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自闭症谱系障碍与年龄相关的颞顶叶皮质变薄。

Age-related temporal and parietal cortical thinning in autism spectrum disorders.

机构信息

Laboratory of Brain and Cognition, National Institute of Mental Health, Bethesda, MD 20892-1366, USA.

出版信息

Brain. 2010 Dec;133(Pt 12):3745-54. doi: 10.1093/brain/awq279. Epub 2010 Oct 5.

Abstract

Studies of head size and brain volume in autism spectrum disorders have suggested that early cortical overgrowth may be followed by prematurely arrested growth. However, the few investigations quantifying cortical thickness have yielded inconsistent results, probably due to variable ages and/or small sample sizes. We assessed differences in cortical thickness between high-functioning adolescent and young adult males with autism spectrum disorders (n = 41) and matched typically developing males (n = 40). We hypothesized thinner cortex, particularly in frontal, parietal and temporal regions, for individuals with autism spectrum disorders in comparison with typically developing controls. Furthermore, we expected to find an age × diagnosis interaction: with increasing age, more pronounced cortical thinning would be observed in autism spectrum disorders than typically developing participants. T(1)-weighted magnetization prepared rapid gradient echo 3 T magnetic resonance imaging scans were acquired from high-functioning males with autism spectrum disorders and from typically developing males matched group-wise on age (range 12-24 years), intelligence quotient (≥ 85) and handedness. Both gyral-level and vertex-based analyses revealed significantly thinner cortex in the autism spectrum disorders group that was located predominantly in left temporal and parietal regions (i.e. the superior temporal sulcus, inferior temporal, postcentral/superior parietal and supramarginal gyri). These findings remained largely unchanged after controlling for intelligence quotient and after accounting for psychotropic medication usage and comorbid psychopathology. Furthermore, a significant age × diagnosis interaction was found in the left fusiform/inferior temporal cortex: participants with autism spectrum disorders had thinner cortex in this region with increasing age to a greater degree than did typically developing participants. Follow-up within group comparisons revealed significant age-related thinning in the autism spectrum disorders group but not in the typically developing group. Both thinner temporal and parietal cortices during adolescence and young adulthood and discrepantly accelerated age-related cortical thinning in autism spectrum disorders suggest that a second period of abnormal cortical growth (i.e. greater thinning) may be characteristic of these disorders.

摘要

自闭症谱系障碍的头围和脑容量研究表明,早期皮质过度生长可能随后会出现过早的生长停滞。然而,少数量化皮质厚度的研究结果不一致,可能是由于年龄不同和/或样本量小。我们评估了自闭症谱系障碍(n=41)和匹配的高功能青少年和年轻成年男性与对照组之间的皮质厚度差异。我们假设自闭症谱系障碍患者的皮质较薄,特别是在额、顶和颞叶区域,与对照组相比。此外,我们预计会发现年龄×诊断的相互作用:随着年龄的增长,自闭症谱系障碍患者的皮质变薄会更加明显,而对照组则不会。使用 T1 加权磁化准备快速梯度回波 3T 磁共振成像扫描,从自闭症谱系障碍的高功能男性和与年龄(12-24 岁)、智商(≥85)和利手匹配的对照组男性中获取。基于回波的分析和基于顶点的分析均显示自闭症谱系障碍组的皮质明显变薄,主要位于左侧颞叶和顶叶区域(即颞上回、颞下回、中央后回/上顶叶和缘上回)。在控制智商、考虑精神药物使用和共病精神病理学后,这些发现基本保持不变。此外,还发现左梭状回/颞下回存在显著的年龄×诊断相互作用:自闭症谱系障碍患者的皮质在该区域变薄,随着年龄的增长,比对照组更为明显。组内比较的随访显示自闭症谱系障碍组的皮质随年龄变薄,但对照组则没有。青少年和年轻成年时期的颞叶和顶叶皮质变薄,以及自闭症谱系障碍患者皮质变薄的速度明显加快,这表明这些疾病可能存在第二个异常皮质生长期(即更严重的变薄)。

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