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Localization and subcellular distribution of smg p25A, a ras p21-like GTP-binding protein, in rat brain.

作者信息

Mizoguchi A, Kim S, Ueda T, Kikuchi A, Yorifuji H, Hirokawa N, Takai Y

机构信息

Department of Anatomy and Biochemistry, Kobe University School of Medicine, Japan.

出版信息

J Biol Chem. 1990 Jul 15;265(20):11872-9.

PMID:2114404
Abstract

We have made a monoclonal antibody which specifically recognizes smg p25A among many ras p21/ras p21-like GTP-binding proteins thus far purified from bovine brain membranes. By use of this antibody, we have investigated the localization and subcellular distribution of smg p25A in rat brain by light and electron microscopic immunocytochemistry and by immunoblotting. By light microscopic immunocytochemistry, specific immunoreactivity is widely distributed, most abundant in neuropil, weak in neuronal somata, and absent from white matter. By electron microscopic immunocytochemistry, intense labeling is demonstrated on most of the synapses and concentrated in the presynaptic area where synaptic vesicles are observed. Presynaptic plasma membranes are weakly labeled but mitochondria, postsynaptic plasma membranes, and postsynaptic densities are unlabeled. In subcellular fractionation analysis of cerebrum, about one-fifth of smg p25A is found in the soluble cytosol fraction and the rest is found in the particulate fraction. About half of the particulate-bound smg p25A is recovered in the P2 fraction containing synaptosomes, mitochondria, and myelin, among which a major portion of smg p25A is recovered in the synaptosomal fraction. In the synaptosomal fraction, smg p25A is concentrated about 8-fold in the fraction containing synaptic vesicles and about 3-fold in the fraction containing synaptic plasma membranes compared with the original homogenate. smg p25A is present at a low level in the fraction containing synaptosomal soluble substances but almost absent from the fractions containing intrasynaptosomal mitochondria or post-synaptic densities. These results suggest that smg p25A plays important roles in the regulation of synaptic functions such as exo-endocytotic recycling of synaptic vesicles during neurotransmitter release.

摘要

相似文献

1
Localization and subcellular distribution of smg p25A, a ras p21-like GTP-binding protein, in rat brain.
J Biol Chem. 1990 Jul 15;265(20):11872-9.
2
Regulation of reversible binding of smg p25A, a ras p21-like GTP-binding protein, to synaptic plasma membranes and vesicles by its specific regulatory protein, GDP dissociation inhibitor.通过其特异性调节蛋白GDP解离抑制剂对类Ras p21 GTP结合蛋白smg p25A与突触质膜和囊泡的可逆结合进行调节。
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Purification and characterization from bovine brain cytosol of a protein that inhibits the dissociation of GDP from and the subsequent binding of GTP to smg p25A, a ras p21-like GTP-binding protein.从牛脑细胞质中纯化并鉴定一种蛋白质,该蛋白质可抑制GDP从类Ras p21的GTP结合蛋白smg p25A上解离以及随后GTP与smg p25A的结合。
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Purification and characterization from rat liver cytosol of a GDP dissociation inhibitor (GDI) for liver 24K G, a ras p21-like GTP-binding protein, with properties similar to those of smg p25A GDI.从大鼠肝脏胞质溶胶中纯化并鉴定一种用于肝脏24K G(一种类ras p21 GTP结合蛋白)的GDP解离抑制剂(GDI),其性质与smg p25A GDI相似。
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A small GTP-binding protein (G protein) recognized by smg p25A GDP dissociation inhibitor (GDI) in human platelet membranes and GDI for this small G protein in human platelet cytosol.一种小GTP结合蛋白(G蛋白),可被人血小板膜中的smg p25A GDP解离抑制剂(GDI)识别,以及人血小板胞质溶胶中该小G蛋白的GDI。
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