Department of Clinical and Experimental Epilepsy, UCL Institute of Neurology, London, UK.
School of Physiology, Pharmacology, and Neuroscience, University of Bristol, Bristol, UK.
Cell Rep. 2017 Oct 3;21(1):97-109. doi: 10.1016/j.celrep.2017.09.004.
Mutations in the Golgi SNARE (SNAP [soluble NSF attachment protein] receptor) protein Membrin (encoded by the GOSR2 gene) cause progressive myoclonus epilepsy (PME). Membrin is a ubiquitous and essential protein mediating ER-to-Golgi membrane fusion. Thus, it is unclear how mutations in Membrin result in a disorder restricted to the nervous system. Here, we use a multi-layered strategy to elucidate the consequences of Membrin mutations from protein to neuron. We show that the pathogenic mutations cause partial reductions in SNARE-mediated membrane fusion. Importantly, these alterations were sufficient to profoundly impair dendritic growth in Drosophila models of GOSR2-PME. Furthermore, we show that Membrin mutations cause fragmentation of the presynaptic cytoskeleton coupled with transsynaptic instability and hyperactive neurotransmission. Our study highlights how dendritic growth is vulnerable even to subtle secretory pathway deficits, uncovers a role for Membrin in synaptic function, and provides a comprehensive explanatory basis for genotype-phenotype relationships in GOSR2-PME.
高尔基 SNARE(SNAP [可溶性 NSF 附着蛋白]受体)蛋白 Membrin(由 GOSR2 基因编码)中的突变导致进行性肌阵挛性癫痫(PME)。Membrin 是一种普遍存在且必不可少的蛋白,介导内质网到高尔基体的膜融合。因此,尚不清楚 Membrin 中的突变如何导致仅局限于神经系统的疾病。在这里,我们使用多层次策略从蛋白到神经元阐明 Membrin 突变的后果。我们表明,致病性突变导致 SNARE 介导的膜融合部分减少。重要的是,这些改变足以严重损害 GOSR2-PME 的果蝇模型中的树突生长。此外,我们表明 Membrin 突变导致突触前细胞骨架碎片化,伴有突触不稳定和神经递质过度活跃。我们的研究强调了即使是微妙的分泌途径缺陷也会使树突生长变得脆弱,揭示了 Membrin 在突触功能中的作用,并为 GOSR2-PME 中的基因型-表型关系提供了全面的解释基础。
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