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突触素作为主要的神经元钙/ S100A1相互作用蛋白。

Synapsins as major neuronal Ca2+/S100A1-interacting proteins.

作者信息

Heierhorst J, Mitchelhill K I, Mann R J, Tiganis T, Czernik A J, Greengard P, Kemp B E

机构信息

St. Vincent's Institute of Medical Research, 41 Victoria Parade, Fitzroy, VIC 3065, Australia.

出版信息

Biochem J. 1999 Dec 1;344 Pt 2(Pt 2):577-83.

Abstract

The mammalian S100A1 protein can activate the invertebrate myosin-associated giant protein kinase twitchin in a Ca(2+)-dependent manner by more than 1000-fold in vitro; however, no mammalian S100-dependent protein kinases are known. In an attempt to identify novel mammalian Ca(2+)/S100A1-regulated protein kinases, brain extracts were subjected to combined Ca(2+)-dependent affinity chromatography with S100A1 and an ATP analogue. This resulted in the purification to near-homogeneity of the four major synapsin isoforms Ia, Ib, IIa and IIb. All four synapsins were specifically affinity-labelled with the ATP analogue 5'-p-fluorosulphonylbenzoyladenosine. S100A1 bound to immobilized synapsin IIa in BIAcore experiments in a Ca(2+)-dependent and Zn(2+)-enhanced manner with submicromolar affinity; this interaction could be competed for with synthetic peptides of the proposed S100A1-binding sites of synapsin. Double-labelling confocal immunofluorescence microscopy demonstrated that synapsins and S100A1 are both present in the soma and neurites of PC12 cells, indicating their potential to interact in neurons in vivo.

摘要

哺乳动物的S100A1蛋白在体外可通过Ca(2+)依赖性方式将无脊椎动物的肌球蛋白相关巨蛋白激酶抽动蛋白激活1000多倍;然而,目前尚未发现依赖于哺乳动物S100的蛋白激酶。为了鉴定新型的哺乳动物Ca(2+)/S100A1调节的蛋白激酶,对脑提取物进行了S100A1和ATP类似物的联合Ca(2+)依赖性亲和层析。这使得四种主要的突触素同工型Ia、Ib、IIa和IIb纯化至接近均一性。所有四种突触素均被ATP类似物5'-对氟磺酰苯甲酰腺苷特异性亲和标记。在BIAcore实验中,S100A1以亚微摩尔亲和力通过Ca(2+)依赖性和Zn(2+)增强的方式与固定化的突触素IIa结合;这种相互作用可以被突触素的拟S100A1结合位点的合成肽竞争。双标记共聚焦免疫荧光显微镜显示,突触素和S100A1均存在于PC12细胞的胞体和神经突中,表明它们在体内神经元中具有相互作用的潜力。

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