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从基因型到 EEG 内表型:了解复杂精神疾病的后基因组学途径?

From genotype to EEG endophenotype: a route for post-genomic understanding of complex psychiatric disease?

机构信息

Department of Biological Psychology, VU University, van der Boechorststraat 1, 1081 BT, Amsterdam, the Netherlands.

出版信息

Genome Med. 2010 Sep 7;2(9):63. doi: 10.1186/gm184.

Abstract

Twin and family studies have shown the importance of biological variation in psychiatric disorders. Heritability estimates vary from 50% to 80% for cognitive disorders, such as schizophrenia, attention deficit hyperactivity disorder and autism, and from 40% to 65% for affective disorders, such as major depression, anxiety disorders and substance abuse. Pinpointing the actual genetic variants responsible for this heritability has proven difficult, even in the recent wave of genome-wide association studies. Brain endophenotypes derived from electroencephalography (EEG) have been proposed as a way to support gene-finding efforts. A variety of EEG and event-related-potential endophenotypes are linked to psychiatric disorders, and twin studies have shown a striking genetic contribution to these endophenotypes. However, the clear need for very large sample sizes strongly limits the usefulness of EEG endophenotypes in gene-finding studies. They require extended laboratory recordings with sophisticated and expensive equipment that are not amenable to epidemiology-scaled samples. Instead, EEG endophenotypes are far more promising as tools to make sense of candidate genetic variants that derive from association studies; existing clinical data from patients or questionnaire-based assessment of psychiatric symptoms in the population at large are better suited for the association studies themselves. EEG endophenotypes can help us understand where in the brain, in which stage and during what type of information processing these genetic variants have a role. Such testing can be done in the more modest samples that are feasible for EEG research. With increased understanding of how genes affect the brain, combinations of genetic risk scores and brain endophenotypes may become part of the future classification of psychiatric disorders.

摘要

双胞胎和家庭研究表明,生物学变异在精神疾病中起着重要作用。认知障碍(如精神分裂症、注意缺陷多动障碍和自闭症)的遗传率估计在 50%到 80%之间,情感障碍(如重度抑郁症、焦虑症和药物滥用)的遗传率在 40%到 65%之间。即使在最近的全基因组关联研究浪潮中,确定导致这种遗传率的实际遗传变异也证明是困难的。源自脑电图(EEG)的脑内表型已被提议作为支持基因发现工作的一种方法。各种 EEG 和事件相关电位内表型与精神疾病有关,双胞胎研究表明这些内表型具有惊人的遗传贡献。然而,对非常大的样本量的明确需求强烈限制了 EEG 内表型在基因发现研究中的有用性。它们需要使用复杂且昂贵的设备进行扩展的实验室记录,而这些设备不适用于流行病学规模的样本。相反,EEG 内表型作为理解来自关联研究的候选遗传变异的工具更有前途;现有的来自患者的临床数据或针对一般人群的精神症状的问卷调查评估更适合用于关联研究本身。EEG 内表型可以帮助我们了解这些遗传变异在大脑中的哪个部位、在哪个阶段以及在何种类型的信息处理中起作用。这种测试可以在更适合 EEG 研究的较小样本中进行。随着对基因如何影响大脑的理解的增加,遗传风险评分和脑内表型的组合可能成为未来精神疾病分类的一部分。

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