Search CORE

2 research outputs found

Polymorphic Structures of Alzheimer's β-Amyloid Globulomers

Author: A Olofsson
A Quist
A Schmechel
A Zhang
AE Roher
AK Paravastu
AM Catriona
Amit Singh
AT Petkova
AT Petkova
B Ma
C Haass
DJ Selkoe
DM Alexander Jr
E Cerf
G Bellesia
G Reddy
G Reddy
GM Shankar
GP Gellermann
H Jang
HKL Blackley
J Zheng
J Zheng
J Zheng
J Zheng
J Zheng
JC Rochet
Jie Zheng
KL Viola
L Kale
L Yu
LW Hung
M Ahmed
M Cheon
M Di Carlo
M Zhu
MD Kirkitadze
MG Krone
MW Dominic
N Chaudhary
N Rezaei-Ghaleh
PN Lacor
R Goda
R Kayed
R Stehanie
R Tycko
S Barghorn
S Kim
S Mukherjee
S Wray
SC Meredith
T Luhrs
T Sato
THJ Huang
V Nimmrich
W Humphrey
W Hwang
W Im
X Yu
Xiang Yu
Y Miller
Y Miller
Y Miller
Y-H Lee
Publication venue: Public Library of Science
Publication date: 07/06/2011
Field of study

Misfolding and self-assembly of Amyloid-β (Aβ) peptides into amyloid fibrils is pathologically linked to the development of Alzheimer's disease. Polymorphic Aβ structures derived from monomers to intermediate oligomers, protofilaments, and mature fibrils have been often observed in solution. Some aggregates are on-pathway species to amyloid fibrils, while the others are off-pathway species that do not evolve into amyloid fibrils. Both on-pathway and off-pathway species could be biologically relevant species. But, the lack of atomic-level structural information for these Aβ species leads to the difficulty in the understanding of their biological roles in amyloid toxicity and amyloid formation.Here, we model a series of molecular structures of Aβ globulomers assembled by monomer and dimer building blocks using our peptide-packing program and explicit-solvent molecular dynamics (MD) simulations. Structural and energetic analysis shows that although Aβ globulomers could adopt different energetically favorable but structurally heterogeneous conformations in a rugged energy landscape, they are still preferentially organized by dynamic dimeric subunits with a hydrophobic core formed by the C-terminal residues independence of initial peptide packing and organization. Such structural organizations offer high structural stability by maximizing peptide-peptide association and optimizing peptide-water solvation. Moreover, curved surface, compact size, and less populated β-structure in Aβ globulomers make them difficult to convert into other high-order Aβ aggregates and fibrils with dominant β-structure, suggesting that they are likely to be off-pathway species to amyloid fibrils. These Aβ globulomers are compatible with experimental data in overall size, subunit organization, and molecular weight from AFM images and H/D amide exchange NMR.Our computationally modeled Aβ globulomers provide useful insights into structure, dynamics, and polymorphic nature of Aβ globulomers which are completely different from Aβ fibrils, suggesting that these globulomers are likely off-pathway species and explaining the independence of the aggregation kinetics between Aβ globulomers and fibrils

Public Library of Science (PLOS)

Crossref

PubMed Central

Comparative Molecular Dynamics Study of Aβ Adsorption on the Self-Assembled Monolayers

Crossref