雌激素受体α基因多态性与心肌梗死风险

Estrogen receptor alpha gene polymorphisms and risk of myocardial infarction.

作者信息

Schuit Stephanie C E, Oei Hok-Hay S, Witteman Jacqueline C M, Geurts van Kessel Corine H, van Meurs Joyce B J, Nijhuis Rogier L, van Leeuwen Johannes P T M, de Jong Frank H, Zillikens M Carola, Hofman Albert, Pols Huibert A P, Uitterlinden André G

机构信息

Department of Internal Medicine, Erasmus Medical Center, Rotterdam, The Netherlands.

出版信息

JAMA. 2004 Jun 23;291(24):2969-77. doi: 10.1001/jama.291.24.2969.

DOI:10.1001/jama.291.24.2969

PMID:15213208

Abstract

CONTEXT

The role of estrogens in ischemic heart disease (IHD) is uncertain. Evidence suggests that genetic variations in the estrogen receptor alpha (ESR1) gene may influence IHD risk, but the role of common sequence variations in the ESR1 gene is unclear.

OBJECTIVE

To determine whether the ESR1 haplotype created by the c.454-397T>C (PvuII) and c.454-351A>G (XbaI) polymorphisms is associated with myocardial infarction (MI) and IHD risk.

DESIGN, SETTING, AND PARTICIPANTS: In 2617 men and 3791 postmenopausal women from The Rotterdam Study (enrollment between 1989-1993 and follow-up to January 2000), a population-based, prospective cohort study of participants aged 55 years and older, ESR1 c.454-397T>C and c.454-351A>G haplotypes were determined. Detailed interviews and physical examinations were performed, blood samples were obtained, and cardiovascular risk factors were assessed.

MAIN OUTCOME MEASURE

The primary outcome was MI and IHD defined as MIs, revascularization procedures, and IHD mortality.

RESULTS

Approximately 29% of women and 28.2% of men were homozygous carriers of the ESR1 haplotype 1 (-397 T and -351 A) allele, 49% of women and 50% of men were heterozygous carriers, and 22% of women and 21.4% of men were noncarriers. During a mean follow-up of 7.0 years, 285 participants (115 women; 170 men) had MI, and 440 (168 women; 272 men) had an IHD event, of which 97 were fatal. After adjustment for known cardiovascular risk factors, female heterozygous carriers of haplotype 1 had an increased risk of MI (event rate, 2.8%; relative risk [RR], 2.23; 95% confidence interval [CI], 1.13-4.43) compared with noncarriers (event rate, 1.3%), whereas homozygous carriers had an increased risk (event rate, 3.2%; RR, 2.48; 95% CI, 1.22-5.03). For IHD events, we observed a similar association. In women, the effect of haplotype 1 on fatal IHD was larger than on nonfatal IHD. In men, the ESR1 haplotypes were not associated with an increased risk of MI (event rate, 5.7%; RR, 0.93; 95% CI, 0.59-1.46 for heterozygous carriers; and event rate, 5.1%; RR, 0.82; 95% CI, 0.49-1.38 for homozygous carriers) compared with noncarriers (event rate, 5.8%) and were not associated with an increased risk of IHD.

CONCLUSIONS

In this population-based, prospective cohort study, postmenopausal women who carry ESR1 haplotype 1 (c.454-397 T allele and c.454-351 A allele) have an increased risk of MI and IHD, independent of known cardiovascular risk factors. In men, no association was observed.

摘要

背景

雌激素在缺血性心脏病（IHD）中的作用尚不确定。有证据表明，雌激素受体α（ESR1）基因的遗传变异可能影响IHD风险，但ESR1基因常见序列变异的作用尚不清楚。

目的

确定由c.454 - 397T>C（PvuII）和c.454 - 351A>G（XbaI）多态性产生的ESR1单倍型是否与心肌梗死（MI）和IHD风险相关。

设计、地点和参与者：在鹿特丹研究中纳入的2617名男性和3791名绝经后女性（1989 - 1993年入组，随访至2000年1月）中，这是一项针对55岁及以上参与者的基于人群的前瞻性队列研究，确定了ESR1 c.454 - 397T>C和c.454 - 351A>G单倍型。进行了详细的访谈和体格检查，采集了血样，并评估了心血管危险因素。

主要结局指标

主要结局为定义为心肌梗死、血运重建手术和IHD死亡的MI和IHD。

结果

约29%的女性和28.2%的男性是ESR1单倍型1（-397T和-351A）等位基因的纯合携带者，49%的女性和50%的男性是杂合携带者，22%的女性和21.4%的男性是非携带者。在平均7.0年的随访期间，285名参与者（115名女性；170名男性）发生了MI，440名（168名女性；272名男性）发生了IHD事件，其中97例是致命的。在对已知心血管危险因素进行调整后，与非携带者（事件发生率为1.3%）相比，单倍型1的女性杂合携带者发生MI的风险增加（事件发生率为2.8%；相对风险[RR]为2.23；95%置信区间[CI]为1.13 - 4.43），而纯合携带者的风险增加（事件发生率为3.2%；RR为2.48；95%CI为1.22 - 5.03）。对于IHD事件，我们观察到了类似的关联。在女性中，单倍型1对致命IHD的影响大于对非致命IHD的影响。在男性中，与非携带者（事件发生率为5.8%）相比，ESR1单倍型与MI风险增加无关（杂合携带者的事件发生率为5.7%；RR为0.93；95%CI为0.59 - 1.46；纯合携带者的事件发生率为5.1%；RR为0.82；95%CI为0.49 - 1.38），也与IHD风险增加无关。