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唐氏综合征胎儿的大脑并非普遍存在细胞缺陷。

Cellularity Defects Are Not Ubiquitous in the Brains of Fetuses With Down Syndrome.

机构信息

Department for Life Quality Studies, University of Bologna, Rimini, Italy.

Pathology Unit, Azienda Unità Sanitaria Locale - IRCCS, Reggio Emilia, Italy.

出版信息

Dev Neurobiol. 2024 Oct;84(4):264-273. doi: 10.1002/dneu.22953. Epub 2024 Sep 30.

DOI:10.1002/dneu.22953
PMID:39344402
Abstract

Down syndrome (DS) is a genetic pathology characterized by various developmental defects. Unlike other clinical problems, intellectual disability is an invariant clinical trait of DS. Impairment of neurogenesis accompanied by brain hypotrophy is a typical neurodevelopmental phenotype of DS, suggesting that a reduction in the number of cells forming the brain may be a key determinant of intellectual disability. Previous evidence showed that fetuses with DS exhibit widespread hypocellularity in brain regions belonging to the temporal lobe memory systems, which may account for the typical explicit memory impairment that characterizes DS. In the current study, we have examined the basal ganglia, the insular cortex (INS), and the cingulate cortex (CCX) of fetuses with DS and age-matched controls (18-22 weeks of gestation), to establish whether cellularity defects involve regions that are not primarily involved in explicit memory. We found that fetuses with DS exhibit a notable hypocellularity in the putamen (-30%) and globus pallidus (-35%). In contrast, no cellularity differences were found in the INS and CCX, indicating that hypocellularity is not ubiquitous in the DS brain. The hypocellularity found in the basal ganglia, which are critically implicated in the control of movement, suggests that such alterations may contribute to the motor abnormalities of DS. The normal cytoarchitecture of the INS and CCX suggests that the alterations exhibited by people with DS in functions in which these regions are involved are not attributable to neuron paucity.

摘要

唐氏综合征(DS)是一种以多种发育缺陷为特征的遗传病理学。与其他临床问题不同,智力障碍是 DS 的一个不变的临床特征。神经发生受损伴随着脑萎缩是 DS 的典型神经发育表型,这表明形成大脑的细胞数量减少可能是智力障碍的关键决定因素。先前的证据表明,患有 DS 的胎儿在属于颞叶记忆系统的脑区表现出广泛的细胞减少,这可能解释了 DS 典型的明确记忆障碍。在本研究中,我们检查了唐氏综合征胎儿和年龄匹配的对照组(18-22 周妊娠)的基底节、岛叶皮层(INS)和扣带回皮层(CCX),以确定细胞缺陷是否涉及主要不参与明确记忆的区域。我们发现,患有 DS 的胎儿在壳核(-30%)和苍白球(-35%)中表现出明显的细胞减少。相比之下,INS 和 CCX 中没有发现细胞数量差异,这表明细胞减少并非 DS 大脑的普遍现象。基底节在运动控制中起着至关重要的作用,其细胞减少表明这种改变可能导致 DS 的运动异常。INS 和 CCX 的正常细胞结构表明,这些区域参与的功能障碍并非归因于神经元数量减少。

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