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鱼类视网膜顶盖系统中轴突生长的靶点识别与动力学

Target recognition and dynamics of axonal growth in the retinotectal system of fish.

作者信息

Stuermer C A

机构信息

Friedrich-Miescher Laboratorium, Max-Planck-Gesellschaft, Tübingen, F.R.G.

出版信息

Neurosci Res Suppl. 1990;13:S1-10. doi: 10.1016/0921-8696(90)90024-w.

Abstract

Embryonic and regenerating retinal axons in fish are able to seek out their retinotopic target sites in the tectum. Neither a specific preordering of axons in the retinotectal pathway nor activity-dependent axon-target interactions are required for appropriate axonal targeting. Axon-target recognition appears to be predominantly mediated by positional cell surface markers. The discrimination of position-dependent differences by retinal axons in a special in vitro assay is consistent with this concept. To understand retinal axonal regeneration we have analyzed the glial cells of the fish optic nerve and the expression of growth-associated cell surface molecules on the regenerating axons. The surfaces of the glial cells identified as oligodendrocytes are excellent substrates for the elongation of regenerating axons. Raising monoclonal antibodies we have found 3 cell surface proteins specific for growing axons. In the normal adult goldfish optic nerve, these proteins are only expressed by the few new axons from the newborn ganglion cells at the retinal margin. They are re-expressed on all axons during regeneration. A known cell surface molecule, NCAM, is expressed in a similar, specific spatiotemporal pattern on the fish retinal axons and may--in normal nerves--contribute to the establishment of the age-related fiber association. Whether the re-expression of NCAM and the antigens detected by the novel monoclonal antibodies are functionally involved in axonal growth and regeneration remains to be investigated.

摘要

鱼类胚胎期和再生期的视网膜轴突能够在视顶盖中找到它们的视网膜拓扑靶位点。在视网膜-视顶盖通路中,轴突既不需要特定的预排序,也不需要依赖活动的轴突-靶标相互作用来实现恰当的轴突靶向。轴突-靶标识别似乎主要由位置性细胞表面标志物介导。视网膜轴突在一种特殊的体外实验中对位置依赖性差异的辨别与这一概念相符。为了理解视网膜轴突再生,我们分析了鱼类视神经的胶质细胞以及再生轴突上生长相关细胞表面分子的表达。被鉴定为少突胶质细胞的胶质细胞表面是再生轴突伸长的优良底物。通过制备单克隆抗体,我们发现了3种生长轴突特有的细胞表面蛋白。在正常成年金鱼的视神经中,这些蛋白仅由视网膜边缘新生神经节细胞产生的少数新轴突表达。在再生过程中,它们在所有轴突上重新表达。一种已知的细胞表面分子,神经细胞黏附分子(NCAM),在鱼类视网膜轴突上以类似的、特定的时空模式表达,并且在正常神经中可能有助于建立与年龄相关的纤维联系。NCAM以及新型单克隆抗体检测到的抗原的重新表达是否在功能上参与轴突生长和再生仍有待研究。

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