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目标相关顶叶 P3 和内侧额颞θ 指数与物质使用问题的遗传风险相关。

Target-related parietal P3 and medial frontal theta index the genetic risk for problematic substance use.

机构信息

Department of Psychology, University of Minnesota, Minneapolis, Minnesota.

出版信息

Psychophysiology. 2019 Aug;56(8):e13383. doi: 10.1111/psyp.13383. Epub 2019 Apr 23.

Abstract

Theoretical and empirical work suggests that problematic substance use (PSU) is associated with individual differences in prefrontal cortex activity. While research has strongly linked parietal P3 amplitude reduction (P3AR) to genetic risk for problematic substance use, few studies have tested whether prefrontal EEG measures are sensitive to this genetic liability. In addition to P3, oddball target detection tasks elicit medial frontal theta power, reflecting attentional allocation, and parietal delta, indexing decision making or stimulus-response link updating. Midfrontal theta and parietal delta may index neurocognitive processes relevant to PSU beyond P3AR. The present investigation examined the etiological relationship between PSU and P3, frontal theta, and parietal delta in a large twin sample (N = 754). EEG was recorded during a visual oddball task. Greater PSU was associated with reduced target P3 amplitude and midfrontal theta/parietal delta power, and increased mean reaction time and reaction time variability (RTV; indexing attentional fluctuations). P3, theta, and RTV, but not delta or mean RT, explained unique variance in PSU (R  = 0.04). Twin biometric modeling indicated a genetic relationship between PSU and P3, theta, and RTV. Theta accounted for distinct genetic variance in PSU beyond P3 and RTV. Together, 23% of the total additive genetic variance in PSU was explained by the three endophenotypes. Results replicate P3AR as an endophenotype and provide support for additional behavioral (RTV) and neurophysiological (midfrontal theta) endophenotypes of PSU. Reduced theta and greater RTV may reflect variations in a prefrontal attentional network that confers genetic risk for substance use problems.

摘要

理论和实证研究表明,有问题的物质使用(PSU)与前额叶皮层活动的个体差异有关。虽然研究强烈地将顶叶 P3 波幅降低(P3AR)与物质使用障碍的遗传风险联系起来,但很少有研究测试前额叶 EEG 测量是否对这种遗传倾向敏感。除了 P3,oddball 目标检测任务还会引发内侧额θ功率,反映注意力分配,以及顶叶δ,反映决策或刺激-反应链接更新。中额θ和顶叶δ可能会反映出与 P3AR 相关的与 PSU 相关的神经认知过程。本研究在一个大型双胞胎样本(N=754)中检查了 PSU 与 P3、前额θ和顶叶δ之间的病因关系。在视觉 oddball 任务中记录 EEG。更大的 PSU 与目标 P3 波幅降低和前额θ/顶叶δ功率增加以及平均反应时间和反应时间变异性(RTV;反映注意力波动)相关。P3、θ和 RTV,但不是δ或平均 RT,解释了 PSU 的独特方差(R=0.04)。双胞胎生物计量建模表明 PSU 与 P3、θ和 RTV 之间存在遗传关系。θ解释了 P3 和 RTV 之外 PSU 的独特遗传方差。总的来说,3 种内表型解释了 PSU 总可加遗传方差的 23%。结果复制了 P3AR 作为内表型,并为 PSU 的其他行为(RTV)和神经生理学(前额叶θ)内表型提供了支持。θ的减少和 RTV 的增加可能反映了前额叶注意力网络的变化,该网络赋予了物质使用问题的遗传风险。

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