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Infrared Laser-Induced Amyloid Fibril Dissociation: A Joint Experimental/Theoretical Study on the GNNQQNY Peptide
Author(s) -
Takayasu Kawasaki,
Viet Hoang Man,
Yasunobu Sugimoto,
Nobuyuki Sugiyama,
Hiroko Yamamoto,
Koichi Tsukiyama∥,
Junmei Wang,
Philippe Derreumaux,
Phuong H. Nguyen
Publication year - 2020
Publication title -
the journal of physical chemistry b
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.864
H-Index - 392
eISSN - 1520-6106
pISSN - 1520-5207
DOI - 10.1021/acs.jpcb.0c05385
Subject(s) - fibril , dissociation (chemistry) , amyloid fibril , chemistry , intermolecular force , biophysics , laser , hydrogen bond , chemical physics , materials science , crystallography , photochemistry , molecule , amyloid β , optics , biochemistry , organic chemistry , physics , biology , medicine , disease , pathology
Neurodegenerative diseases are usually characterized by plaques made of well-ordered aggregates of distinct amyloid proteins. Dissociating these very stable amyloid plaques is a critical clinical issue. In this study, we present a joint mid-infrared free electron laser experiment/nonequilibrium molecular dynamics simulation to understand the dissociation process of a representative example GNNQQNY fibril. By tuning the laser frequency to the amide I band of the fibril, the resonance takes place and dissociation is occurred. With the calculated and observed wide-angle X-ray scattering profiles and secondary structures before and after laser irradiation being identical, we can propose a dissociation mechanism with high confidence from our simulations. We find that dissociation starts in the core of the fibrils by fragmenting the intermolecular hydrogen bonds and separating the peptides and then propagates to the fibril extremities leading to the formation of unstructured expanded oligomers. We suggest that this should be a generic mechanism of the laser-induced dissociation of amyloid fibrils.

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