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Src在神经元细胞中与发动蛋白和突触蛋白相互作用。

Src interacts with dynamin and synapsin in neuronal cells.

作者信息

Foster-Barber A, Bishop J M

机构信息

G. W. Hooper Foundation, University of California, San Francisco, CA 94143-0552, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Apr 14;95(8):4673-7. doi: 10.1073/pnas.95.8.4673.

Abstract

The nonreceptor tyrosine kinase Src is expressed at a high level in cells that are specialized for regulated secretion, such as the neuron, and is concentrated on secretory vesicles or at the site of exocytosis. To investigate the possibility that Src may play a role in regulating membrane traffic, we searched for neuronal proteins that will interact with Src. The SH3 domain of Src, but not that of the splice variant N-Src, bound to three proteins from mouse synaptosomes or PC12 cells: dynamin, synapsin Ia, and synapsin Ib. Dynamin and the synapsins coprecipitated with Src from PC12 cell extracts, and they colocalized with a subset of Src in the PC12 cell by immunofluorescence. Neither dynamin nor the synapsins were phosphorylated by Src, suggesting that the interaction of these proteins serves to direct the kinase activity of Src toward other proteins in the vesicle population. In immunoprecipitates containing Src and dynamin, the clathrin adaptor protein alpha-adaptin was also found. The association of Src and synapsin suggests a role for Src in the life cycle of the synaptic vesicle. The identification of a complex containing Src, dynamin, and alpha-adaptin indicates that Src may play a more general role in membrane traffic as well.

摘要

非受体酪氨酸激酶Src在专门用于调节性分泌的细胞(如神经元)中高水平表达,并集中在分泌小泡或胞吐作用部位。为了研究Src可能在调节膜运输中发挥作用的可能性,我们寻找了能与Src相互作用的神经元蛋白。Src的SH3结构域,而非剪接变体N-Src的SH3结构域,与来自小鼠突触体或PC12细胞的三种蛋白结合:发动蛋白、突触结合蛋白Ia和突触结合蛋白Ib。发动蛋白和突触结合蛋白与PC12细胞提取物中的Src共沉淀,并且通过免疫荧光在PC12细胞中它们与一部分Src共定位。发动蛋白和突触结合蛋白都不会被Src磷酸化,这表明这些蛋白的相互作用有助于将Src的激酶活性导向小泡群体中的其他蛋白。在含有Src和发动蛋白的免疫沉淀物中,还发现了网格蛋白衔接蛋白α衔接蛋白。Src与突触结合蛋白的关联表明Src在突触小泡的生命周期中发挥作用。含有Src、发动蛋白和α衔接蛋白的复合物的鉴定表明,Src可能在膜运输中也发挥更普遍的作用。

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