Abstract
The transmissible spongiform encephalopathies (TSEs) are neurodegenerative diseases characterized by amyloid formation in the brain. The major amyloid protein is the prion protein (PrP). PrP and the beta-amyloid protein of Alzheimer disease share a similar sequence that, in both cases, may be responsible for the initiation of protein aggregation in vivo. We report here that a peptide based on this sequence in PrP (PrP96-111M) forms amyloid fibrils. The existence of a kinetic barrier to amyloid formation by this peptide was demonstrated, suggesting that formation of an ordered nucleus is the rate-determining step for aggregation. Seeding was demonstrated to occur with PrP96-111M amyloid fibrils but not with amyloid fibrils of a related peptide. This effect is consistent with the proposal that the aggregation of PrP, which characterizes TSE, involves a nucleation event analogous to the seeding of a crystallization.
Dates
| Type | When |
|---|---|
| Created | 19 years, 3 months ago (May 31, 2006, 8:25 a.m.) |
| Deposited | 3 years, 4 months ago (April 13, 2022, 1:26 p.m.) |
| Indexed | 2 weeks, 1 day ago (Aug. 20, 2025, 8:42 a.m.) |
| Issued | 32 years, 2 months ago (July 1, 1993) |
| Published | 32 years, 2 months ago (July 1, 1993) |
| Published Online | 32 years, 2 months ago (July 1, 1993) |
| Published Print | 32 years, 2 months ago (July 1, 1993) |
@article{Come_1993, title={A kinetic model for amyloid formation in the prion diseases: importance of seeding.}, volume={90}, ISSN={1091-6490}, url={http://dx.doi.org/10.1073/pnas.90.13.5959}, DOI={10.1073/pnas.90.13.5959}, number={13}, journal={Proceedings of the National Academy of Sciences}, publisher={Proceedings of the National Academy of Sciences}, author={Come, J H and Fraser, P E and Lansbury, P T}, year={1993}, month=jul, pages={5959–5963} }