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一种阻断神经突再生促进因子活性的单克隆抗体:结合位点及其体内定位研究

A monoclonal antibody that blocks the activity of a neurite regeneration-promoting factor: studies on the binding site and its localization in vivo.

作者信息

Chiu A Y, Matthew W D, Patterson P H

出版信息

J Cell Biol. 1986 Oct;103(4):1383-98. doi: 10.1083/jcb.103.4.1383.

Abstract

Work from several laboratories has identified a proteoglycan complex secreted by a variety of non-neuronal cells that can promote neurite regeneration when applied to the surface of culture dishes. Using a novel immunization protocol, a monoclonal antibody (INO) was produced that blocks the activity of this outgrowth-promoting factor (Matthew, W. D., and P. H. Patterson, 1983, Cold Spring Harbor Symp. Quant. Biol. 48:625-631). We have used the antibody to analyze the components of the active site and to localize the complex in vivo. INO binding is lost when the complex is dissociated; if its components are selectively reassociated, INO binds only to a complex containing two different molecular weight species. These are likely to be laminin and heparan sulfate proteoglycan, respectively. On frozen sections of adult rat tissues, INO binding is present on the surfaces of glial cells of the peripheral, but not the central, nervous system. INO also binds to the basement membrane surrounding cardiac and skeletal muscle cells, and binding to the latter greatly increases after denervation. In the adrenal gland and kidney, INO selectively reacts with areas rich in basement membranes, staining a subset of structures that are immunoreactive for both laminin and heparan sulfate proteoglycan. In general, the outgrowth-blocking antibody binds to areas known to promote axonal regeneration and is absent from areas known to lack this ability. This suggests that this complex, which is active in culture, may be the physiological substrate supporting nerve regeneration in vivo.

摘要

多个实验室的研究工作已鉴定出一种由多种非神经细胞分泌的蛋白聚糖复合物,将其应用于培养皿表面时可促进神经突再生。采用一种新的免疫方案,制备了一种单克隆抗体(INO),该抗体可阻断这种促进生长因子的活性(马修,W.D.,和P.H.帕特森,1983年,《冷泉港定量生物学研讨会》48:625 - 631)。我们已使用该抗体分析活性位点的成分并在体内定位该复合物。当复合物解离时,INO结合丧失;如果其成分选择性重新结合,INO仅与包含两种不同分子量物种的复合物结合。这两种物种可能分别是层粘连蛋白和硫酸乙酰肝素蛋白聚糖。在成年大鼠组织的冰冻切片上,INO结合存在于外周神经系统而非中枢神经系统的神经胶质细胞表面。INO也与心脏和骨骼肌细胞周围的基底膜结合,去神经支配后与后者的结合大大增加。在肾上腺和肾脏中,INO选择性地与富含基底膜的区域反应,使对层粘连蛋白和硫酸乙酰肝素蛋白聚糖均具有免疫反应性的一部分结构染色。一般来说,这种生长阻断抗体与已知促进轴突再生的区域结合,而在已知缺乏这种能力的区域则不存在。这表明这种在培养中具有活性的复合物可能是体内支持神经再生的生理底物。

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