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本文引用的文献

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Differential effects of SNAP-25 deletion on Ca2+ -dependent and Ca2+ -independent neurotransmission.SNAP-25缺失对钙依赖性和非钙依赖性神经传递的不同影响。
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Synaptic vesicles recycling spontaneously and during activity belong to the same vesicle pool.突触小泡在自发状态下以及活动期间的循环属于同一个小泡池。
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Expression and function of SNAP-25 as a universal SNARE component in GABAergic neurons.SNAP-25作为γ-氨基丁酸能神经元中一种通用的可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体组分的表达及功能
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Structural determinants of synaptobrevin 2 function in synaptic vesicle fusion.突触小泡融合中突触结合蛋白2功能的结构决定因素。
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A role for synaptotagmin VII-regulated exocytosis of lysosomes in neurite outgrowth from primary sympathetic neurons.突触结合蛋白VII调节的溶酶体胞吐作用在原代交感神经元轴突生长中的作用。
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Autonomous function of synaptotagmin 1 in triggering synchronous release independent of asynchronous release.突触结合蛋白1在触发同步释放中独立于异步释放的自主功能。
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Alternative splicing of SNAP-25 regulates secretion through nonconservative substitutions in the SNARE domain.SNAP-25的可变剪接通过SNARE结构域中的非保守替换调节分泌。
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SNAP-25同源物支持神经元功能的差异能力。

Differential abilities of SNAP-25 homologs to support neuronal function.

作者信息

Delgado-Martínez Ignacio, Nehring Ralf B, Sørensen Jakob B

机构信息

Department of Membrane Biophysics, Max Planck Institute for Biophysical Chemistry, D-37077 Göttingen, Germany.

出版信息

J Neurosci. 2007 Aug 29;27(35):9380-91. doi: 10.1523/JNEUROSCI.5092-06.2007.

DOI:10.1523/JNEUROSCI.5092-06.2007
PMID:17728451
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6673127/
Abstract

The SNAP receptor (SNARE) complex, consisting of synaptosome-associated protein of 25 kDa (SNAP-25), synaptobrevin-2, and syntaxin-1, is involved in synaptic vesicles exocytosis. In addition, SNAP-25 has been implicated in constitutive exocytosis processes required for neurite outgrowth. However, at least three isoforms of SNAP-25 have been reported from neurons: SNAP-23, which is also present in non-neuronal cells, and the two alternative splice variants SNAP-25a and SNAP-25b. Here, we studied the differential ability of these isoforms to support the functions previously broadly ascribed to "SNAP-25." We studied the rescue of snap-25 null neurons in culture with different SNAP-25 homologs. We find that deletion of SNAP-25 leads to strongly reduced neuron survival, and, in the few surviving cells, impaired arborization, reduced spontaneous release, and complete arrest of evoked release. Lentiviral expression of SNAP-25a, SNAP-25b, or SNAP-23 rescued neuronal survival, arborization, amplitude, and frequency of spontaneous events. Also evoked release was rescued by all isoforms, but synchronous release required SNAP-25a/b in both glutamatergic and GABAergic neurons. SNAP-23 supported asynchronous release only, reminiscent of synaptotagmin-1 null neurons. SNAP-25b was superior to SNAP-25a in vesicle priming, resembling the shift to larger releasable vesicle pools that accompanies synaptic maturation. These data demonstrate a differential ability of SNAP-25b, SNAP-25a, and SNAP-23 to support neuronal function.

摘要

由25 kDa的突触体相关蛋白(SNAP-25)、突触小泡蛋白-2和 syntaxin-1组成的可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体(SNARE)复合体参与突触小泡的胞吐作用。此外,SNAP-25还与神经突生长所需的组成型胞吐过程有关。然而,从神经元中已报道至少有三种SNAP-25的亚型:SNAP-23,其也存在于非神经元细胞中,以及两种选择性剪接变体SNAP-25a和SNAP-25b。在这里,我们研究了这些亚型支持先前广泛归因于“SNAP-25”的功能的不同能力。我们用不同的SNAP-25同源物研究了培养的snap-25基因敲除神经元的拯救情况。我们发现,SNAP-25的缺失导致神经元存活率大幅降低,并且在少数存活细胞中,树突化受损、自发释放减少以及诱发释放完全停止。SNAP-25a、SNAP-25b或SNAP-23的慢病毒表达挽救了神经元的存活、树突化、自发事件的幅度和频率。所有亚型也都挽救了诱发释放,但在谷氨酸能和γ-氨基丁酸能神经元中,同步释放需要SNAP-25a/b。SNAP-23仅支持异步释放,这与突触结合蛋白-1基因敲除神经元相似。在囊泡启动方面,SNAP-25b优于SNAP-25a,类似于伴随突触成熟向更大的可释放囊泡池的转变。这些数据证明了SNAP-25b、SNAP-25a和SNAP-23在支持神经元功能方面的不同能力。