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Munc18-1与神经元SNARE复合体的结合控制突触小泡的启动。

Munc18-1 binding to the neuronal SNARE complex controls synaptic vesicle priming.

作者信息

Deák Ferenc, Xu Yi, Chang Wen-Pin, Dulubova Irina, Khvotchev Mikhail, Liu Xinran, Südhof Thomas C, Rizo Josep

机构信息

Howard Hughes Medical Institute, Department of Neuroscience, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

J Cell Biol. 2009 Mar 9;184(5):751-64. doi: 10.1083/jcb.200812026. Epub 2009 Mar 2.

Abstract

Munc18-1 and soluble NSF attachment protein receptors (SNAREs) are critical for synaptic vesicle fusion. Munc18-1 binds to the SNARE syntaxin-1 folded into a closed conformation and to SNARE complexes containing open syntaxin-1. Understanding which steps in fusion depend on the latter interaction and whether Munc18-1 competes with other factors such as complexins for SNARE complex binding is critical to elucidate the mechanisms involved. In this study, we show that lentiviral expression of Munc18-1 rescues abrogation of release in Munc18-1 knockout mice. We describe point mutations in Munc18-1 that preserve tight binding to closed syntaxin-1 but markedly disrupt Munc18-1 binding to SNARE complexes containing open syntaxin-1. Lentiviral rescue experiments reveal that such disruption selectively impairs synaptic vesicle priming but not Ca(2+)-triggered fusion of primed vesicles. We also find that Munc18-1 and complexin-1 bind simultaneously to SNARE complexes. These results suggest that Munc18-1 binding to SNARE complexes mediates synaptic vesicle priming and that the resulting primed state involves a Munc18-1-SNARE-complexin macromolecular assembly that is poised for Ca(2+) triggering of fusion.

摘要

Munc18-1和可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体(SNAREs)对于突触小泡融合至关重要。Munc18-1与折叠成闭合构象的SNARE syntaxin-1以及含有开放syntaxin-1的SNARE复合体结合。了解融合过程中的哪些步骤依赖于后一种相互作用,以及Munc18-1是否与其他因子(如复合体蛋白)竞争SNARE复合体结合,对于阐明其中涉及的机制至关重要。在本研究中,我们表明慢病毒表达的Munc18-1可挽救Munc18-1基因敲除小鼠中释放的缺失。我们描述了Munc18-1中的点突变,这些突变保留了与闭合syntaxin-1的紧密结合,但显著破坏了Munc18-1与含有开放syntaxin-1的SNARE复合体的结合。慢病毒挽救实验表明,这种破坏选择性地损害突触小泡的启动,但不影响Ca(2+)触发的已启动小泡的融合。我们还发现Munc18-1和复合体蛋白-1同时与SNARE复合体结合。这些结果表明,Munc18-1与SNARE复合体的结合介导了突触小泡的启动,并且由此产生的启动状态涉及一个Munc18-1-SNARE-复合体蛋白大分子组装体,该组装体为Ca(2+)触发融合做好了准备。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4865/2686405/21f676a1e541/JCB_200812026_RGB_Fig1.jpg

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