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突触结合蛋白 I 是一种寡甘露糖载体糖蛋白,作为一种寡甘露糖结合凝集素,在通过神经胶质衍生的外泌体释放时促进神经突生长和神经元存活。

Synapsin I is an oligomannose-carrying glycoprotein, acts as an oligomannose-binding lectin, and promotes neurite outgrowth and neuronal survival when released via glia-derived exosomes.

机构信息

Zentrum für Molekulare Neurobiologie, Universitätsklinikum Hamburg-Eppendorf, 20246 Hamburg, Germany.

出版信息

J Neurosci. 2011 May 18;31(20):7275-90. doi: 10.1523/JNEUROSCI.6476-10.2011.

Abstract

Oligomannosidic glycans play important roles in nervous system development and function. By performing a phage display screening with oligomannose-specific antibodies, we identified an oligomannose-mimicking peptide that was functionally active in modulating neurite outgrowth and neuron-astrocyte adhesion. Using the oligomannose-mimicking peptide in crosslinking experiments, synapsin I was identified as a novel oligomannose-binding protein in mouse brain. Further analyses not only verified that synapsin I is an oligomannose-binding lectin, but also indicated that it is a glycoprotein carrying oligomannose and Lewis(x). We also found that synapsin I is expressed in glia-enriched cultures and is released from glial cells via exosomes. Incubation of glial-derived exosomes in the presence of high KCl concentrations or subjecting glial cell cultures to either oxygen/glucose deprivation or hydrogen peroxide resulted in release of synapsin I from exosomes. Application of synapsin I promoted neurite outgrowth from hippocampal neurons and increased survival of cortical neurons upon hydrogen peroxide treatment or oxygen/glucose deprivation. Coculture experiments using wild-type hippocampal neurons and wild-type or synapsin-deficient glial cells showed enhanced neurite outgrowth when synapsin was expressed by glial cells. Synapsin-induced neurite outgrowth was dependent on oligomannose on synapsin I and the neural cell adhesion molecule NCAM at the neuronal cell surface. The data indicate that, under conditions of high neuronal activity and/or oxidative stress, synapsin can be released from glial-derived exosomes and promotes neurite outgrowth and neuronal survival by modulating the interactions between glia and neurons.

摘要

寡糖基聚糖在神经系统的发育和功能中发挥着重要作用。通过用寡甘露糖特异性抗体进行噬菌体展示筛选,我们鉴定出一种具有功能活性的寡甘露糖模拟肽,该肽可调节轴突生长和神经元-星形胶质细胞黏附。使用寡甘露糖模拟肽进行交联实验,鉴定出突触结合蛋白 I 是小鼠脑中的一种新的寡甘露糖结合蛋白。进一步的分析不仅验证了突触结合蛋白 I 是一种寡甘露糖结合凝集素,而且表明它是一种携带寡甘露糖和 Lewis(x)的糖蛋白。我们还发现突触结合蛋白 I 在富含胶质的培养物中表达,并通过外泌体从胶质细胞中释放。用高浓度 KCl 孵育源自胶质的外泌体,或使胶质细胞培养物经历氧/葡萄糖剥夺或过氧化氢处理,均可导致外泌体中的突触结合蛋白 I 释放。应用突触结合蛋白 I 可促进海马神经元的轴突生长,并增加皮质神经元在过氧化氢处理或氧/葡萄糖剥夺后的存活率。使用野生型海马神经元和野生型或突触结合蛋白缺失型胶质细胞进行共培养实验表明,当胶质细胞表达突触结合蛋白时,轴突生长增强。突触结合蛋白诱导的轴突生长依赖于突触结合蛋白 I 上的寡甘露糖和神经元细胞表面上的神经细胞黏附分子 NCAM。这些数据表明,在神经元活动和/或氧化应激增加的情况下,突触结合蛋白可以从胶质衍生的外泌体中释放出来,并通过调节胶质细胞和神经元之间的相互作用来促进轴突生长和神经元存活。

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