A Mendelian randomization study of alcohol use and cardiometabolic disease risk in a multi-ancestry population from the Million Veteran Program.

IF 3 Q2 SUBSTANCE ABUSE Alcohol (Hanover, York County, Pa.) Pub Date : 2024-11-24 DOI:10.1111/acer.15445
Rachel L Kember, Christopher T Rentsch, Julie Lynch, Marijana Vujkovic, Benjamin Voight, Amy C Justice, Themistocles L Assimes, Henry R Kranzler
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Abstract

Background: Observational studies link moderate alcohol consumption to reduced risk of cardiometabolic diseases, including coronary heart disease (CHD) and type 2 diabetes mellitus (T2D). Mendelian randomization (MR) studies suggest that these associations are due to confounding. We present observed and genetically proxied associations between alcohol consumption and the incidence of CHD and T2D among African Americans (AA), European Americans (EA), and Hispanic Americans (HA) from the Million Veteran Program.

Methods: We conducted two retrospective, nested case-control studies of 33,053 CHD and 28,278 T2D cases matched to five controls each at the time of the event (index date). We used the Alcohol Use Disorders Identification Test-Consumption (AUDIT-C) score closest in time prior to the index date to estimate alcohol exposure. Models were adjusted for smoking, body mass index (BMI), chronic kidney disease, rheumatoid arthritis, and the use of statins or antihypertensive medications. MR analyses used either a single variant in ADH1B or a genetic score (GS) as instrumental variables.

Results: Observational analysis showed a U-shaped association of alcohol consumption with CHD and T2D risk. However, in MR analyses, neither ADH1B genotype-predicted (in 36,465 AAs, 146,464 EAs, and 11,342 HAs) nor GS-predicted (in EAs) alcohol consumption was associated with CHD risk. Similarly, T2D was not associated with alcohol consumption predicted either by ADH1B genotype (in 42,008 AAs, 109,351 EAs, and 13,538 HAs) or GS (in EAs). Multivariable MR analyses that adjusted for the effects of blood pressure and smoking also showed no association between alcohol consumption and cardiometabolic diseases.

Conclusions: We replicate prior observational studies that show a U-shaped association between alcohol consumption and cardiometabolic diseases, but MR findings show no causal association between these traits. This is largely consistent with previous MR analyses in EAs and expands the literature by providing similar findings in AA and HA populations.

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一项关于 "百万退伍军人计划 "中多种族人群饮酒和心脏代谢疾病风险的孟德尔随机研究。
背景:观察性研究表明,适量饮酒可降低罹患冠心病和 2 型糖尿病等心血管代谢疾病的风险。孟德尔随机化(MR)研究表明,这些关联是由混杂因素造成的。我们从 "百万退伍军人计划"(Million Veteran Program)中观察到了饮酒与非裔美国人(AA)、欧裔美国人(EA)和西班牙裔美国人(HA)的冠心病和T2D发病率之间的关系,并对其进行了基因替代:我们对 33,053 例冠心病病例和 28,278 例肺结核病例进行了两项回顾性巢式病例对照研究,每项研究都在事件发生时(指数日期)与五名对照者进行了配对。我们使用指数日期前最接近时间的酒精使用障碍识别测试-消费(AUDIT-C)评分来估计酒精暴露。模型对吸烟、体重指数 (BMI)、慢性肾病、类风湿性关节炎以及他汀类药物或降压药物的使用进行了调整。MR分析使用ADH1B的单个变异体或基因评分(GS)作为工具变量:结果:观察分析表明,饮酒与冠心病和T2D风险呈U型关系。然而,在 MR 分析中,无论是 ADH1B 基因型预测的饮酒量(36,465 名 AA 人、146,464 名 EAs 人和 11,342 名 HAs 人)还是 GS 预测的饮酒量(EAs 人)都与心脏病风险无关。同样,T2D 也与 ADH1B 基因型(42,008 名 AAs、109,351 名 EAs 和 13,538 名 HAs)或 GS(EAs)预测的饮酒量无关。调整了血压和吸烟影响的多变量 MR 分析也显示,饮酒与心脏代谢疾病之间没有关联:我们重复了之前的观察性研究,这些研究显示饮酒与心血管代谢疾病之间存在 U 型关系,但 MR 分析结果显示这些特征之间没有因果关系。这与之前对 EAs 进行的 MR 分析结果基本一致,并通过在 AA 和 HA 群体中提供类似的结果扩展了文献。
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