The role of ependymin in the development of long lasting synaptic changes.

Journal de physiologie Pub Date : 1988-01-01
V E Shashoua
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Abstract

1.) Three types of training experiments (a complex motor task, avoidance conditioning and classical conditioning) in the goldfish and one in the mouse (T-maze learning) indicate that the brain extracellular glycoprotein (ependymin) has a role in the consolidation process of long-term memory formation. 2.) Direct ELISA measures of the concentration of ependymin in the brain extracellular fluid (ECF) indicate that its level decreases after goldfish learn to associate a light stimulus (cs) with the subsequent arrival of a shock (US): paired CS-US gave changes whereas an unpaired presentation of CS-US gave no changes in comparison to unstimulated controls. 3.) Ependymin is released into ECF and CSF as mixtures of three types of disulfide-linked dimers of two acidic polypeptide chains (M. W. 37 kDa and 31 kDa). It contains 10% carbohydrate as an N-linked glycan. 4.) Ependymin has the capacity to polymerize in response to events that deplete Ca2+ from the brain extracellular environment. A molecular hypothesis relating polymerization properties to the process of formation of long-lasting synaptic changes is proposed. 5.) Investigations of the pattern of regeneration of goldfish optic nerve and the mechanisms of long-term potentiation (LTP) of rat brain hippocampal slices suggest that ependymin has a role in the formation of long-lasting synaptic changes. The E.M. data show that polymerized products which stain with anti-ependymin sera accumulate at synapses and in new spines after LTP.

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室管素在长期突触变化发展中的作用。
1)。三种类型的训练实验(复杂运动任务、回避条件反射和经典条件反射)在金鱼和一种类型的小鼠(t迷宫学习)中表明,脑细胞外糖蛋白(室管ymin)在长期记忆形成的巩固过程中发挥作用。2)。直接ELISA法测量脑细胞外液(ECF)中室管素的浓度表明,在金鱼学会将光刺激(cs)与随后到来的电击(US)联系起来后,其水平下降:配对的cs -US产生变化,而未配对的cs -US与未刺激的对照组相比没有变化。3)。Ependymin作为两种酸性多肽链(M. W. 37 kDa和31 kDa)的三种二硫连接二聚体的混合物释放到ECF和CSF中。它含有10%的碳水化合物作为n链聚糖。4)。Ependymin具有聚合能力,以响应从大脑细胞外环境中消耗Ca2+的事件。提出了一种分子假说,将聚合特性与形成持久突触变化的过程联系起来。5)。对金鱼视神经再生模式和大鼠脑海马切片长时程增强(LTP)机制的研究表明,室管素参与了长时程突触变化的形成。emm数据显示抗室管素血清染色的聚合产物在LTP后突触和新棘中积累。
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