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The Formation Mechanism of Segmented Ring-Shaped A beta Oligomers and Protofibrils

Authors
Choi, HyunsungLee, WonseokLee, GyudoYoon, Dae SungNa, Sungsoo
Issue Date
8월-2019
Publisher
AMER CHEMICAL SOC
Keywords
beta-amyloid; p3 peptide; molecular dynamics; atomic force microscopy; segmented ring-shaped structure
Citation
ACS CHEMICAL NEUROSCIENCE, v.10, no.8, pp.3830 - 3838
Indexed
SCIE
SCOPUS
Journal Title
ACS CHEMICAL NEUROSCIENCE
Volume
10
Number
8
Start Page
3830
End Page
3838
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/64014
DOI
10.1021/acschemneuro.9b00324
ISSN
1948-7193
Abstract
A clear understanding of amyloid formation with diverse morphologies is critical to overcoming the fatal disease amyloidosis. Studies have revealed that monomer concentration is a crucial factor for determining amyloid morphologies, such as protofibrils, annular, or spherical oligomers. However, gaining a complete understanding of the mechanism of formation of the various amyloid morphologies has been limited by the lack of experimental devices and insufficient knowledge. In this study, we demonstrate that the monomer concentration is an essential factor in determining the morphology of beta-amyloid (A beta) oligomers or protofibrils. By computational and experimental approaches, we investigated the strategies for structural stabilization of amyloid protein, the morphological changes, and amyloid aggregation. In particular, we found unprecedented conformations, e.g., single bent oligomers and segmented ring-shaped protofibrils, the formation of which was explained by the computational analysis. Our findings provide insight into the structural features of amyloid molecules formed at low concentrations of monomer, which will help determine the clinical targets (in therapy) to effectively inhibit amyloid formation in the early stages of the amyloid growth phase.
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