Department of Psychiatry & Behavioral Sciences, Stanford University School of Medicine, Stanford, California.
Center for Health Sciences, SRI International, Menlo Park, California.
JAMA Psychiatry. 2021 Apr 1;78(4):407-415. doi: 10.1001/jamapsychiatry.2020.4064.
Maturation of white matter fiber systems subserves cognitive, behavioral, emotional, and motor development during adolescence. Hazardous drinking during this active neurodevelopmental period may alter the trajectory of white matter microstructural development, potentially increasing risk for developing alcohol-related dysfunction and alcohol use disorder in adulthood.
To identify disrupted adolescent microstructural brain development linked to drinking onset and to assess whether the disruption is more pronounced in younger rather than older adolescents.
DESIGN, SETTING, AND PARTICIPANTS: This case-control study, conducted from January 13, 2013, to January 15, 2019, consisted of an analysis of 451 participants from the National Consortium on Alcohol and Neurodevelopment in Adolescence cohort. Participants were aged 12 to 21 years at baseline and had at least 2 usable magnetic resonance diffusion tensor imaging (DTI) scans and up to 5 examination visits spanning 4 years. Participants with a youth-adjusted Cahalan score of 0 were labeled as no-to-low drinkers; those with a score of greater than 1 for at least 2 consecutive visits were labeled as heavy drinkers. Exploratory analysis was conducted between no-to-low and heavy drinkers. A between-group analysis was conducted between age- and sex-matched youths, and a within-participant analysis was performed before and after drinking.
Self-reported alcohol consumption in the past year summarized by categorical drinking levels.
Diffusion tensor imaging measurement of fractional anisotropy (FA) in the whole brain and fiber systems quantifying the developmental change of each participant as a slope.
Analysis of whole-brain FA of 451 adolescents included 291 (64.5%) no-to-low drinkers and 160 (35.5%) heavy drinkers who indicated the potential for a deleterious association of alcohol with microstructural development. Among the no-to-low drinkers, 142 (48.4%) were boys with mean (SD) age of 16.5 (2.2) years and 149 (51.2%) were girls with mean (SD) age of 16.5 (2.1) years and 192 (66.0%) were White participants. Among the heavy drinkers, 86 (53.8%) were boys with mean (SD) age of 20.1 (1.5) years and 74 (46.3%) were girls with mean (SD) age of 20.5 (2.0) years and 142 (88.8%) were White participants. A group analysis revealed FA reduction in heavy-drinking youth compared with age- and sex-matched controls (t154 = -2.7, P = .008). The slope of this reduction correlated with log of days of drinking since the baseline visit (r156 = -0.21, 2-tailed P = .008). A within-participant analysis contrasting developmental trajectories of youths before and after they initiated heavy drinking supported the prediction that drinking onset was associated with and potentially preceded disrupted white matter integrity. Age-alcohol interactions (t152 = 3.0, P = .004) observed for the FA slopes indicated that the alcohol-associated disruption was greater in younger than older adolescents and was most pronounced in the genu and body of the corpus callosum, regions known to continue developing throughout adolescence.
This case-control study of adolescents found a deleterious association of alcohol use with white matter microstructural integrity. These findings support the concept of heightened vulnerability to environmental agents, including alcohol, associated with attenuated development of major white matter tracts in early adolescence.
白质纤维系统的成熟促进了青少年时期认知、行为、情感和运动的发展。在这个活跃的神经发育期间,危险饮酒可能会改变白质微观结构发育的轨迹,潜在增加成年后与酒精相关的功能障碍和酒精使用障碍的风险。
确定与饮酒开始相关的青少年微观结构脑发育障碍,并评估这种破坏在较年轻的青少年中是否比在较年长的青少年中更为明显。
设计、地点和参与者: 这是一项病例对照研究,于 2013 年 1 月 13 日至 2019 年 1 月 15 日进行,包括来自酒精和青少年神经发育国家联盟队列的 451 名参与者的分析。参与者在基线时年龄在 12 至 21 岁之间,至少有 2 次可使用的磁共振扩散张量成像 (DTI) 扫描,最多有 5 次检查访问,跨度为 4 年。青年调整后的 Cahalan 评分为 0 的参与者被标记为无到低饮酒者;至少有 2 次连续评分大于 1 的参与者被标记为重度饮酒者。在无到低饮酒者和重度饮酒者之间进行了探索性分析。在年龄和性别匹配的青少年之间进行了组间分析,并在饮酒前后进行了个体内分析。
过去一年的自我报告饮酒量总结为分类饮酒水平。
对全脑和纤维系统的分数各向异性 (FA) 进行了扩散张量成像测量,以量化每个参与者的发育变化作为斜率。
对 451 名青少年的全脑 FA 分析包括 291 名(64.5%)无到低饮酒者和 160 名(35.5%)重度饮酒者,他们表明酒精与微观结构发育之间可能存在有害关联。在无到低饮酒者中,142 名(48.4%)是男孩,平均(SD)年龄为 16.5(2.2)岁,149 名(51.2%)是女孩,平均(SD)年龄为 16.5(2.1)岁,192 名(66.0%)是白人参与者。在重度饮酒者中,86 名(53.8%)是男孩,平均(SD)年龄为 20.1(1.5)岁,74 名(46.3%)是女孩,平均(SD)年龄为 20.5(2.0)岁,142 名(88.8%)是白人参与者。组间分析显示,与年龄和性别匹配的对照组相比,重度饮酒者的 FA 减少(t154 =-2.7,P=.008)。这种减少的斜率与自基线访问以来的饮酒天数的对数相关(r156 =-0.21,2 尾 P=.008)。在饮酒前后对比青少年发展轨迹的个体内分析支持了这样的预测,即饮酒开始与潜在的白质完整性破坏有关,并可能先于白质完整性破坏。观察到的 FA 斜率的年龄-酒精相互作用(t152 =3.0,P=.004)表明,酒精相关的破坏在较年轻的青少年中比在较年长的青少年中更大,在胼胝体的膝部和体部最为明显,这些区域已知在整个青春期仍在发育。
这项对青少年的病例对照研究发现,饮酒与白质微观结构完整性之间存在有害关联。这些发现支持了这样的概念,即与酒精相关的环境因素(包括酒精)与主要白质束在青春期早期发育减弱有关,青少年更容易受到这些因素的影响。
