Smoking-Related Increases in Alcohol Outcomes and Preliminary Evidence for the Protective Effect of a Functional Nicotine Receptor Gene (CHRNA5) Variant on Alcohol Consumption in Individuals Without Alcohol Use Disorder.

IF 4.5 2区 医学 Q1 CLINICAL NEUROLOGY
Shyamala K Venkatesh, Bethany L Stangl, Jia Yan, Natalia A Quijano Cardé, Elliot A Stein, Nancy Diazgranados, Melanie L Schwandt, Hui Sun, Reza Momenan, David Goldman, Mariella De Biasi, Vijay A Ramchandani
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Abstract

Background: Alcohol and nicotine interact with the nicotinic acetylcholine receptor system to alter reward-related responses, thereby contributing to the co-use and misuse of these drugs. A missense polymorphism rs16969968 (G>A) in the CHRNA5 gene has shown a strong association with nicotine-related phenotypes. However, less is known about the impact of this variant on alcohol-related phenotypes.

Methods: We assessed the main and interactive effect of smoking and rs16969968 polymorphism on alcohol consumption using the Alcohol Use Disorders Identification Test (AUDIT), Timeline Follow Back (TLFB), and Lifetime Drinking History (LDH) in 980 healthy adults without alcohol use disorder. We further examined the effect of the rs16969968 polymorphism on acute alcohol consumption using a free-access i.v. alcohol self-administration (IV-ASA) human laboratory paradigm in a subset of 153 nonsmoking participants. Subjective alcohol responses, alcohol sensitivity, and expectancy measures were compared between genotype groups (GG; AA/AG).

Results: We observed a significant association of smoking with AUDIT, TLFB, and LDH measures across genotype groups, with smokers showing higher scores compared with nonsmokers. Additionally, we found an association between genotype and TLFB-total drinks in the IV-ASA subset, with the GG group showing higher scores than AA/AG group. Relatedly, the alcohol negative expectancy score was significantly lower in the GG group than the AA/AG group.

Conclusions: Our findings underscore the association of smoking with alcohol measures. We found preliminary evidence for the protective effect of the functional CHRNA5 polymorphism on alcohol consumption and its association with increased negative alcohol expectancies, which highlights the substantial heterogeneity in alcohol responses.

与吸烟有关的酒精结果增加,以及功能性尼古丁受体基因(CHRNA5)变异对无酒精使用障碍者酒精消费的保护作用的初步证据。
背景:酒精和尼古丁与烟碱乙酰胆碱受体系统相互作用,改变与奖赏相关的反应,从而导致这些药物的共同使用和滥用。CHRNA5 基因中的一个错义多态性 rs16969968 (G>A) 与尼古丁相关表型有密切联系。然而,人们对这一变异对酒精相关表型的影响知之甚少:我们使用酒精使用障碍鉴定测试(AUDIT)、时间线回溯(TLFB)和终生饮酒史(LDH)评估了吸烟和 rs16969968 多态性对 980 名无酒精使用障碍的健康成年人饮酒的主要影响和交互影响。我们还进一步研究了 rs16969968 多态性对急性酒精消费的影响,在 153 名非吸烟者中采用了自由静脉注射酒精自我给药(IV-ASA)人体实验室范式。比较了不同基因型组(GG;AA/AG)的主观酒精反应、酒精敏感性和期望值:结果:我们观察到,在不同基因型组中,吸烟与 AUDIT、TLFB 和 LDH 的测量结果有明显的关联,吸烟者的得分高于不吸烟者。此外,我们还发现在 IV-ASA 亚组中,基因型与 TLFB-总饮酒量之间存在关联,GG 组的得分高于 AA/AG 组。与此相关的是,GG 组的酒精负期望值得分明显低于 AA/AG 组:我们的研究结果强调了吸烟与酒精测量之间的联系。我们发现了功能性 CHRNA5 多态性对酒精消费的保护作用及其与酒精负期望值增加相关的初步证据,这凸显了酒精反应的巨大异质性。
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来源期刊
CiteScore
8.40
自引率
2.10%
发文量
230
审稿时长
4-8 weeks
期刊介绍: The central focus of the journal is on research that advances understanding of existing and new neuropsychopharmacological agents including their mode of action and clinical application or provides insights into the biological basis of psychiatric disorders and thereby advances their pharmacological treatment. Such research may derive from the full spectrum of biological and psychological fields of inquiry encompassing classical and novel techniques in neuropsychopharmacology as well as strategies such as neuroimaging, genetics, psychoneuroendocrinology and neuropsychology.
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