首页> 外文期刊>Journal of Neuroscience Research >Cell adhesion molecule L1 promotes neurite outgrowth of septal neurons.
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Cell adhesion molecule L1 promotes neurite outgrowth of septal neurons.

机译:细胞粘附分子L1促进间隔神经元的神经突向外生长。

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摘要

To establish if the cell adhesion molecule L1 could promote neurite outgrowth of septal neurons, L1-positive substrates were prepared by genetically modifying 3T3 fibroblasts with a retroviral vector encoding human L1 under the control of a negative tetracycline-regulatory system. In several clones of L1-transfected fibroblasts, L1 expression at the cell surface was prominent and efficiently regulated by doxycycline, a tetracycline analogue. In co-culture of septal neurons and fibroblasts, a two-dimensional fractionator probe provided systematic random sampling of the neurites to be measured. Septal neurons, isolated at embryonic Day 17, were found to express L1 in vitro and to extend significantly longer neurites when plated on L1-expressing fibroblasts compared to control fibroblasts. The neurite outgrowth-promoting effect of L1 was inhibited after a doxycycline treatment, which specifically suppressed L1 expression from the modified fibroblasts. The findings that septal neurons at embryonic Day 17 in vitro express L1 and respond to L1-modulation suggest that this molecule is involved in development of the septohippocampal pathway.
机译:为了确定细胞粘附分子L1是否能促进间隔神经元的神经突向外生长,通过在负四环素调节系统的控制下,用编码人L1的逆转录病毒载体对3T3成纤维细胞进行遗传修饰,从而制备L1阳性底物。在L1转染的成纤维细胞的几个克隆中,L1在细胞表面的表达是突出的,并被强力霉素(一种四环素类似物)有效地调节。在间隔神经元和成纤维细胞的共培养中,二维分馏探针可对要测量的神经突提供系统的随机采样。与对照成纤维细胞相比,发现在胚胎第17天分离出的间隔神经元在体外表达L1,并且当铺在表达L1的成纤维细胞上时,其神经突明显延长。强力霉素处理后,L1的神经突生长促进作用受到抑制,这特别抑制了修饰的成纤维细胞中L1的表达。隔壁神经元在胚胎第17天在体外表达L1并响应L1调节的发现表明,该分子参与了海马海马通路的发育。

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