首页> 外文期刊>Behavioural Brain Research: An International Journal >Auditory event-related potentials (P3a, P3b) and genetic variants within the dopamine and serotonin system in healthy females
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Auditory event-related potentials (P3a, P3b) and genetic variants within the dopamine and serotonin system in healthy females

机译:健康女性多巴胺和5-羟色胺系统内与听觉事件相关的电位(P3a,P3b)和遗传变异

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The late positive components of the human event-related brain potential comprise electrocortical reflections of stimulus-driven attentional capture (the anteriorly distributed P3a) and top-down control detection of relevant events (the posteriorly distributed P3b). As of yet, the neuropharmacologic and neurogenetic origin of the P3a and P3b is not fully understood.In this study, we address the contribution of dopaminergic and serotoninergic mechanisms. Sixty healthy females completed an active auditory novelty oddball paradigm while EEG was recorded. In all subjects, genetic polymorphisms within the dopamine system (dopamine transporter [DAT1], catecholamine-O-methyltransferase val158met [COMT val158met]) and the serotonin system (serotonin transporter [5HTTLPR]) were assessed.Across genotypes, novels (relative to standards) elicited a fronto-centrally distributed P3a, and targets (relative to standards) a parieto-centrally distributed P3b. Genotypes effects were observed for both P3a (COMT, 5HTTPLR) and P3b (DAT1, COMT, 5HTTLPR) only at prefrontal electrode location (Fz). Specifically, the frontal P3a was enhanced in COMT met/met homozygotes, but not in DAT1 9R. The target-related P3b was enhanced in COMT met/met and DAT1 9R relative to its genetic counterparts, but only at frontal electrodes. This 'anteriorized' enhancement may reflect either an additional frontal component in the target-related P3 dependent on dopamine, or a more subtle shift in the neural ensemble that generates the target-related P3. Results for 5HTTLPR short allele homozygotes mimicked those in COMT met/met homozygotes.In all, the present findings suggest involvement of frontal-cortical dopaminergic and serotoninergic mechanisms in bottom-up attentional capture (COMT val158met, 5HTTLPR), with an additional top-down component sensitive to striatal signals (DAT1).
机译:人类事件相关脑电势的晚期阳性成分包括刺激驱动的注意捕获的电皮层反射(前向分布的P3a)和相关事件的自顶向下控制检测(后向分布的P3b)。到目前为止,P3a和P3b的神经药理学和神经遗传学起源尚不完全清楚。在本研究中,我们探讨了多巴胺能和5-羟色胺能机制的作用。记录脑电图的同时,有60名健康女性完成了活跃的听觉新奇古怪的范例。在所有受试者中,评估了多巴胺系统(多巴胺转运蛋白[DAT1],儿茶酚胺-O-甲基转移酶val158met [COMT val158met])和5-羟色胺系统(5-羟色胺转运蛋白[5HTTLPR])内的遗传多态性。跨基因型,新颖性(相对于标准)引发了一个位于前中央的P3a,并针对(相对于标准)了一个位于上中央的P3b。仅在前额电极位置(Fz)观察到P3a(COMT,5HTTPLR)和P3b(DAT1,COMT,5HTTLPR)的基因型效应。具体而言,额叶P3a在COMT met / met纯合子中增强,但在DAT1 9R中未增强。相对于其遗传对应物,目标相关的P3b在COMT met / met和DAT1 9R中得到增强,但仅在额电极处增强。这种“前瞻性”增强可能反映了依赖于多巴胺的靶标相关P3中的额叶成分的增加,或者反映了产生靶标相关P3的神经系中更细微的变化。 5HTTLPR短等位基因纯合子的结果模拟了COMT met / met纯合子中的那些。总的来说,目前的发现表明额叶皮质多巴胺能和5-羟色胺能机制参与了自下而上的注意力捕获(COMT val158met,5HTTLPR),另外自上而下对纹状体信号(DAT1)敏感的组件。

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