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自闭症儿童的神经元核和细胞质体积不足,而青少年和成年人的体积增加。

Neuronal nucleus and cytoplasm volume deficit in children with autism and volume increase in adolescents and adults.

出版信息

Acta Neuropathol Commun. 2015 Jan 17;3:2. doi: 10.1186/s40478-015-0183-5.

Abstract

INTRODUCTION

Characterization of the type and topography of structural changes and their alterations throughout the lifespan of individuals with autism is essential for understanding the mechanisms contributing to the autistic phenotype. The aim of this stereological study of neurons in 16 brain structures of 14 autistic and 14 control subjects from 4 to 64 years of age was to establish the course of neuronal nuclear and cytoplasmic volume changes throughout the lifespan of individuals with autism.

RESULTS

Our data indicate that a deficit of neuronal soma volume in children with autism is associated with deficits in the volume of the neuronal nucleus and cytoplasm. The significant deficits of neuronal nuclear and cytoplasmic volumes in 13 of 16 examined subcortical structures, archicortex, cerebellum, and brainstem in 4- to 8-year-old autistic children suggest a global nature of brain developmental abnormalities, but with region-specific differences in the severity of neuronal pathology. The observed increase in nuclear volumes in 8 of 16 structures in the autistic teenagers/young adults and decrease in nuclear volumes in 14 of 16 regions in the age-matched control subjects reveal opposite trajectories throughout the lifespan. The deficit in neuronal nuclear volumes, ranging from 7% to 42% in the 16 examined regions in children with autism, and in neuronal cytoplasmic volumes from 1% to 31%, as well as the broader range of interindividual differences for the nuclear than the cytoplasmic volume deficits, suggest a partial distinction between nuclear and cytoplasmic pathology.

CONCLUSIONS

The most severe deficit of both neuronal nucleus and cytoplasm volume in 4-to 8-year-old autistic children appears to be a reflection of early developmental alterations that may have a major contribution to the autistic phenotype. The broad range of functions of the affected structures implies that their developmental and age-associated abnormalities contribute not only to the diagnostic features of autism but also to the broad spectrum of clinical alterations associated with autism. Lack of clinical improvement in autistic teenagers and adults indicates that the observed increase in neuron nucleus and cytoplasm volume close to control level does not normalize brain function.

摘要

简介

描述自闭症个体一生中结构变化的类型和拓扑结构及其变化对于理解促成自闭症表型的机制至关重要。本研究对 14 名自闭症患者和 14 名对照者的 16 个脑区的神经元进行了体视学研究,旨在确定自闭症个体一生中神经元核和细胞质体积变化的过程。

结果

我们的数据表明,自闭症儿童的神经元体体积缺陷与神经元核和细胞质体积缺陷有关。在 4 至 8 岁自闭症儿童的 16 个皮质下结构、古皮质、小脑和脑干中,有 13 个的神经元核和细胞质体积显著减少,这表明大脑发育异常具有普遍性,但在神经元病变的严重程度上存在区域特异性差异。在 8 岁的自闭症青少年/年轻成人中,16 个结构中有 8 个的核体积增加,而在年龄匹配的对照组中,16 个区域中有 14 个的核体积减少,这表明在整个生命过程中存在相反的轨迹。自闭症儿童 16 个检查区域的神经元核体积减少 7%至 42%,神经元细胞质体积减少 1%至 31%,以及核体积缺陷的个体间差异范围比细胞质体积缺陷更广泛,这表明核和细胞质病理存在部分区别。

结论

4 至 8 岁自闭症儿童的神经元核和细胞质体积都出现最严重的缺陷,这似乎反映了早期发育的改变,这些改变可能对自闭症表型有重大贡献。受影响结构的广泛功能意味着它们的发育和年龄相关异常不仅有助于自闭症的诊断特征,也有助于与自闭症相关的广泛临床改变。自闭症青少年和成年人的临床改善缺乏表明,观察到的神经元核和细胞质体积接近对照水平的增加并没有使大脑功能正常化。

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