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强迫症的神经认知内表型

Neurocognitive endophenotypes of obsessive-compulsive disorder.

作者信息

Menzies Lara, Achard Sophie, Chamberlain Samuel R, Fineberg Naomi, Chen Chi-Hua, del Campo Natalia, Sahakian Barbara J, Robbins Trevor W, Bullmore Ed

机构信息

Brain Mapping Unit, University of Cambridge, Cambridge, UK.

出版信息

Brain. 2007 Dec;130(Pt 12):3223-36. doi: 10.1093/brain/awm205. Epub 2007 Sep 13.

DOI:10.1093/brain/awm205
PMID:17855376
Abstract

Endophenotypes (intermediate phenotypes) are objective, heritable, quantitative traits hypothesized to represent genetic risk for polygenic disorders at more biologically tractable levels than distal behavioural and clinical phenotypes. It is theorized that endophenotype models of disease will help to clarify both diagnostic classification and aetiological understanding of complex brain disorders such as obsessive-compulsive disorder (OCD). To investigate endophenotypes in OCD, we measured brain structure using magnetic resonance imaging (MRI), and behavioural performance on a response inhibition task (Stop-Signal) in 31 OCD patients, 31 of their unaffected first-degree relatives, and 31 unrelated matched controls. Both patients and relatives had delayed response inhibition on the Stop-Signal task compared with healthy controls. We used a multivoxel analysis method (partial least squares) to identify large-scale brain systems in which anatomical variation was associated with variation in performance on the response inhibition task. Behavioural impairment on the Stop-Signal task, occurring predominantly in patients and relatives, was significantly associated with reduced grey matter in orbitofrontal and right inferior frontal regions and increased grey matter in cingulate, parietal and striatal regions. A novel permutation test indicated significant familial effects on variation of the MRI markers of inhibitory processing, supporting the candidacy of these brain structural systems as endophenotypes of OCD. In summary, structural variation in large-scale brain systems related to motor inhibitory control may mediate genetic risk for OCD, representing the first evidence for a neurocognitive endophenotype of OCD.

摘要

内表型(中间表型)是客观、可遗传的定量性状,被假定为在比远端行为和临床表型更易于进行生物学研究的水平上代表多基因疾病的遗传风险。理论认为,疾病的内表型模型将有助于阐明复杂脑疾病如强迫症(OCD)的诊断分类和病因学理解。为了研究强迫症的内表型,我们使用磁共振成像(MRI)测量了31名强迫症患者、31名未受影响的一级亲属以及31名无关匹配对照的脑结构,并在一项反应抑制任务(停止信号任务)中测量了他们的行为表现。与健康对照相比,患者和亲属在停止信号任务中的反应抑制均延迟。我们使用一种多体素分析方法(偏最小二乘法)来识别大规模脑系统,其中解剖结构变异与反应抑制任务表现的变异相关。停止信号任务中的行为损害主要发生在患者和亲属中,与眶额和右下额叶区域灰质减少以及扣带回、顶叶和纹状体区域灰质增加显著相关。一项新的置换检验表明,家族对抑制加工的MRI标记变异有显著影响,支持这些脑结构系统作为强迫症内表型的候选资格。总之,与运动抑制控制相关的大规模脑系统的结构变异可能介导强迫症的遗传风险,这是强迫症神经认知内表型的首个证据。

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