Wang Chunhong, Zhou Xin, Ye Shuiqing, Han Dingfen, Tan Xiaodong, Zheng Fang, Shi Qun
Department of Hygiene, School of Medicine, Wuhan University, DongHu Road 115, Wuhan 430071, PR China.
Int J Hyg Environ Health. 2006 May;209(3):265-73. doi: 10.1016/j.ijheh.2005.12.005. Epub 2006 Feb 3.
To investigate associations of gene polymorphisms of the apoE-CI-CII gene cluster and the LDL-R gene on coronary artery disease (CAD) and their interactions with alcohol drinking and smoking in the Chinese Han population.
A questionnaire survey of the behaviors of smoking and drinking, dietary patterns and anamnesis was conducted among 203 patients of CAD, aged 65.0 +/- 11.1 years, and 365 controls, aged 63.6 +/- 12.0 years. Peripheral blood samples were colleted and the total DNA was extracted. The apoE genotypes were identified by multiplex amplification refractory mutation system (multi-AMRS), the apoCI promoter polymorphisms and AvaII polymorphisms of the apoCII and LDL-R gene were detected by using PCR-RFLP. Pairwise linkage disequilibrium coefficients (D, D') were estimated by the LINKAGE program. The interactions between genes with alcohol drinking and smoking were analyzed by using multivariate logistic regression models.
The differences of systolic/diastolic blood pressure, total cholesterol (TC) and low-density lipoprotein cholesterol (LDL-C) concentrations, smoking and drinking were significant between subjects with CAD and controls. The frequencies of apoE gene epsilon 3/4 genotype (25.9%) and epsilon 4 (13.9%) in CAD were significantly higher than those in controls (12.5% and 6.9%, respectively, p < 0.05). A significant difference was also found for the apoCI locus, the frequencies of H2 allele were 20.5% in the CAD and 11.3% in the control. Linkage disequilibrium coefficient D' was 0.672 (p < 0.01) between apoE and apoCI genes. Significant differences for a deficit of epsilon 3-H1-T1 and excess of epsilon 4-H2-T1 was found in CAD by estimation of the haplotype frequencies. After control for possible confounding factors, the multivariate logistic analysis showed that epsilon 4, H2 allele, smoking and drinking were risk factors of CAD. A significant interaction among epsilon 4, H2 and smoking was observed (OR 18.3, 95% CI: 2.35-150.81, p < 0.05), it was a multiplicative model. An additive model was shown among epsilon 4, H2 and drinking (OR12.7, 95% CI: 2.8-58.6, p < 0.05).
The results suggested that both apoE and apoCI on chromosome 19 were the susceptibility locus for CAD, their linkage disequilibrium should be responsible for the development of CAD. Drinking and smoking enhance the genetic predisposition to CAD.
研究载脂蛋白E-CI-CII基因簇和低密度脂蛋白受体(LDL-R)基因多态性与中国汉族人群冠状动脉疾病(CAD)的关联及其与饮酒和吸烟的相互作用。
对203例年龄为65.0±11.1岁的CAD患者和365例年龄为63.6±12.0岁的对照者进行吸烟、饮酒行为、饮食习惯和病史的问卷调查。采集外周血样本并提取总DNA。采用多重扩增阻滞突变系统(multi-AMRS)鉴定载脂蛋白E(apoE)基因型,利用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)检测apoCI启动子多态性以及apoCII和LDL-R基因的AvaII多态性。通过LINKAGE程序估计成对连锁不平衡系数(D、D')。使用多因素logistic回归模型分析基因与饮酒和吸烟之间的相互作用。
CAD患者与对照者之间的收缩压/舒张压、总胆固醇(TC)和低密度脂蛋白胆固醇(LDL-C)浓度、吸烟和饮酒情况存在显著差异。CAD患者中apoE基因ε3/4基因型频率(25.9%)和ε4频率(13.9%)显著高于对照者(分别为12.5%和6.9%,p<0.05)。apoCI位点也存在显著差异,CAD组中H2等位基因频率为20.5%,对照组中为11.3%。apoE与apoCI基因之间的连锁不平衡系数D'为0.672(p<0.01)。通过单倍型频率估计发现,CAD组中ε3-H1-T1单倍型缺失和ε4-H2-T1单倍型增加存在显著差异。在控制可能的混杂因素后,多因素logistic分析显示,ε4、H2等位基因、吸烟和饮酒是CAD的危险因素。观察到ε4、H2与吸烟之间存在显著的相互作用(比值比18.3,95%可信区间:2.35-150.81,p<0.05),为相乘模型。ε4、H2与饮酒之间显示为相加模型(比值比12.7,95%可信区间:2.8-58.6,p<0.05)。
结果提示,19号染色体上的apoE和apoCI均为CAD的易感位点,它们之间的连锁不平衡可能与CAD的发生有关。饮酒和吸烟增强了CAD的遗传易感性。
