自闭症谱系障碍高家族风险婴儿的共同注意与丘脑和海马宏观结构的关系

Cerebral cortex communications Pub Date : 2022-07-22 eCollection Date: 2022-01-01 DOI:10.1093/texcom/tgac029
Julia T P Montenegro, Diane Seguin, Emma G Duerden
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摘要

自闭症谱系障碍(ASD)是一种遗传性神经发育障碍。被诊断为ASD的婴儿可以表现出自发注视跟随的损伤,并且很少参与联合注意(JA)。启动JA (IJA)的能力比响应JA (RJA)的能力更明显受损。在一项纵向研究中,101名有ASD家族风险的婴儿被纳入研究(62%为男性)。参与者在4或6个月大时完成了磁共振成像扫描。皮质下体积(丘脑、海马、杏仁核、基底神经节、间脑腹侧和小脑)被自动提取。采用标准化方法评估早期凝视和JA行为。大多数婴儿对IJA无反应(n = 93,92%),超过一半的婴儿对RJA无反应(n = 50,52%)。在无反应组中,测试皮层下体积与后来的ASD诊断之间关系的模型考虑了年龄、性别和脑体积。在IJA无反应组,采用回归方法,左侧海马(B = -0.009, aOR = 0.991, P = 0.025)、右侧丘脑(B = -0.016, aOR = 0.984, P = 0.026)、左侧丘脑(B = 0.015, aOR = 1.015, P = 0.019)预测ASD的后期诊断。未参与IJA的高危婴儿的丘脑和海马宏观结构的改变可能反映了易感性的增强,并可能是后期ASD发展的关键预测因素。
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Joint attention in infants at high familial risk for autism spectrum disorder and the association with thalamic and hippocampal macrostructure.

Autism spectrum disorder (ASD) is a heritable neurodevelopmental disorder. Infants diagnosed with ASD can show impairments in spontaneous gaze-following and will seldom engage in joint attention (JA). The ability to initiate JA (IJA) can be more significantly impaired than the ability to respond to JA (RJA). In a longitudinal study, 101 infants who had a familial risk for ASD were enrolled (62% males). Participants completed magnetic resonance imaging scans at 4 or 6 months of age. Subcortical volumes (thalamus, hippocampus, amygdala, basal ganglia, ventral diencephalon, and cerebellum) were automatically extracted. Early gaze and JA behaviors were assessed with standardized measures. The majority of infants were IJA nonresponders (n = 93, 92%), and over half were RJA nonresponders (n = 50, 52%). In the nonresponder groups, models testing the association of subcortical volumes with later ASD diagnosis accounted for age, sex, and cerebral volumes. In the nonresponder IJA group, using regression method, the left hippocampus (B = -0.009, aOR = 0.991, P = 0.025), the right thalamus (B = -0.016, aOR = 0.984, P = 0.026), as well as the left thalamus (B = 0.015, aOR = 1.015, P = 0.019), predicted later ASD diagnosis. Alterations in thalamic and hippocampal macrostructure in at-risk infants who do not engage in IJA may reflect an enhanced vulnerability and may be the key predictors of later ASD development.

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