Monitoring Alzheimer Amyloid Peptide Aggregation by EPR

被引:0
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作者
I. Sepkhanova
M. Drescher
N. J. Meeuwenoord
R. W. A. L. Limpens
R. I. Koning
D. V. Filippov
M. Huber
机构
[1] Leiden University,Huygens Laboratory, Department of Molecular Physics
[2] Leiden University,Leiden Institute of Chemistry
[3] Leiden University Medical Center,Section Electron Microscopy, Department of Molecular Cell Biology
来源
关键词
Electron Paramagnetic Resonance; Fibril; Electron Paramagnetic Resonance Spectrum; Spin Label; Electron Paramagnetic Resonance Experiment;
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摘要
Plaques containing the aggregated β-Amyloid (Aβ) peptide in the brain are the main indicators of Alzheimer’s disease. Fibrils, the building blocks of plaques, can also be produced in vitro and consist of a regular arrangement of the peptide. The initial steps of fibril formation are not well understood and could involve smaller aggregates (oligomers) of Aβ. Such oligomers have even been implicated as the toxic agents. Here, a method to study oligomers on the time scale of aggregation is suggested. We have labeled the 40 residue Aβ peptide variant containing an N-terminal cysteine (cys-Aβ) with the MTSL [1-oxyl-2,2,5,5-tetramethyl-Δ-pyrroline-3-methyl] methanethiosulfonate spin label (SL-Aβ). Fibril formation in solutions of pure SL-Aβ and of SL-Aβ mixed with Aβ was shown by Congo-red binding and electron microscopy. Continuous-wave 9 GHz electron paramagnetic resonance reveals three fractions of different spin-label mobility: one attributed to monomeric Aβ, one to a multimer (8–15 monomers), and the last one to larger aggregates or fibrils. The approach, in principle, allows detection of oligomers on the time scale of aggregation.
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页码:209 / 222
页数:13
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