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Screening and classifying small molecule inhibitors of amyloid formation using ion mobility spectrometry-mass spectrometry

机译:使用离子淌度质谱-质谱法对淀粉样蛋白形成的小分子抑制剂进行筛选和分类

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摘要

The search for therapeutic agents which bind specifically to precursor protein conformations and inhibit amyloid assembly is an important challenge. Identifying such inhibitors is difficult since many protein precursors of aggregation are partially folded or intrinsically disordered, ruling out structure-based design. Furthermore, inhibitors can act by a variety of mechanisms, including specific or non-specific binding, as well as colloidal inhibition. Here we report a high throughput method based on ion mobility spectrometry-mass spectrometry (IMS-MS) that is capable of rapidly detecting small molecules that bind to amyloid precursors, identifying the interacting protein species, and defining the mode of inhibition. Using this method we have classified a variety of small molecules that are potential inhibitors of human islet amyloid polypeptide (hIAPP) aggregation or amyloid-beta 1-40 (Aβ40) aggregation as either specific, non-specific, colloidal or non-interacting. We also demonstrate the ability of IMS-MS to screen for inhibitory small molecules in a 96-well plate format and use this to discover a new inhibitor of hIAPP amyloid assembly.
机译:寻找与前体蛋白构象特异性结合并抑制淀粉样蛋白组装的治疗剂是一项重要的挑战。由于许多聚集的蛋白质前体被部分折叠或固有地无序,因此难以鉴定此类抑制剂,从而排除了基于结构的设计。此外,抑制剂可以通过多种机制起作用,包括特异性或非特异性结合以及胶体抑制。在这里,我们报告基于离子淌度质谱-质谱(IMS-MS)的高通量方法,该方法能够快速检测与淀粉样蛋白前体结合的小分子,识别相互作用的蛋白质种类,并定义抑制方式。使用这种方法,我们已将各种小分子分类为特异性,非特异性,胶体性或非相互作用性,这些小分子是人类胰岛淀粉样多肽(hIAPP)聚集或淀粉样β1-40(Aβ40)聚集的潜在抑制剂。我们还展示了IMS-MS筛选96孔板格式的抑制性小分子的能力,并使用它来发现hIAPP淀粉样蛋白组装的新抑制剂。

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