首页> 外文期刊>The European physical journal, E. Soft matter >Synaptic vesicles studied by dynamic light scattering.
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Synaptic vesicles studied by dynamic light scattering.

机译:通过动态光散射研究突触小泡。

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摘要

The size polydispersity distribution of synaptic vesicles (SVs) is characterized under quasi-physiological conditions by dynamic light scattering (DLS). Highly purified fractions of SVs obtained from rat brain still contain a small amount of larger contaminant structures, which can be quantified by DLS and further reduced by asymmetric-flow field-flow (AFFF) fractionation. The intensity autocorrelation functions g (2)(τ) recorded from these samples are analyzed by a constrained regularization method as well as by an alternative direct modeling approach. The results are in quantitative agreement with the polydispersity obtained from cryogenic electron microscopy of vitrified SVs. Next, different vesicle fusion assays based on samples composed of SVs and small unilamellar proteoliposomes with the fusion proteins syntaxin 1 and SNAP-25A are characterized by DLS. The size increase of the proteoliposomes due to SNARE-dependent fusion with SVs is quantified by DLS under quasi-physiological conditions.
机译:突触小泡(SVs)的大小多分散性分布在准生理条件下通过动态光散射(DLS)进行表征。从大鼠脑中获得的高度纯化的SV馏分仍包含少量较大的污染物结构,可以通过DLS进行定量,并通过不对称流场流(AFFF)分级进一步降低。从这些样本记录的强度自相关函数g(2)(τ)通过约束正则化方法以及其他直接建模方法进行分析。结果与从玻璃化SV的低温电子显微镜获得的多分散度定量一致。接下来,通过DLS表征基于由SV和具有融合蛋白syntaxin 1和SNAP-25A的小的单层蛋白脂质体组成的样品的不同囊泡融合测定。在准生理条件下,通过DLS量化了由于SNARE依赖性与SVs融合而引起的蛋白脂质体的大小增加。

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