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Identification of distinct physiochemical properties of the toxic prefibrillar species formed by Aβ peptide variants

机译:鉴定由Aβ肽变体形成的有毒原纤维物种的独特理化特性

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摘要

The formation of amyloid-β peptide (Aβ) aggregates at an early stage during the self-assembly process is an important factor in the development of Alzheimer’s disease. The toxic effect is believed to be exerted by prefibrillar species of Aβ. It is therefore important to identify which prefibrillar species are toxic and characterize their distinct properties. In the present study, we investigated the in vitro aggregation behavior of Aβ-derived peptides possessing different levels of neurotoxic activity, using fluorescence spectroscopy in combination with transmission electron microscopy. The toxicity of various Aβ aggregates was assessed by using cultures of human neuroblastoma cells. Through combined use of the fluorescence probe 8-anilino-1-napthalenesulfonate (ANS) and the novel luminescent probe pentamer formyl thiophene acetic acid (p-FTAA), we were able to identify those Aβ peptide-derived prefibrillar species which exhibited cellular toxicity. In particular, species, which formed early during the aggregation process and showed strong p-FTAA and ANS fluorescence, were the species that possessed toxic activities. Moreover, by manipulating the aggregation conditions, it was possible to change the capacity of the Aβ peptide to form nontoxic versus toxic species.
机译:在自组装过程的早期阶段,淀粉样β肽(Aβ)聚集的形成是阿尔茨海默氏病发展的重要因素。据信该毒性作用是由Aβ的原纤维种类产生的。因此,重要的是要确定哪些原纤维种是有毒的,并表征其独特的性能。在本研究中,我们使用荧光光谱结合透射电子显微镜研究了具有不同水平神经毒性活性的Aβ衍生肽的体外聚集行为。通过使用人类神经母细胞瘤细胞培养物评估了各种Aβ聚集体的毒性。通过结合使用荧光探针8-苯胺基-1-萘磺酸盐(ANS)和新型发光探针五聚体甲酰基噻吩乙酸(p-FTAA),我们能够鉴定出那些表现出细胞毒性的Aβ肽来源的原纤维。特别地,具有聚集活性的物种在聚集过程的早期形成并显示出强的p-FTAA和ANS荧光。此外,通过控制聚集条件,可以改变Aβ肽形成无毒和有毒物种的能力。

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