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脑细胞外蛋白在神经可塑性和学习中的作用。

The role of brain extracellular proteins in neuroplasticity and learning.

作者信息

Shashoua V E

出版信息

Cell Mol Neurobiol. 1985 Jun;5(1-2):183-207. doi: 10.1007/BF00711092.

Abstract

Double labeling studies of the pattern of protein synthesis in goldfish and mouse brain identified a class of glycoproteins (the ependymins) whose turnover rate was enhanced after training. A variety of control experiments indicated that these macromolecules have an important role in the molecular and cell biology of learning. Antisera to the ependymins when injected into the brains of trained goldfish cause amnesia of a newly acquired behavior. Isolation and localization studies by immunocytochemical methods indicate that the ependymins are released into the brain extracellular fluid by a class of neurosecretory cells. In mammalian brain ependymin-containing cells are highly concentrated in the limibic system. The ependymins are constituted from two disulfide-linked acidic polypeptide chains (M.W.37K and 31K). They contain at least 5% covalently bound carbohydrate per chain with mannose, galactose, N-acetylglucosamine and N-acetylneuraminic acid as the predominant components. The highly soluble ependymins can rapidly polymerize to form an insoluble fibrous matrix if calcium is removed from solution by the addition of a Ca2+-chelating agent or dialysis. The self-aggregation property of the ependymins can be triggered by the depletion of Ca2+ from the extracellular space. Studies of the kinetics of the aggregation phenomenon by measurements of turbidity changes indicate that the process can be terminated but not reversed by restoring Ca2+ to its normal CSF level. Immunohistochemical studies of the brains of trained goldfish show the presence of punctate statining sites in the perimeter of certain cells located in specific brain regions. This suggests that ependymin aggregation might occur in vivo during learning. A molecular hypothesis relating the aggregation properties of the ependymins to neuroplasticity and learning is proposed.

摘要

对金鱼和小鼠大脑中蛋白质合成模式的双重标记研究确定了一类糖蛋白(室管膜蛋白),其更新率在训练后会提高。各种对照实验表明,这些大分子在学习的分子和细胞生物学中具有重要作用。将抗室管膜蛋白的抗血清注入受过训练的金鱼大脑中,会导致新习得行为的失忆。通过免疫细胞化学方法进行的分离和定位研究表明,室管膜蛋白由一类神经分泌细胞释放到脑细胞外液中。在哺乳动物大脑中,含室管膜蛋白的细胞高度集中在边缘系统。室管膜蛋白由两条通过二硫键连接的酸性多肽链(分子量分别为37K和31K)组成。每条链至少含有5%的共价结合碳水化合物,主要成分是甘露糖、半乳糖、N-乙酰葡糖胺和N-乙酰神经氨酸。如果通过添加Ca2+螯合剂或透析从溶液中去除钙,高度可溶的室管膜蛋白会迅速聚合形成不溶性纤维基质。室管膜蛋白的自聚集特性可由细胞外空间中Ca2+的耗尽引发。通过测量浊度变化对聚集现象动力学的研究表明,通过将Ca2+恢复到正常脑脊液水平,该过程可以终止但不能逆转。对受过训练的金鱼大脑进行的免疫组织化学研究表明,在特定脑区的某些细胞周边存在点状染色位点。这表明室管膜蛋白聚集可能在学习过程中在体内发生。提出了一个将室管膜蛋白的聚集特性与神经可塑性和学习相关联的分子假说。

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