze,ZHOU Jin,HUANG Hui,PAN Xiao-Ping.Association of CYP2C19 Gene Polymorphisms with Risk of Recurrent Stroke in First-ever Ischemic Stroke Patients with Clopidogrel for Secondary Prevention[J].Chinese Journal of Stroke,2018,13(9):908-914.
Authors:ZENG Tao  XIAO Xuan-Hao  XU Bang-Lao  LEI Xiu-Xia  LI Ze  ZHOU Jin  HUANG Hui  PAN Xiao-Ping
Abstract:Objective To investigate the association of CYP2C19 gene polymorphism with the risk of recurrent
stroke in first-ever ischemic stroke (FIS) patients with clopidogrel for secondary prevention.
Methods A total of 326 FIS patients who took Clopidogrel regularly were enrolled in this study,
and recurrent stroke of all patients were recorded by follow-up. The CYP2C19 gene polymorphism
were detected using DNA microarray method. The correlation between CYP2C19 gene
polymorphism and stroke recurrence in patients taking Clopidogrel regularly was analyzed.
Results After a mean follow-up period of (14.44±5.07) months, there were 139 patients who took
Clopidogrel regularly, and 29 ones of which occurred recurrent stroke. Patients of poor metabolizer
(PM) and intermediate metabolizer (IM) had higher risk of stroke recurrence comparing with patients
of extensive metabolize (EM), and the odds ratio (OR) were 3.05 95% confidence interval (CI) 1.11-
8.43, P =0.025] and 9.17 (95%CI 2.39-35.16, P <0.001), respectively. The recurrence risk of *2 (G681A )
A allele carriers was 2.63 times that of G allele carriers (P <0.001). The recurrence rate of stroke in
patients carrying heterozygous and homozygous *2 allele mutant were 2.82 times (P =0.026) and
9.69 times (P <0.001) that of patients with wild-type genes. The recurrence rate in patients with one
loss-of-function (LOF) allele was 3.02 times that of patients without mutant gene (95%CI 1.13-8.05,P =0.030), and this recurrence rate in patients with two LOF alleles was 11.01 times that of patients
without mutant gene (95%CI 2.67-45.24, P <0.001). Multifactor logistic regression analysis result
indicated carrying LOF allele was an independent risk factor of stroke recurrence.
Conclusion For FIS patients taking Clopidogrel regularly for secondary prevention, IM and PM
patients had higher risk of recurrent stroke comparing with EM ones. Carrying CYP2C19 LOF
allele is an independent risk factor of stroke recurrence in FIS patients.
Keywords:Gene polymorphism  Clopidogrel  First-ever ischemic stroke  Recurrence  
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