Transport at Nanoscale Interfaces Laboratory, Swiss Federal Laboratories for Materials Science and Technology, Dübendorf, CH-8600, Switzerland.
Department of Physics, Bernal Institute, University of Limerick, Limerick V94T9PX, Ireland.
Sci Adv. 2024 Oct 25;10(43):eadp5059. doi: 10.1126/sciadv.adp5059.
Protein fibril surfaces tend to generate toxic oligomers catalytically. To date, efforts to study the accelerated aggregation steps involved with Alzheimer's disease-linked amyloid-β (Aβ)-42 proteins on fibril surfaces have mainly relied on fluorophore-based analytics. Here, we visualize rare secondary nucleation events on the surface of Aβ-42 fibrils from embryonic to endpoint stages using liquid-based atomic force microscopy. Nanoscale imaging supported by atomic-scale molecular simulations tracked the adsorption and proliferation of oligomeric assemblies at nonperiodically spaced catalytic sites on the fibril surface. Upon confirming that fibril edges are preferential binding sites for oligomers during embryonic stages, the secondary fibrillar size changes were quantified during the growth stages. Notably, a small population of fibrils that displayed higher surface catalytic activity was identified as superspreaders. Profiling secondary fibrils during endpoint stages revealed a nearly threefold increase in their surface corrugation, a parameter we exploit to classify fibril subpopulations.
蛋白原纤维表面往往具有催化生成毒性寡聚物的特性。迄今为止,研究与阿尔茨海默病相关的淀粉样蛋白-β(Aβ)-42 蛋白在原纤维表面上加速聚集步骤的工作主要依赖于基于荧光团的分析方法。在这里,我们使用基于液体的原子力显微镜,可视化了从胚胎期到终点阶段 Aβ-42 原纤维表面上罕见的二次成核事件。原子尺度分子模拟支持的纳米级成像,跟踪了寡聚体组装在原纤维表面非周期性间隔催化位点上的吸附和增殖。在确认原纤维边缘是寡聚体在胚胎期的优先结合位点后,在生长阶段定量了二级原纤维的大小变化。值得注意的是,鉴定出一小部分具有更高表面催化活性的原纤维作为超级传播者。在终点阶段对二级原纤维进行分析,发现其表面波纹度增加了近三倍,我们利用这一参数对原纤维亚群进行分类。
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