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小鼠小脑出生后发育过程中神经细胞黏附分子L1和N-CAM的免疫电子显微镜定位

Immunoelectron microscopic localization of the neural cell adhesion molecules L1 and N-CAM during postnatal development of the mouse cerebellum.

作者信息

Persohn E, Schachner M

出版信息

J Cell Biol. 1987 Jul;105(1):569-76. doi: 10.1083/jcb.105.1.569.

DOI:10.1083/jcb.105.1.569
PMID:3301870
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2114902/
Abstract

The cellular and subcellular localization of the neural cell adhesion molecules L1 and N-CAM was studied by pre- and postembedding immunoelectron microscopic labeling procedures in the developing mouse cerebellar cortex. The salient features of the study are: L1 displays a previously unrecognized restricted expression by particular neuronal cell types (i.e., it is expressed by granule cells but not by stellate and basket cells) and by particular subcellular compartments (i.e., it is expressed on axons but not on dendrites or cell bodies of Purkinje cells). L1 is always expressed on fasciculating axons and on postmitotic, premigratory, and migrating granule cells at sites of neuron-neuron contact, but never at contact sites between neuron and glia, thus strengthening the view that L1 is not involved in granule cell migration as a neuron-glia adhesion molecule. While N-CAM antibodies reacting with the three major components of N-CAM (180, 140, and 120 kD) show a rather uniform labeling of all cell types, antibodies to the 180-kD component (N-CAM180) stain only the postmigratory granule cell bodies supporting the notion that N-CAM180, the N-CAM component with the longest cytoplasmic domain, is not expressed before stable cell contacts are formed. Furthermore, N-CAM180 is only transiently expressed on Purkinje cell dendrites. N-CAM is present in synapses on both pre- and post-synaptic membranes. L1 is expressed only preterminally and not in the subsynaptic membranes. These observations indicate an exquisite degree of fine tuning in adhesion molecule expression during neural development and suggest a rich combinatorial repertoire in the specification of cell surface contacts.

摘要

通过包埋前和包埋后免疫电子显微镜标记程序,对发育中小鼠小脑皮质中神经细胞黏附分子L1和N-CAM进行了细胞和亚细胞定位研究。该研究的显著特点是:L1在特定神经元细胞类型中表现出以前未被认识到的限制性表达(即由颗粒细胞表达,但星状细胞和篮状细胞不表达),并且在特定亚细胞区室中表达(即在轴突上表达,但在浦肯野细胞的树突或细胞体上不表达)。L1总是在成束的轴突上以及有丝分裂后、迁移前和迁移中的颗粒细胞在神经元-神经元接触部位表达,但在神经元与神经胶质细胞的接触部位从不表达,因此强化了L1作为神经元-神经胶质细胞黏附分子不参与颗粒细胞迁移的观点。与N-CAM的三种主要成分(180、140和120kD)反应的N-CAM抗体对所有细胞类型显示出相当均匀的标记,而针对180-kD成分(N-CAM180)的抗体仅对迁移后的颗粒细胞体染色,支持了N-CAM180(具有最长细胞质结构域的N-CAM成分)在稳定细胞接触形成之前不表达的观点。此外,N-CAM180仅在浦肯野细胞树突上短暂表达。N-CAM存在于突触前和突触后膜的突触中。L1仅在终末前表达,不在突触下膜表达。这些观察结果表明神经发育过程中黏附分子表达存在精细的调控程度,并提示细胞表面接触的特异性中存在丰富的组合库。

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