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轴突多唾液酸神经细胞黏附分子表达的下调与人类胎儿前脑髓鞘形成的起始同时发生。

Down-regulation of the axonal polysialic acid-neural cell adhesion molecule expression coincides with the onset of myelination in the human fetal forebrain.

作者信息

Jakovcevski I, Mo Z, Zecevic N

机构信息

Neuroscience Department, University of Connecticut Health Center, 263 Farmington Avenue, Farmington, CT 06030-3401, USA.

出版信息

Neuroscience. 2007 Oct 26;149(2):328-37. doi: 10.1016/j.neuroscience.2007.07.044. Epub 2007 Aug 8.

Abstract

The polysialic acid (PSA) modification of neural cell adhesion molecule, which reduces neural cell adhesion molecule (NCAM) - mediated cell adhesion, is involved in several developmental processes, such as cell migration, axonal growth, path finding, and synaptic plasticity. It has been suggested that PSA-NCAM expression may inhibit myelination. To clarify the relationship between myelination and the expression of PSA-NCAM we systematically investigated its expression in the human forebrain from embryonic stage to midgestation (19-24 gestation weeks, gw). Immunofluorescence on cryosections showed that PSA-NCAM is expressed at the earliest stage studied (5.5 gw) in the primordial plexiform layer of the telencephalon, which mainly consists of neuronal processes. At midgestation, cortical axonal tracts in the emerging white matter were PSA-NCAM+, but they were not yet myelinated, based on the lack of myelin basic protein (MBP) immunoreaction. To follow the progression of myelination we developed organotypic slice cultures that included the subventricular and intermediate zones of the fetal forebrain. In freshly prepared slices, similar to cryosections, axonal tracts were PSA-NCAM+ but did not express MBP. After 5 days in culture there was a dramatic increase in MBP expression around the axons of the intermediate zone, which suggested the onset of myelination. Simultaneously with MBP up-regulation PSA-NCAM expression in axons was completely lost, as demonstrated both with immunofluorescence and Western blot analysis. These results support the idea that in the human fetal forebrain axonal PSA-NCAM expression is inversely related to primary myelination.

摘要

神经细胞黏附分子的多唾液酸(PSA)修饰可降低神经细胞黏附分子(NCAM)介导的细胞黏附,参与多种发育过程,如细胞迁移、轴突生长、路径寻找和突触可塑性。有人提出,PSA-NCAM的表达可能会抑制髓鞘形成。为了阐明髓鞘形成与PSA-NCAM表达之间的关系我们系统地研究了其在人类前脑从胚胎期到妊娠中期(妊娠19 - 24周,gw)的表达情况。冰冻切片的免疫荧光显示,在研究的最早阶段(5.5 gw),端脑的原始丛状层中表达PSA-NCAM,该层主要由神经突组成。在妊娠中期,新出现的白质中的皮质轴突束为PSA-NCAM阳性,但基于缺乏髓鞘碱性蛋白(MBP)免疫反应,它们尚未形成髓鞘。为了追踪髓鞘形成的进程,我们建立了包含胎儿前脑室下区和中间区的器官型切片培养体系。在新鲜制备的切片中,与冰冻切片类似,轴突束为PSA-NCAM阳性,但不表达MBP。培养5天后,中间区轴突周围的MBP表达显著增加,这表明髓鞘形成开始。与MBP上调同时,轴突中的PSA-NCAM表达完全消失,免疫荧光和蛋白质印迹分析均证实了这一点。这些结果支持了这样一种观点,即在人类胎儿前脑中,轴突PSA-NCAM的表达与初级髓鞘形成呈负相关。

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