Brain Development in Adolescents with Genetic Risk Factors for Alcoholism

具有酗酒遗传风险因素的青少年的大脑发育

• 批准号: 8270607
• 负责人: Daniel S. O Leary
• 金额: $ 51.94万
• 依托单位: UNIVERSITY OF IOWA
• 依托单位国家: 美国
• 财政年份: 2010
• 资助国家: 美国
• 起止时间: 2010-08-20 至 2015-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8270607
• 关键词: 18 year old; Adolescent; Adult; Affect; Age; Alcohol abuse; Alcohol consumption; Alcohol dependence; Alcoholism; Alcohols; Amygdaloid structure; Anisotropy; Basic Science; Behavioral; Behavioral inhibition; Brain; Brain imaging; Cerebrospinal Fluid; Cognitive; Cognitive deficits; Conduct Disorder; Corpus Callosum; Data; Databases; Decision Making; Development; Diffusion Magnetic Resonance Imaging; Disease; Disinhibition; Emotional; Exclusion Criteria; Family; Functional Imaging; Functional Magnetic Resonance Imaging; Funding; Gambling; Gender; Genes; Genetic; Genetic Predisposition to Disease; Genetic Risk; Goals; Gray unit of radiation dose; Hippocampus (Brain); Image; Image Analysis; Imaging Techniques; Individual; Informatics; Iowa; Magnetic Resonance Imaging; Matched Group; Measures; Mental disorders; Methods; Monitor; National Institute on Alcohol Abuse and Alcoholism; Normal Range; Parietal; Pathway interactions; Pattern; Performance; Pharmaceutical Preparations; Prefrontal Cortex; Process; Process Measure; Prosencephalon; Prospective Studies; Recording of previous events; Recreational Drugs; Recruitment Activity; Regression Analysis; Relative (related person); Research; Resolution; Rewards; Risk; Risk-Taking; Site; Structure; Surface; Symptoms; System; Techniques; Temporal Lobe; Testing; Universities; aged; alcohol exposure; alcohol related problem; alcohol use disorder; base; brain morphology; brain volume; clinically significant; cognitive function; experience; frontal lobe; genetic pedigree; genetic risk factor; genetics of alcoholism; gray matter; high risk; inclusion criteria; meetings; member; nervous system disorder; neuroimaging; public health relevance; response; volunteer; white matter

DESCRIPTION (provided by applicant): This is a resubmission of a project whose overall aim is to assess the effects of genetic vulnerability to alcoholism on the developing adolescent brain, using cognitive assessments and functional and structural brain imaging. The University of Iowa is one of several sites that have participated in the Collaborative Studies on Genetics of Alcoholism (COGA) project since 1989. COGA is funded by NIAAA (U10AA008401) with the goal of identifying specific genes underlying vulnerability to alcoholism and related disorders. COGA recently began a prospective study, assessing adolescents every two years, beginning at age 12. The project proposed here would assess adolescent COGA volunteers from high genetic risk (HGR) families with state-of-the-art measures of brain structure, using structural magnetic resonance imaging (MRI) measures, and brain function, assessed both by functional MRI (fMRI) and cognitive assessment. The fMRI tasks will focus upon the forebrain reward system, and frontal lobe inhibitory function. Over a five-year period we propose to recruit a group of 96, 13-18 year old HGR COGA subjects, who have minimal use of alcohol and other recreational drugs, and 96 age and gender matched low genetic risk (LGR) controls. Exclusion criteria for both groups will include any history of a psychiatric or neurologic disorder other than conduct disorder. Because conduct disorder (CD) is the most frequent co-morbid psychiatric disorder in adolescents and adults with alcohol use disorders (AUDs) we will recruit HGR subjects with a range of CD symptoms. Regression analyses will then be used to assess the unique variance in the dependent variables associated with CD versus genetic risk for alcohol disorders. We will assess whether adolescents at genetic risk for developing alcohol problems differ from normal adolescent volunteers in brain morphology, activation patterns on fMRI tasks, and/or performance on a range of cognitive tasks that have been shown to be associated with AUD or CD. Although adolescents meeting the rigorous inclusion criteria will be recruited at several of the COGA sites, the neuroimaging and cognitive assessments will take place exclusively in Iowa. While it is feasible to collect imaging data at each site, our experience with the functional Brain Informatics Research Network (fBIRN) project (Dr. O'Leary is the Iowa site PI) indicates that acquiring compatible imaging data at multiple sites requires considerable expense and effort, raises the possibility of non-uniform assessment, and is typically worthwhile only when very large numbers of subjects are required. Our strategy of using a smaller number of adolescent subjects with pedigrees densely affected with alcoholism, selected according to rigorous criteria, makes good use of the extensive COGA data base that has already been collected. The brain imaging and cognitive assessments of adolescents that we propose will provide important information concerning brain structure and function that will profit synergistically from the existing COGA data base, and add information that has both basic science and clinical significance. PUBLIC HEALTH RELEVANCE: Alcoholism and related problems have been shown to have a genetic component. This project will determine whether adolescents who are at genetic risk of developing alcohol-related problems have differences from other adolescents in brain structure and/or function before they start abusing alcohol or other drugs.

描述（由申请人提供）：这是一个项目的重新提交，其总体目标是评估遗传脆弱性对酒精中毒对青少年大脑发育的影响，使用认知评估和功能和结构脑成像。爱荷华州大学是自1989年以来参与酒精中毒遗传学合作研究（COGA）项目的几个地点之一。COGA由NIAAA（U10AA008401）资助，目标是确定导致酒精中毒和相关疾病的特定基因。COGA最近开始了一项前瞻性研究，从12岁开始每两年对青少年进行一次评估。这里提出的项目将评估来自高遗传风险（HGR）家庭的青少年COGA志愿者，使用结构磁共振成像（MRI）测量大脑结构的最先进测量方法，以及通过功能性MRI（fMRI）和认知评估评估的大脑功能。功能磁共振成像任务将集中在前脑奖励系统，额叶抑制功能。在五年的时间里，我们建议招募一组96名13 - 18岁的HGR COGA受试者，他们很少使用酒精和其他娱乐性药物，以及96名年龄和性别匹配的低遗传风险（LGR）对照。两组的排除标准将包括除品行障碍外的任何精神或神经障碍病史。由于行为障碍（CD）是青少年和成人酒精使用障碍（AUD）中最常见的共病精神障碍，因此我们将招募具有一系列CD症状的HGR受试者。然后将使用回归分析评估与CD相关的因变量与酒精障碍遗传风险的独特方差。我们将评估是否青少年在发展酒精问题的遗传风险不同，从正常的青少年志愿者的大脑形态，激活模式的功能磁共振成像任务，和/或性能的一系列认知任务，已被证明与AUD或CD。虽然符合严格入选标准的青少年将在几个COGA站点招募，但神经影像学和认知评估将仅在爱荷华州进行。虽然在每个研究中心收集成像数据是可行的，但我们在功能性脑信息学研究网络（fBIRN）项目（O'Leary博士是爱荷华州研究中心的主要研究者）方面的经验表明，在多个研究中心获取兼容的成像数据需要相当大的费用和努力，增加了非统一评估的可能性，并且通常只有在需要大量受试者时才值得。我们的策略是使用少量的青少年受试者，根据严格的标准选择受酒精中毒影响的家系，很好地利用了已经收集的广泛的COGA数据库。我们提出的青少年脑成像和认知评估将提供有关大脑结构和功能的重要信息，这些信息将从现有的COGA数据库中协同受益，并增加具有基础科学和临床意义的信息。 公共卫生相关性：酒精中毒和相关问题已被证明具有遗传成分。该项目将确定有遗传风险的青少年在开始滥用酒精或其他药物之前，是否与其他青少年在大脑结构和/或功能方面存在差异。