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. 2018 Jun 26;12(6):5408-5416.
doi: 10.1021/acsnano.8b00448. Epub 2018 May 22.

Rapid Growth of Acetylated Aβ(16-20) into Macroscopic Crystals

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Rapid Growth of Acetylated Aβ(16-20) into Macroscopic Crystals

Christian Bortolini et al. ACS Nano. .

Abstract

Aberrant assembly of the amyloid-β (Aβ) is responsible for the development of Alzheimer's disease, but can also be exploited to obtain highly functional biomaterials. The short Aβ fragment, KLVFF (Aβ16-20), is crucial for Aβ assembly and considered to be an Aβ aggregation inhibitor. Here, we show that acetylation of KLVFF turns it into an extremely fast self-assembling molecule, reaching macroscopic ( i.e., mm) size in seconds. We show that KLVFF is metastable and that the self-assembly can be directed toward a crystalline or fibrillar phase simply through chemical modification, via acetylation or amidation of the peptide. Amidated KLVFF can form amyloid fibrils; we observed folding events of such fibrils occurring in as little as 60 ms. The ability of single KLVFF molecules to rapidly assemble as highly ordered macroscopic structures makes it a promising candidate for applications as a rapid-forming templating material.

Keywords: amyloid crystals; atomic force microscopy; biomaterials; circular dichroism; protein misfolding; self-assembly; stopped-flow.

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