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research article

Pharmacological profiles of peptide drug candidates for the treatment of Alzheimer's disease

Adessi, C
•
Frossard, MJ
•
Boissard, C
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2003
Journal of Biological Chemistry

Amyloid plaques in brain, composed of aggregates of amyloid-beta peptide, play a central role in the pathogenesis of Alzheimer's disease and represent a good target for treatment. We have shown previously that a 5-amino acid beta-sheet breaker peptide (iAbeta5p), end-protected, has the ability to induce a dramatic reduction in amyloid deposition in two different transgenic Alzheimer's models (Permanne, B., Adessi, C., Saborio, G. P., Fraga, S., Frossard, M.-J., Dewachter, I., Van Dorpe, J., Banks, W. A., Van Leuven, F., and Soto, C. (2002) FASEB J. 16, 860 - 862). The aim of this study was to evaluate the effect of chemical modifications of the peptide bonds at the metabolite cleavage sites on the pharmacological properties of iAbeta5p derivatives. Using a rational approach, peptide analogs were designed and tested for in vitro activity and enzymatic stability. One peptide analog containing a methyl group introduced at the nitrogen atom of one amide bond showed increased stability in vitro, a 10-fold higher in vivo half-life, and good brain uptake compared with iAbeta5p while maintaining a similar activity in vitro. Our results suggest that the pharmacological profile of beta-sheet breaker peptides can be improved to produce compounds with drug-like properties that might offer a new promise in the treatment of Alzheimer's disease.

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Type
research article
DOI
10.1074/jbc.M211976200
Web of Science ID

WOS:000182405000045

Author(s)
Adessi, C
Frossard, MJ
Boissard, C
Fraga, S
Bieler, S
Ruckle, T
Vilbois, F
Robinson, SM
Mutter, M  
Banks, WA
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Date Issued

2003

Published in
Journal of Biological Chemistry
Volume

278

Issue

16

Start page

13905

End page

13911

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LCBP  
Available on Infoscience
February 9, 2006
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/222295
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