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错义 DISC1 变异对双相情感障碍或精神分裂症高危两个队列大脑激活的影响。

Effects of a mis-sense DISC1 variant on brain activation in two cohorts at high risk of bipolar disorder or schizophrenia.

机构信息

Division of Psychiatry, University of Edinburgh, Royal Edinburgh Hospital, Edinburgh, UK.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2012 Apr;159B(3):343-53. doi: 10.1002/ajmg.b.32035. Epub 2012 Feb 15.

DOI:10.1002/ajmg.b.32035
PMID:22337479
Abstract

Bipolar disorder and schizophrenia share a number of clinical features and genetic risk variants of small effect, suggesting overlapping pathogenic mechanisms. The effect of single genetic risk variants on brain function is likely to differ in people at high familial risk versus controls as these individuals have a higher overall genetic loading and are therefore closer to crossing a threshold of disease liability. Therefore, whilst the effects of genetic risk variants on brain function may be similar across individuals at risk of both disorders, they are hypothesized to differ compared to that seen in control subjects. We sought to examine the effects of the DISC1 Leu(607) Phe polymorphism on brain activation in young healthy individuals at familial risk of bipolar disorder (n = 84), in a group of controls (n = 78), and in a group at familial risk of schizophrenia (n = 47), performing a language task. We assessed whether genotype effects on brain activation differed according to risk status. There was a significant genotype × group interaction in a cluster centered on the left pre/postcentral gyrus, extending to the inferior frontal gyrus. The origin of this genotype × group effect originated from a significant effect of the presumed risk variant (Phe) on brain activation in the control group, which was absent in both high-risk groups. Differential effects of this polymorphism in controls compared to the two familial groups suggests a commonality of effect across individuals at high-risk of the disorders, which is likely to be dependant upon existing genetic background.

摘要

双相情感障碍和精神分裂症具有许多临床特征和遗传风险变异,这些变异的影响较小,表明它们具有重叠的发病机制。单一遗传风险变异对脑功能的影响在高家族风险个体与对照个体之间可能存在差异,因为这些个体的整体遗传负荷更高,因此更接近疾病易感性的阈值。因此,虽然遗传风险变异对两种疾病风险个体的脑功能的影响可能相似,但与对照个体相比,它们被假设存在差异。我们试图研究 DISC1 Leu(607) Phe 多态性对双相情感障碍高家族风险的年轻健康个体(n=84)、对照组(n=78)和精神分裂症高家族风险个体(n=47)的脑激活的影响,进行语言任务。我们评估了基因型对脑激活的影响是否因风险状况而异。在以左侧额/顶叶回为中心的一个簇中,存在基因型×组的显著交互作用,延伸到额下回。这种基因型×组效应的起源源于假定风险变异(Phe)对对照组脑激活的显著影响,而在两个高风险组中则不存在这种影响。这种多态性在对照组中与两个家族组的差异影响表明,该变异在两种疾病的高风险个体中具有共同的效应,这可能依赖于现有的遗传背景。

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