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神经组织中的网格蛋白包被小泡主要参与突触小泡的循环利用。

Clathrin-coated vesicles in nervous tissue are involved primarily in synaptic vesicle recycling.

作者信息

Maycox P R, Link E, Reetz A, Morris S A, Jahn R

机构信息

Abteilung Neurochemie, Max-Planck-Institut für Psychiatrie, Martinsried, Germany.

出版信息

J Cell Biol. 1992 Sep;118(6):1379-88. doi: 10.1083/jcb.118.6.1379.

Abstract

The recycling of synaptic vesicles in nerve terminals is thought to involve clathrin-coated vesicles. However, the properties of nerve terminal coated vesicles have not been characterized. Starting from a preparation of purified nerve terminals obtained from rat brain, we isolated clathrin-coated vesicles by a series of differential and density gradient centrifugation steps. The enrichment of coated vesicles during fractionation was monitored by EM. The final fraction consisted of greater than 90% of coated vesicles, with only negligible contamination by synaptic vesicles. Control experiments revealed that the contribution by coated vesicles derived from the axo-dendritic region or from nonneuronal cells is minimal. The membrane composition of nerve terminal-derived coated vesicles was very similar to that of synaptic vesicles, containing the membrane proteins synaptophysin, synaptotagmin, p29, synaptobrevin and the 116-kD subunit of the vacuolar proton pump, in similar stoichiometric ratios. The small GTP-binding protein rab3A was absent, probably reflecting its dissociation from synaptic vesicles during endocytosis. Immunogold EM revealed that virtually all coated vesicles carried synaptic vesicle proteins, demonstrating that the contribution by coated vesicles derived from other membrane traffic pathways is negligible. Coated vesicles isolated from the whole brain exhibited a similar composition, most of them carrying synaptic vesicle proteins. This indicates that in nervous tissue, coated vesicles function predominantly in the synaptic vesicle pathway. Nerve terminal-derived coated vesicles contained AP-2 adaptor complexes, which is in agreement with their plasmalemmal origin. Furthermore, the neuron-specific coat proteins AP 180 and auxilin, as well as the alpha a1 and alpha c1-adaptins, were enriched in this fraction, suggesting a function for these coat proteins in synaptic vesicle recycling.

摘要

神经末梢中突触小泡的循环被认为涉及网格蛋白包被小泡。然而,神经末梢包被小泡的特性尚未得到表征。我们从大鼠脑获得的纯化神经末梢制剂开始,通过一系列差速离心和密度梯度离心步骤分离出网格蛋白包被小泡。通过电子显微镜监测分级分离过程中包被小泡的富集情况。最终级分中包被小泡的含量超过90%,突触小泡的污染可忽略不计。对照实验表明,源自轴突-树突区域或非神经元细胞的包被小泡的贡献极小。神经末梢来源的包被小泡的膜组成与突触小泡非常相似,含有膜蛋白突触素、突触结合蛋白、p29、突触小泡蛋白和液泡质子泵的116-kD亚基,其化学计量比相似。小GTP结合蛋白rab3A不存在,这可能反映了其在内吞过程中从突触小泡上解离。免疫金电子显微镜显示,几乎所有包被小泡都携带突触小泡蛋白,这表明源自其他膜运输途径的包被小泡的贡献可忽略不计。从全脑分离的包被小泡表现出相似的组成,其中大多数携带突触小泡蛋白。这表明在神经组织中,包被小泡主要在突触小泡途径中发挥作用。神经末梢来源的包被小泡含有AP-2衔接复合物,这与其质膜起源一致。此外,神经元特异性包被蛋白AP 180和辅助蛋白,以及α a1和α c1衔接蛋白,在该级分中富集,表明这些包被蛋白在突触小泡循环中发挥作用。

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