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成年小鼠受损视神经纤维中NCAM - 180免疫反应性增加及L1免疫反应性维持

Increased NCAM-180 immunoreactivity and maintenance of L1 immunoreactivity in injured optic fibers of adult mice.

作者信息

Becker C G, Becker T, Meyer R L

机构信息

Department of Developmental and Cell Biology, University of California, Irvine, CA 92697-2275, USA.

出版信息

Exp Neurol. 2001 Jun;169(2):438-48. doi: 10.1006/exnr.2001.7657.

Abstract

The injury related expression of two axon-growth promoting cell adhesion molecules (CAMs), NCAM-180 which is developmentally downregulated and L1 which is regionally restricted, were compared in optic fibers in the adult mouse. The neuron-specific isoform of NCAM (NCAM-180) is present at very low levels in unlesioned adult optic axons. At 7 days after nerve crush, immunoreactivity was strongly and uniformly increased in optic axons within the nerve and throughout retina. Reactivity in surviving axons had returned to control levels at 4 weeks. To induce regrowth of adult retinal ganglion cell axons retinal explants were placed in culture. Strong NCAM-180 staining was observed on these regenerating optic axons. The neuronal cell adhesion molecule L1 is restricted to retina and to the unmyelinated segment of the optic nerve near the optic nerve head in unlesioned adult animals. Following nerve crush, L1 immunoreactivity was retained within retina and proximal nerve and novel staining was detected in the more distal segment of the optic nerve up to the lesion site where it persisted for at least eight months. The capacity of optic fibers to show increased NCAM-180 immunoreactivity and maintain L1 expression after a lesion may explain why these fibers exhibit relatively good potential for regeneration.

摘要

在成年小鼠的视神经纤维中,比较了两种促进轴突生长的细胞粘附分子(CAMs)——发育过程中表达下调的神经细胞粘附分子180(NCAM - 180)和区域受限的L1分子——与损伤相关的表达情况。神经细胞粘附分子(NCAM)的神经元特异性异构体(NCAM - 180)在未受损的成年视神经轴突中的表达水平非常低。在神经挤压伤后7天,神经内和整个视网膜中的视神经轴突免疫反应性强烈且均匀增加。在4周时,存活轴突中的反应性已恢复到对照水平。为诱导成年视网膜神经节细胞轴突再生,将视网膜外植体置于培养中。在这些再生的视神经轴突上观察到强烈的NCAM - 180染色。在未受损的成年动物中,神经元细胞粘附分子L1局限于视网膜和靠近视神经乳头的视神经无髓鞘段。神经挤压伤后,L1免疫反应性保留在视网膜和近端神经内,并且在视神经更远端直至损伤部位检测到新的染色,这种染色持续至少八个月。损伤后视神经纤维显示NCAM - 180免疫反应性增加和维持L1表达的能力,可能解释了为什么这些纤维表现出相对良好的再生潜力。

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