Sun Brian, Ding Tianben, Zhou Weiyan, Porter Tara S, Lew Matthew D
Department of Electrical and Systems Engineering, Washington University in St. Louis, St. Louis, MO, 63130.
bioRxiv. 2024 Mar 27:2024.03.24.586510. doi: 10.1101/2024.03.24.586510.
Amyloid-beta aggregates are characteristic signatures of Alzheimer's disease, but probing how their nanoscale architectures influence their growth and decay remains challenging using current technologies. Here, we apply time-lapse single-molecule orientation-localization microscopy (SMOLM) to measure the orientations and rotational "wobble" of Nile blue (NB) molecules transiently binding to fibrils. We quantify correlations between fibril architectures, measured by SMOLM, and their growth and decay visualized by single-molecule localization microscopy (SMLM). We discover that stable fibrils tend to be well-ordered, signified by well-aligned NB orientations and small wobble. SMOLM also shows that increasing order and disorder are signatures of growing and decaying fibrils, respectively. We also observe SMLM-invisible fibril remodeling, including steady growth and decay patterns that conserve -sheet organization. SMOLM reveals that increased heterogeneity in fibril architectures is correlated with more dynamic remodeling and that large-scale fibril remodeling tends to originate from local regions that exhibit strong heterogeneity.
淀粉样β蛋白聚集体是阿尔茨海默病的特征性标志,但利用现有技术探究其纳米级结构如何影响其生长和衰变仍然具有挑战性。在此,我们应用延时单分子取向定位显微镜(SMOLM)来测量尼罗蓝(NB)分子与原纤维瞬时结合的取向和旋转“摆动”。我们量化了通过SMOLM测量的原纤维结构与其通过单分子定位显微镜(SMLM)可视化的生长和衰变之间的相关性。我们发现稳定的原纤维往往排列有序,表现为NB取向良好对齐且摆动较小。SMOLM还表明,有序度增加和无序分别是生长中和衰变中原纤维的标志。我们还观察到SMLM不可见的原纤维重塑,包括保持β折叠结构的稳定生长和衰变模式。SMOLM揭示,原纤维结构中增加的异质性与更动态的重塑相关,并且大规模的原纤维重塑往往起源于表现出强烈异质性的局部区域。