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Neuronal Porosome-The Secretory Portal at the Nerve Terminal: It’s Structure-Function Composition and Reconstitution

机译:神经元孔隙-神经终末的分泌门户:它的结构功能组成和重构

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摘要

Cup-shaped secretory portals at the cell plasma membrane called porosomes mediate secretion from cells. Membrane bound secretory vesicles transiently dock and fuse at the cytosolic compartment of the porosome base to expel intravesicular contents to the outside during cell secretion. In the past decade, the structure, isolation, composition, and functional reconstitution of the neuronal porosome complex has been accomplished providing a molecular understanding of its structure-function. Neuronal porosomes are 15 nm cup-shaped lipoprotein structures composed of nearly 40 proteins. Being a membrane-associated supramolecular complex has precluded determination of the atomic structure of the porosome. However recent studies using small-angle X-ray solution scattering (SAXS), provide at sub-nanometer resolution, the native 3D structure of the neuronal porosome complex associated with docked synaptic vesicle at the nerve terminal. Additionally, results from the SAXS study and earlier studies using atomic force microscopy, provide the possible molecular mechanism involved in porosome-mediated neurotransmitter release at the nerve terminal.
机译:在细胞质膜上的杯状分泌门户称为小体,介导细胞分泌。膜结合的分泌囊泡暂时停泊并融合在多孔体碱基的胞质区室中,从而在细胞分泌过程中将囊泡内的物质排出体外。在过去的十年中,神经元孔隙体复合物的结构,分离,组成和功能重构已经完成,提供了对其结构功能的分子理解。神经元孔小体是由近40种蛋白质组成的15 nm杯状脂蛋白结构。由于是膜相关的超分子复合物,因此无法确定孔隙体的原子结构。但是,最近使用小角度X射线溶液散射(SAXS)进行的研究以亚纳米分辨率提供了与神经末梢停靠的突触小囊相关的神经元孔隙体复合物的天然3D结构。此外,来自SAXS研究和使用原子力显微镜的早期研究的结果提供了可能的分子机制,涉及在神经末梢由孔隙体介导的神经递质释放。

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