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Aβ42 fibril formation from predominantly oligomeric samples suggests a link between oligomer heterogeneity and fibril polymorphism

机译:主要由寡聚样品形成的Aβ42原纤维表明寡聚物异质性与原纤维多态性之间存在联系

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摘要

Amyloid-β (Aβ) oligomers play a central role in the pathogenesis of Alzheimer's disease. Oligomers of different sizes, morphology and structures have been reported in both in vivo and in vitro studies, but there is a general lack of understanding about where to place these oligomers in the overall process of Aβ aggregation and fibrillization. Here, we show that Aβ42 spontaneously forms oligomers with a wide range of sizes in the same sample. These Aβ42 samples contain predominantly oligomers, and they quickly form fibrils upon incubation at 37°C. When fractionated using ultrafiltration filters, the samples enriched with smaller oligomers form fibrils at a faster rate than the samples enriched with larger oligomers, with both a shorter lag time and faster fibril growth rate. This observation is independent of Aβ42 batches and hexafluoroisopropanol treatment. Furthermore, the fibrils formed by the samples enriched with larger oligomers are more readily solubilized by epigallocatechin gallate, a main catechin component of green tea. These results suggest that the fibrils formed by larger oligomers may adopt a different structure from fibrils formed by smaller oligomers, pointing to a link between oligomer heterogeneity and fibril polymorphism.
机译:淀粉样β(Aβ)低聚物在阿尔茨海默氏病的发病机理中起着核心作用。在体内和体外研究中都报道了不同大小,形态和结构的低聚物,但是对于在Aβ聚集和原纤维化的整个过程中将这些低聚物放置在何处普遍缺乏了解。在这里,我们显示Aβ42在同一样品中自发形成各种大小的寡聚物。这些Aβ42样品主要包含寡聚物,在37°C孵育后会迅速形成原纤维。当使用超滤过滤器进行分馏时,富集较小寡聚物的样品形成原纤维的速度比富集较大寡聚物的样品快,滞后时间较短,原纤维生长速度更快。该观察结果与Aβ42批次和六氟异丙醇处理无关。此外,由富含较大的低聚物的样品形成的原纤维更容易被表没食子儿茶素没食子酸酯(绿茶中的儿茶素的主要成分)溶解。这些结果表明,由较大的寡聚物形成的原纤维可能与由较小的寡聚物形成的原纤维采取不同的结构,这表明寡聚物异质性和原纤维多态性之间存在联系。

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