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Botulinum neurotoxin type-A enters a non-recycling pool of synaptic vesicles

机译:肉毒杆菌神经毒素类型-A进入非再循环突触囊泡池

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摘要

Neuronal communication relies on synaptic vesicles undergoing regulated exocytosis and recycling for multiple rounds of fusion. Whether all synaptic vesicles have identical protein content has been challenged, suggesting that their recycling ability may differ greatly. Botulinum neurotoxin type-A (BoNT/A) is a highly potent neurotoxin that is internalized in synaptic vesicles at motor nerve terminals and induces flaccid paralysis. Recently, BoNT/A was also shown to undergo retrograde transport, suggesting it might enter a specific pool of synaptic vesicles with a retrograde trafficking fate. Using high-resolution microscopy techniques including electron microscopy and single molecule imaging, we found that the BoNT/A binding domain is internalized within a subset of vesicles that only partially co-localize with cholera toxin B-subunit and have markedly reduced VAMP2 immunoreactivity. Synaptic vesicles loaded with pHrodo-BoNT/A-Hc exhibited a significantly reduced ability to fuse with the plasma membrane in mouse hippocampal nerve terminals when compared with pHrodo-dextran-containing synaptic vesicles and pHrodo-labeled anti-GFP nanobodies bound to VAMP2-pHluorin or vGlut-pHluorin. Similar results were also obtained at the amphibian neuromuscular junction. These results reveal that BoNT/A is internalized in a subpopulation of synaptic vesicles that are not destined to recycle, highlighting the existence of significant molecular and functional heterogeneity between synaptic vesicles.
机译:神经元通信依赖于经历受管制卵尿的突触囊泡和回收多轮融合的回收。所有突触囊泡是否具有相同的蛋白质含量受到挑战,表明它们的回收能力可能会很大。肉毒杆菌神经毒素型-a(BONT / A)是一种高效的神经毒素,其在电动神经末端的突触囊泡中内化,并诱导弛缓性瘫痪。最近,ONT / A也显示出逆行运输,建议它可能进入具有逆行贩运命运的特定突触囊泡。使用包括电子显微镜和单分子成像的高分辨率显微镜技术,我们发现Bont / A结合结构域内化在囊泡的子集中,其仅与霍乱毒素B-亚基部分共定位并且具有显着降低的Vamp2免疫反应性。与Phrodo-Dextran的突触囊泡和Bumodo标记的抗GFP纳米菌相比,与Phrodo-Bont / A-Hc负载的突出能力显着降低了在小鼠海马神经末端中的血浆膜和与Vamp2-荧光素结合的前葡聚糖的抗GFP纳米髓质植物或vglut-嘌呤素。在两栖动物神经肌肉结处也得到了类似的结果。这些结果表明,突触囊泡的亚级内化的突触囊泡的亚化群体内化,突出了突触囊泡之间的显着分子和功能异质性的存在。

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