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The Reelin Receptors Apoer2 and Vldlr Coordinate the Patterning of Purkinje Cell Topography in the Developing Mouse Cerebellum

机译:Reelin受体Apoer2和Vldlr协调发育中的小鼠小脑浦肯野细胞地形图的模式。

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摘要

The adult cerebellar cortex is comprised of reproducible arrays of transverse zones and parasagittal stripes of Purkinje cells. Adult stripes are created through the perinatal rostrocaudal dispersion of embryonic Purkinje cell clusters, triggered by signaling through the Reelin pathway. Reelin is secreted by neurons in the external granular layer and deep cerebellar nuclei and binds to two high affinity extracellular receptors on Purkinje cells-the Very low density lipoprotein receptor (Vldlr) and apolipoprotein E receptor 2 (Apoer2). In mice null for either Reelin or double null for Vldlr and Apoer2, Purkinje cell clusters fail to disperse. Here we report that animals null for either Vldlr or Apoer2 individually, exhibit specific and parasagittally-restricted Purkinje cell ectopias. For example, in mice lacking Apoer2 function immunostaining reveals ectopic Purkinje cells that are largely restricted to the zebrin II-immunonegative population of the anterior vermis. In contrast, mice null for Vldlr have a much larger population of ectopic Purkinje cells that includes members from both the zebrin II-immunonegative and -immunopositive phenotypes. HSP25 immunoreactivity reveals that in Vldlr null animals a large portion of zebrin II-immunopositive ectopic cells are probably destined to become stripes in the central zone (lobules VI–VII). A small population of ectopic zebrin II-immunonegative Purkinje cells is also observed in animals heterozygous for both receptors (Apoer2+/−: Vldlr+/−), but no ectopia is present in mice heterozygous for either receptor alone. These results indicate that Apoer2 and Vldlr coordinate the dispersal of distinct, but overlapping subsets of Purkinje cells in the developing cerebellum.
机译:成年小脑皮层由可重复的横向区域阵列和浦肯野细胞的矢状旁条纹组成。成年的条纹是通过胚胎的浦肯野细胞簇的围产期尾状尾核分散体产生的,并通过Reelin途径的信号触发。 Reelin由外部颗粒层和小脑深核中的神经元分泌,并与Purkinje细胞上的两个高亲和力细胞外受体结合-超低密度脂蛋白受体(Vldlr)和载脂蛋白E受体2(Apoer2)。在小鼠中,Reelin无效或Vldlr和Apoer2无效,浦肯野细胞簇无法分散。在这里,我们报告动物为Vldlr或Apoer2单独无效,表现出特定的和腹主旁限制的Purkinje细胞异视症。例如,在缺乏Apoer2功能的小鼠中,免疫染色揭示了异位的Purkinje细胞,该细胞主要局限于前to的Zebrin II-免疫阴性人群。相反,对Vldlr无效的小鼠具有异位的Purkinje细胞群,其包括来自zebrin II-免疫阳性和-免疫阳性表型的成员。 HSP25的免疫反应性表明,在无Vldlr动物中,大部分Zebrin II-免疫阳性异位细胞可能注定会在中央区(小叶VI-VII)变成条纹。在两种受体杂合的动物中也观察到少量的异位斑马蛋白II免疫浦肯野细胞(Apoer2 +/-:Vldlr +/-),但在小鼠中不存在仅对任一受体杂合的异盲。这些结果表明,Apoer2和Vldlr协调了发育中的小脑中不同但重叠的Purkinje细胞子集的扩散。

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