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胞吐过程中 syntaxin 的构象转换:munc18 的作用

A conformational switch in syntaxin during exocytosis: role of munc18.

作者信息

Dulubova I, Sugita S, Hill S, Hosaka M, Fernandez I, Südhof T C, Rizo J

机构信息

Department of Biochemistry, University of Texas Southwestern Medical Center, 5323 Harry Hines Boulevard, Dallas, TX 75235, USA.

出版信息

EMBO J. 1999 Aug 16;18(16):4372-82. doi: 10.1093/emboj/18.16.4372.

Abstract

Syntaxin 1, an essential protein in synaptic membrane fusion, contains a helical autonomously folded N-terminal domain, a C-terminal SNARE motif and a transmembrane region. The SNARE motif binds to synaptobrevin and SNAP-25 to assemble the core complex, whereas almost the entire cytoplasmic sequence participates in a complex with munc18-1, a neuronal Sec1 homolog. We now demonstrate by NMR spectroscopy that, in isolation, syntaxin adopts a 'closed' conformation. This default conformation of syntaxin is incompatible with core complex assembly which requires an 'open' syntaxin conformation. Using site-directed mutagenesis, we find that disruption of the closed conformation abolishes the ability of syntaxin to bind to munc18-1 and to inhibit secretion in PC12 cells. These results indicate that syntaxin binds to munc18-1 in a closed conformation and suggest that this conformation represents an essential intermediate in exocytosis. Our data suggest a model whereby, during exocytosis, syntaxin undergoes a large conformational switch that mediates the transition between the syntaxin-munc18-1 complex and the core complex.

摘要

Syntaxin 1是突触膜融合中的一种必需蛋白质,它包含一个螺旋状自主折叠的N端结构域、一个C端SNARE基序和一个跨膜区域。SNARE基序与突触小泡蛋白和SNAP - 25结合以组装核心复合体,而几乎整个胞质序列都参与与munc18 - 1(一种神经元Sec1同源物)形成的复合体。我们现在通过核磁共振光谱证明,单独存在时,Syntaxin呈现“闭合”构象。Syntaxin的这种默认构象与需要“开放”Syntaxin构象的核心复合体组装不相容。使用定点诱变,我们发现破坏闭合构象会消除Syntaxin与munc18 - 1结合以及抑制PC12细胞分泌的能力。这些结果表明Syntaxin以闭合构象与munc18 - 1结合,并表明这种构象代表胞吐作用中的一个必需中间体。我们的数据提出了一个模型,据此在胞吐作用过程中,Syntaxin经历一个大的构象转换,介导Syntaxin - munc18 - 1复合体和核心复合体之间的转变。

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