Genetic and environmental contributions to drinking milestones in youth

遗传和环境对青少年饮酒里程碑的贡献

• 批准号: 8831194
• 负责人: Emily Hunt Olfson
• 金额: $ 2.93万
• 依托单位: WASHINGTON UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2014
• 资助国家: 美国
• 起止时间: 2014-09-03 至 2016-09-02
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8831194
• 关键词: Acetaldehyde; Address; Adolescence; Adolescent; Adoption; Adult; Affect; African American; Alcohol consumption; Alcohol dehydrogenase; Alcohol dependence; Alcohols; Behavior; Complex; Data; Development; Developmental Process; Diagnostic and Statistical Manual of Mental Disorders; Disease; Disease Progression; Environment; Environmental Risk Factor; Enzymes; Ethanol; Etiology; European; Family; Future; Gene Cluster; Genes; Genetic; Genetic Predisposition to Disease; Genotype; Goals; Intervention; Knowledge; Lead; Nicotine Dependence; Nicotinic Receptors; Onset of illness; Outcome; Pattern; Poison; Public Health; Receptor Gene; Research; Risk; Risk Factors; Role; Sampling; Smoking; Smoking Behavior; Social Environment; Substance Use Disorder; Testing; Twin Multiple Birth; Twin Studies; Variant; Youth; adolescent alcohol; alcohol involvement; alcohol related problem; alcohol use disorder; alcohol use initiation; base; critical developmental period; critical period; drinking; drinking behavior; early drinking; effective intervention; genetic variant; genetics of alcoholism; genome-wide; insight; meetings; modifiable risk; parental monitoring; peer; prevent; public health relevance; underage drinking

DESCRIPTION (provided by applicant): Alcohol use behaviors that begin in youth are important contributors to alcohol use disorders in adulthood. Large-scale studies of adults have identified specific genetic variants that are associated at a genome-wide level with substance use disorders. The extent to which these genetic variants, individually and with other risk factors, influence early drinking behaviors is not fully understood. The goal of this project is to determine whether genetic variants identified in adults impact the development of drinking milestones in youth and how important environmental risk factors modify these effects. We will use an existing longitudinal sample of European and African American youth collected through the Collaborative Study on the Genetics of Alcoholism (COGA). Our central hypothesis is that genetic variants will affect early alcohol- related problems and that environmental factors will modify this effect. Guided by strong preliminary data generated from analyses performed by the applicant, this hypothesis will be examined in two specific aims. Aim 1 will test the effect of wel-established targeted genetic variants on adolescent drinking behaviors from drinking initiation to DSM-5 alcohol use disorders. We will initially examine functional variants in the enzyme alcohol dehydrogenase (ADH) that have been shown to have a genome-wide significant effect on alcohol use disorders in adults. We will then examine variation in the CHRNA5-CHRNA3-CHRNAB4 nicotinic receptor subunit genes that is genome-wide significant for smoking behaviors, with growing evidence for an association with adult alcohol dependence. Aim 2 will then test how known environmental risk factors for early drinking behaviors modify the effect of these targeted genetic variants. We will focus on the two environments of peer drinking and parental monitoring, which have previously been shown to influence youth drinking patterns. The proposed research is significant because it is expected to provide insight into the complex etiology of early drinking behaviors. A better understanding of how specific genetic and environmental factors contribute to these early behaviors will add to our fundamental knowledge of the developmental processes that lead to alcohol use disorders. Ultimately, identification of modifiable risk factors that influence underlying genetic vulnerabilities has the potential to infom new interventions to reduce the burden of this severe disease.

描述（由申请人提供）：青年开始的饮酒行为是成年后饮酒障碍的重要促进者。对成年人的大规模研究已经确定了在全基因组水平上与药物使用障碍相关的特定遗传变异。这些遗传变异的单独和其他风险因素在多大程度上影响早期饮酒行为。这个项目的目标是 确定成人鉴定的遗传变异是否会影响青年饮酒里程碑的发展以及环境风险因素如何改变这些影响。我们将使用有关酒精中毒遗传学（COGA）的合作研究收集的欧洲和非裔美国青年的现有纵向样本。我们的核心假设是，遗传变异将影响早期与酒精有关的问题，并且环境因素将改变这种影响。以申请人进行的分析产生的强大初步数据为指导，该假设将以两个具体的目的进行检查。 AIM 1将测试受欢迎的靶向遗传变异对从饮酒开始到DSM-5酒精使用障碍的青少年饮酒行为的影响。我们最初将检查酶醇脱氢酶（ADH）中的功能变异，这些变体已被证明对成人的酒精使用障碍具有重大影响。然后，我们将检查ChrNA5-CHRNA3-CHRNAB4烟碱受体亚基基因的变化，该基因对吸烟行为具有重要意义，并越来越多地证明与成人酒精依赖相关的证据。 AIM 2然后将测试已知的早期饮酒行为环境风险因素如何改变这些靶向遗传变异的影响。我们将专注于同伴饮酒和父母监测的两个环境，这些环境以前已被证明会影响青年饮酒方式。拟议的研究很重要，因为它有望提供对早期饮酒行为的复杂病因的见解。更好地了解特定的遗传和环境因素如何促进这些早期行为，这将增加我们对导致饮酒障碍的发育过程的基本知识。最终，鉴定影响基本遗传脆弱性的可修改风险因素有可能为减轻这种严重疾病负担的新干预措施提供潜力。