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家族性酒精使用障碍史与神经发育:青少年的功能连接研究。

Family history of alcohol use disorders and neuromaturation: a functional connectivity study with adolescents.

机构信息

Veterans Affairs San Diego Healthcare System , San Diego, CA .

出版信息

Am J Drug Alcohol Abuse. 2013 Nov;39(6):356-64. doi: 10.3109/00952990.2013.818680.

DOI:10.3109/00952990.2013.818680
PMID:24200205
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3959877/
Abstract

BACKGROUND

A positive family history (FHP) of alcohol use disorders (AUD) is linked to increased risk for personal AUD, but the mechanisms behind this risk are unclear. Previous research suggests that a subtle neurodevelopmental lag in FHP adolescents may contribute to risk for future AUD.

METHODS

Functional magnetic resonance imaging (fMRI) response to a spatial working memory (SWM) task was examined for markers of neuromaturational delay in 85 youth with and without FHP. It was hypothesized that FHP adolescents (n = 24, ages 12-14 years), as compared to matched FHN youth (n = 26, ages 12-14 years), would show less similarity to brain connectivity observed in older adolescents (n = 35, ages 16-20 years) and that statistical comparison of SWM functional connectivity models would differentiate FHN and FHP youth. Structural equation modeling tested the fit of brain response connectivity between FH groups and against the older-adolescent model.

RESULTS

Patterns of connectivity were more similar between older adolescent and FHN than FHP adolescents; FHP youth demonstrated higher association between right posterior and left frontal brain regions than FHN and older adolescent youth. Comparison of FH groups indicated a significant difference on the pathway from the right superior parietal lobule to the left middle frontal gyrus.

CONCLUSIONS

These findings provide additional support for the notion of a neuromaturational lag in FHP youth. Protracted neuromaturation may be a mechanism by which FH increases risk for alcohol dependence, and this less mature neural connectivity pattern may provide a novel endophenotype for identifying youth at risk for drinking problems.

摘要

背景

有酗酒障碍家族病史(FHP)会增加个人酗酒障碍的风险,但这种风险背后的机制尚不清楚。先前的研究表明,FHP 青少年可能存在微妙的神经发育滞后,这可能导致他们未来有酗酒障碍的风险。

方法

本研究使用功能磁共振成像(fMRI)对 85 名青少年(有或无 FHP)的空间工作记忆(SWM)任务进行了大脑反应测试,以寻找神经成熟延迟的标记物。研究假设,与匹配的 FHN 青少年(n = 26,年龄 12-14 岁)相比,FHP 青少年(n = 24,年龄 12-14 岁)的大脑连接模式与年龄较大的青少年(n = 35,年龄 16-20 岁)的大脑连接模式的相似度更低,并且 SWM 功能连接模型的统计比较将区分 FHN 和 FHP 青少年。结构方程模型测试了 FH 组之间的大脑反应连接的拟合度,并与年龄较大的青少年模型进行了对比。

结果

FHP 青少年的大脑连接模式与年龄较大的青少年和 FHN 青少年的连接模式差异更大;与 FHN 和年龄较大的青少年相比,FHP 青少年的右后和左前脑区域之间的关联度更高。对 FH 组的比较表明,右侧顶叶上回与左侧额中回之间的通路存在显著差异。

结论

这些发现为 FHP 青少年存在神经发育滞后的观点提供了更多支持。神经发育的延长可能是 FH 增加酒精依赖风险的一种机制,而这种不成熟的神经连接模式可能为识别有饮酒问题风险的青少年提供一个新的候选内表型。

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