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Localization microscopy for the study of amyloid fibril formation

机译:用于研究淀粉样蛋白原纤维形成的定位显微镜

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Super-resolution microscopy has emerged as a powerful and non-invasive tool for the study of molecular processes both in vitro, but also as they occur in live cells. Here we present the application of direct stochastic optical reconstruction microscopy (dSTORM), a super-resolution technique based on single molecule localization, to determine the morphology of protein aggregates and of small extra- and intracellular structures. The technique reveals details down to 20 nm providing information on scales much smaller than the wavelength of the probing light. We use dSTORM in the study of amyloid fibril self-assembly processes associated with neurodegenerative diseases, such as Alzheimer's and Parkinson's diseases. We show that the aggregation process can be followed kinetically and observe the emergence of amyloid structures in time as they occur in vitro. As an all optical technique, there is translation potential from studies in vitro to in vivo applications.
机译:超分辨率显微镜已经成为在体外研究分子过程的强大和非侵入性工具,但也可以在活细胞中发生。 在这里,我们介绍了直接随机光学重建显微镜(Dstorm),一种基于单分子定位的超分辨率技术,确定蛋白质聚集体和小型细胞内结构的形态。 该技术将细节揭示到20nm,提供关于小于探测光的波长的刻度的信息。 我们在研究与神经变性疾病相关的淀粉样蛋白原纤维自组装方法的研究中使用Dstorm,例如阿尔茨海默氏症和帕金森的疾病。 我们表明,可以遵循汇总过程,并在体外发生时及时观察淀粉样蛋白结构的出现。 作为所有光学技术,存在在体外应用中的研究中的翻译潜力。

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