小脑对自闭症患者大脑皮层发育影响的多模态证据:功能紊乱中的结构生长。

IF 9.6 1区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular Psychiatry Pub Date : 2024-10-11 DOI:10.1038/s41380-024-02769-1
Federico d'Oleire Uquillas, Esra Sefik, Bing Li, Matthew A Trotter, Kara A Steele, Jakob Seidlitz, Rowen Gesue, Mariam Latif, Tristano Fasulo, Veronica Zhang, Mikhail Kislin, Jessica L Verpeut, Jonathan D Cohen, Jorge Sepulcre, Samuel S-H Wang, Jesse Gomez
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引用次数: 0

摘要

尽管围产期小脑损伤是日后被诊断为自闭症谱系障碍(ASD)的最高风险因素之一,但目前还不清楚小脑如何影响大脑皮层的发育,以及这种共同发育过程在神经畸形儿童和自闭症谱系障碍儿童之间是否存在差异。我们利用神经畸形儿童和被诊断患有 ASD 的儿童的大型结构性脑磁共振成像数据集,研究了不同个体的小脑组织结构变异是否与发育过程中的新皮质变异相关,包括作为耦合因子的丘脑。我们发现,丘脑在调节 ASD 患者的大脑-小脑结构协调方面发挥着独特的作用。值得注意的是,小脑、丘脑和新皮层之间的结构耦合在幼年时期最强,到青春期早期则逐渐减弱,这反映了以前未曾描述过的ASD儿童和神经畸形儿童之间的行为发展轨迹。互补功能连接分析同样揭示了ASD患者小脑和新皮层之间的非典型连接。这种关系在预测功能连接的小脑结构模型中尤为突出,在该模型中,ASD 儿童和神经畸形儿童表现出不同的模式。有趣的是,这些功能-结构关系随着年龄的增长而变得更加突出,而结构效应在儿童早期最为突出,并表现出明显的侧向性。这种模式可能暗示了一种发育顺序,即早期各区域之间结构生长不协调,随后功能同步越来越不典型。这些发现为自闭症的小脑发育不良模型提供了活体大脑中的多模态证据,其中小脑-大脑结构耦合的增加和大脑-小脑通路功能连接的改变都有助于这种神经发育障碍的本体发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Multimodal evidence for cerebellar influence on cortical development in autism: structural growth amidst functional disruption.

Despite perinatal damage to the cerebellum being one of the highest risk factors for later being diagnosed with autism spectrum disorder (ASD), it is not yet clear how the cerebellum might influence the development of cerebral cortex and whether this co-developmental process is distinct between neurotypical and ASD children. Leveraging a large structural brain MRI dataset of neurotypical children and those diagnosed with ASD, we examined whether structural variation in cerebellar tissue across individuals was correlated with neocortical variation during development, including the thalamus as a coupling factor. We found that the thalamus plays a distinct role in moderating cerebro-cerebellar structural coordination in ASD. Notably, structural coupling between cerebellum, thalamus, and neocortex was strongest in younger childhood and waned by early adolescence, mirroring a previously undescribed trajectory of behavioral development between ASD and neurotypical children. Complementary functional connectivity analyses likewise revealed atypical connectivity between cerebellum and neocortex in ASD. This relationship was particularly prominent in a model of cerebellar structure predicting functional connectivity, where ASD and neurotypical children showed divergent patterns. Interestingly, these functional-structural relationships became more prominent with age, while structural effects were most prominent earlier in childhood, and showed significant lateralization. This pattern may suggest a developmental sequence where early uncoordinated structural growth amongst regions is followed by increasingly atypical functional synchronization. These findings provide multimodal evidence in the living brain for a cerebellar diaschisis model of autism, where both increased cerebellar-cerebral structural coupling and altered functional connectivity in cerebro-cerebellar pathways contribute to the ontogeny of this neurodevelopmental disorder.

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来源期刊
Molecular Psychiatry
Molecular Psychiatry 医学-精神病学
CiteScore
20.50
自引率
4.50%
发文量
459
审稿时长
4-8 weeks
期刊介绍: Molecular Psychiatry focuses on publishing research that aims to uncover the biological mechanisms behind psychiatric disorders and their treatment. The journal emphasizes studies that bridge pre-clinical and clinical research, covering cellular, molecular, integrative, clinical, imaging, and psychopharmacology levels.
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