Mechanochemical mechanism for peptidyl free radical generation by amyloid fibrils

β-Amyloid peptides (Aβ) form the core of Alzheimer's disease (AD) senile plaques, and are implicated in AD neurotoxicity. Aβ and some derivatives generate free radicals upon fibrilogenesis. A mechanism for free radical generation is proposed, based upon fibril cross β-sheet structure: (1) Durin...

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Bibliographic Details
Published in:FEBS letters 1997-02, Vol.403 (3), p.230-235
Main Author: Kay, Christopher J
Format: Article
Language:English
Subjects:
Alzheimer's disease
Amyloid beta-Peptides - chemistry
Amyloid beta-Peptides - metabolism
Amyloid beta-Peptides - toxicity
Amyloid beta-protein
Fibroins - chemistry
Free radical
Free Radicals
Models, Chemical
Models, Molecular
Oxygen - metabolism
Peptides - metabolism
Peptides - toxicity
Prion disease
Protein Denaturation
Protein Structure, Secondary
Stress, Mechanical
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Summary:β-Amyloid peptides (Aβ) form the core of Alzheimer's disease (AD) senile plaques, and are implicated in AD neurotoxicity. Aβ and some derivatives generate free radicals upon fibrilogenesis. A mechanism for free radical generation is proposed, based upon fibril cross β-sheet structure: (1) During fibrilogenesis there is a small probability of mispacking of Aβ monomers, resulting in abnormal fibril packing. (2) Continued fibrilogenesis traps a packing defect within the β-sheet. Surrounding β-sheet resists distortion, and the abnormally packed polypeptide(s) is strained. (3) Thermal processes cause homolytic bond scission and radical production from strained polypeptide through mechanically activated thermal decomposition. (4) Reaction with oxygen produces peroxy radicals, prevents unproductive radical recombination, and promotes observed cross-linking, production of reactive oxygen species and peptide fragmentation. Adiabatic mapping suggested significant strain would be generated by β-sheet misalignment. The mechanism relates the common structure of fibrils to radical production, and may be relevant to cytotoxicity in prion and other amyloidoses. © 1997 Federation of European Biochemical Societies.
ISSN:0014-5793
1873-3468
DOI:10.1016/S0014-5793(97)00076-8