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High Expression of Doublecortin and KIAA0369 Protein in Fetal Brain Suggests Their Specific Role in Neuronal Migration

机译:Doublecortin和KIAA0369蛋白在胎儿脑中的高表达表明它们在神经元迁移中的特定作用。

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摘要

The X-linked subcortical laminar heterotopia and lissencephaly syndrome is a disorder of neuronal migration caused by a mutation in XLIS, a recently cloned gene on chromosome Xq22.3-q23. The predicted protein product for XLIS, doublecortin (DC), shows high homology to a putative calcium calmodulin-dependent kinase, KIAA0369 protein (KI). Here we identified DC and KI in the brains of human and rat fetuses by immunochemical and immunohistochemical means. In this study, Western blotting demonstrated that both DC and KI are specific to the nervous system and are abundant during the fetal period, around 20 gestational weeks in humans and embryonic days 17 to 20 in rats. Immunostaining of the developing neocortex disclosed localization of DC and KI immunoreactivities in neuronal cell bodies and processes in the zones of ongoing neuronal migration. Although KI showed a somewhat wider distribution than DC, the temporal and spatial patterns of their expression were similar. These results suggest that DC and KI participate in a common signaling pathway regulating neuronal migration.
机译:X连锁皮层下层异位症和lissencephaly综合征是由XLIS突变引起的神经元迁移疾病,XLIS是Xq22.3-q23染色体上最近克隆的基因。 XLIS的预测蛋白产物双皮质素(DC)与假定的钙调蛋白依赖性激酶KIAA0369蛋白(KI)具有高度同源性。在这里,我们通过免疫化学和免疫组织化学方法鉴定了人和大鼠胎儿脑中的DC和KI。在这项研究中,蛋白质印迹证明DC和KI都对神经系统具有特异性,并且在胎儿期,人类约20个孕周和大鼠胚胎第17至20天都丰富。发育中的新皮层的免疫染色揭示了DC和KI免疫反应性在正在进行的神经元迁移区域中的神经元细胞体和过程中的定位。尽管KI的分布比DC稍宽,但其表达的时空格局却相似。这些结果表明DC和KI参与调节神经元迁移的共同信号通路。

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