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CAPS(Ca2+-依赖性分泌激活蛋白)与三种神经元 SNARE 蛋白的新型相互作用,这些蛋白对于囊泡融合是必需的。

Novel interactions of CAPS (Ca2+-dependent activator protein for secretion) with the three neuronal SNARE proteins required for vesicle fusion.

机构信息

Department of Biochemistry, University of Wisconsin-Madison, Madison, Wisconsin 53706, USA.

出版信息

J Biol Chem. 2010 Nov 12;285(46):35320-9. doi: 10.1074/jbc.M110.145169. Epub 2010 Sep 8.

Abstract

CAPS (aka CADPS) is required for optimal vesicle exocytosis in neurons and endocrine cells where it functions to prime the exocytic machinery for Ca(2+)-triggered fusion. Fusion is mediated by trans complexes of the SNARE proteins VAMP-2, syntaxin-1, and SNAP-25 that bridge vesicle and plasma membrane. CAPS promotes SNARE complex formation on liposomes, but the SNARE binding properties of CAPS are unknown. The current work revealed that CAPS exhibits high affinity binding to syntaxin-1 and SNAP-25 and moderate affinity binding to VAMP-2. CAPS binding is specific for a subset of exocytic SNARE protein isoforms and requires membrane integration of the SNARE proteins. SNARE protein binding by CAPS is novel and mediated by interactions with the SNARE motifs in the three proteins. The C-terminal site for CAPS binding on syntaxin-1 does not overlap the Munc18-1 binding site and both proteins can co-reside on membrane-integrated syntaxin-1. As expected for a C-terminal binding site on syntaxin-1, CAPS stimulates SNARE-dependent liposome fusion with N-terminal truncated syntaxin-1 but exhibits impaired activity with C-terminal syntaxin-1 mutants. Overall the results suggest that SNARE complex formation promoted by CAPS may be mediated by direct interactions of CAPS with each of the three SNARE proteins required for vesicle exocytosis.

摘要

CAPS(也称为 CADPS)是神经元和内分泌细胞中囊泡胞吐作用所必需的,它的功能是为 Ca(2+)触发的融合作用准备出胞机制。融合作用是由 VAMP-2、突触融合蛋白-1 和 SNAP-25 的 SNARE 蛋白的跨膜复合物介导的,该复合物连接囊泡和质膜。CAPS 促进了脂质体上 SNARE 复合物的形成,但 CAPS 的 SNARE 结合特性是未知的。目前的工作揭示了 CAPS 对突触融合蛋白-1 和 SNAP-25 具有高亲和力结合,对 VAMP-2 具有中等亲和力结合。CAPS 结合是特异性的,仅针对一组特定的出胞 SNARE 蛋白同工型,并且需要 SNARE 蛋白的膜整合。CAPS 通过与三种蛋白中的 SNARE 基序相互作用,结合 SNARE 蛋白,这是一种新的机制。CAPS 结合突触融合蛋白-1 的 C 端结合位点与 Munc18-1 结合位点不重叠,并且两种蛋白都可以共同存在于膜整合的突触融合蛋白-1 上。如预期的那样,CAPS 是突触融合蛋白-1 的 C 端结合位点,刺激 SNARE 依赖性脂质体融合,使用 N 端截断的突触融合蛋白-1,但与 C 端突触融合蛋白-1 突变体的活性受损。总体而言,这些结果表明,CAPS 促进的 SNARE 复合物形成可能是通过 CAPS 与囊泡出胞作用所需的三种 SNARE 蛋白中的每一种的直接相互作用介导的。

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