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全基因组关联分析将多个精神疾病易感性基因与脑振荡活动联系起来。

Genome-wide association analysis links multiple psychiatric liability genes to oscillatory brain activity.

机构信息

Psychiatry department, Amsterdam Neuroscience, Academic Medical Center, University of Amsterdam, The Netherlands.

Queensland Brain Institute, University of Queensland, Brisbane, Australia.

出版信息

Hum Brain Mapp. 2018 Nov;39(11):4183-4195. doi: 10.1002/hbm.24238. Epub 2018 Jun 26.

Abstract

Oscillatory activity is crucial for information processing in the brain, and has a long history as a biomarker for psychopathology. Variation in oscillatory activity is highly heritable, but current understanding of specific genetic influences remains limited. We performed the largest genome-wide association study to date of oscillatory power during eyes-closed resting electroencephalogram (EEG) across a range of frequencies (delta 1-3.75 Hz, theta 4-7.75 Hz, alpha 8-12.75 Hz, and beta 13-30 Hz) in 8,425 subjects. Additionally, we performed KGG positional gene-based analysis and brain-expression analyses. GABRA2-a known genetic marker for alcohol use disorder and epilepsy-significantly affected beta power, consistent with the known relation between GABA interneuron activity and beta oscillations. Tissue-specific SNP-based imputation of gene-expression levels based on the GTEx database revealed that hippocampal GABRA2 expression may mediate this effect. Twenty-four genes at 3p21.1 were significant for alpha power (FDR q < .05). SNPs in this region were linked to expression of GLYCTK in hippocampal tissue, and GNL3 and ITIH4 in the frontal cortex-genes that were previously implicated in schizophrenia and bipolar disorder. In sum, we identified several novel genetic variants associated with oscillatory brain activity; furthermore, we replicated and advanced understanding of previously known genes associated with psychopathology (i.e., schizophrenia and alcohol use disorders). Importantly, these psychopathological liability genes affect brain functioning, linking the genes' expression to specific cortical/subcortical brain regions.

摘要

脑内的震荡活动对信息处理非常重要,一直以来它都是精神病理学的生物标志物。震荡活动的变化具有很强的遗传性,但目前对特定遗传影响的理解仍然有限。我们对闭眼静息脑电图(EEG)在一系列频率(δ 1-3.75 Hz、θ 4-7.75 Hz、α 8-12.75 Hz 和β 13-30 Hz)下的震荡功率进行了迄今为止最大规模的全基因组关联研究,共涉及 8425 名受试者。此外,我们还进行了 KGG 位置基因的分析和大脑表达分析。GABRA2-已知的酒精使用障碍和癫痫的遗传标志物-显著影响β功率,这与 GABA 中间神经元活动与β震荡之间的已知关系一致。基于 GTEx 数据库的组织特异性 SNP 基因为基因表达水平进行的推断显示,海马体 GABRA2 的表达可能介导了这种效应。3p21.1 上的 24 个基因与α功率显著相关(FDR q < 0.05)。该区域的 SNP 与海马组织中 GLYCTK 的表达以及额叶皮质中 GNL3 和 ITIH4 的表达相关,这些基因之前与精神分裂症和双相情感障碍有关。总的来说,我们发现了一些与大脑震荡活动相关的新的遗传变异体;此外,我们还复制并进一步了解了与精神病理学相关的已知基因(即精神分裂症和酒精使用障碍)。重要的是,这些精神病理学倾向基因会影响大脑功能,将基因的表达与特定的皮质/皮质下脑区联系起来。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed52/6866340/458489da8082/HBM-39-4183-g001.jpg

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