Sensory processing disorders (SPD) affect 5–16% of school-aged children and can cause long-term deficits in intellectual and social development. Current theories of SPD implicate primary sensory cortical areas and higher-order multisensory integration (MSI) cortical regions. We investigate the role of white matter microstructural abnormalities in SPD using diffusion tensor imaging (DTI). DTI was acquired in 16 boys, 8–11years old, with SPD and 24 age-, gender-, handedness- and IQ-matched neurotypical controls. Behavior was characterized using a parent report sensory behavior measure, the Sensory Profile. Fractional anisotropy (FA), mean diffusivity (MD) and radial diffusivity (RD) were calculated. Tract-based spatial statistics were used to detect significant group differences in white matter integrity and to determine if microstructural parameters were significantly correlated with behavioral measures. Significant decreases in FA and increases in MD and RD were found in the SPD cohort compared to controls, primarily involving posterior white matter including the posterior corpus callosum, posterior corona radiata and posterior thalamic radiations. Strong positive correlations were observed between FA of these posterior tracts and auditory, multisensory, and inattention scores (r=0.51–0.78; p<0.001) with strong negative correlations between RD and multisensory and inattention scores (r=?0.61–0.71; p<0.001). To our knowledge, this is the first study to demonstrate reduced white matter microstructural integrity in children with SPD. We find that the disrupted white matter microstructure predominantly involves posterior cerebral tracts and correlates strongly with atypical unimodal and multisensory integration behavior. These findings suggest abnormal white matter as a biological basis for SPD and may also distinguish SPD from overlapping clinical conditions such as autism and attention deficit hyperactivity disorder. Highlights ? Abnormal posterior white matter microstructure in sensory processing disorders (SPD) ? Posterior cerebral white matter microstructure correlates with sensory behavior. ? DTI may help distinguish SPD from autism spectrum disorder and ADHD. ? DTI may yield prognostic and predictive biomarkers of SPD for clinical use.
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机译:感官加工障碍(SPD)影响5-16%的学龄儿童,并可能导致智力和社会发展的长期缺陷。 SPD的当前理论牵涉主要的感觉皮层区域和高阶多感觉集成(MSI)皮层区域。我们调查使用扩散张量成像(DTI)的SPD中的白质微结构异常的作用。 DTI在16例8-11岁的男孩中获得,具有SPD和24个与年龄,性别,惯用性和智商相匹配的神经型对照。使用上级报告的感觉行为量度“感觉概况”来表征行为。计算了分数各向异性(FA),平均扩散率(MD)和径向扩散率(RD)。基于区域的空间统计数据可用于检测白质完整性的显着组差异,并确定微结构参数是否与行为指标显着相关。与对照组相比,在SPD队列中发现FA显着下降,MD和RD显着增加,主要涉及后白质,包括后体,后冠放射和丘脑后辐射。在这些后道的FA与听觉,多感觉和注意力不集中得分之间观察到强烈的正相关(r = 0.51–0.78; p <0.001),而RD与多感觉和注意力不集中得分之间存在强烈的负相关(r =?0.61-0.71; p <0.001)。据我们所知,这是第一项证明SPD患儿白质微结构完整性降低的研究。我们发现,破坏的白质微观结构主要涉及后脑束,并且与非典型单峰和多感觉整合行为强烈相关。这些发现表明异常白质是SPD的生物学基础,也可能使SPD与重叠的临床疾病(例如自闭症和注意缺陷多动障碍)区分开来。强调 ?感觉加工障碍(SPD)中后白质组织异常?后脑白质微结构与感觉行为相关。 ? DTI可能有助于区分SPD与自闭症谱系障碍和ADHD。 ? DTI可能会产生SPD的预后和预测生物标志物,以用于临床。
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