Switch-Peptides: Design and Characterization of Controllable Super-Amyloid-Forming Host-Guest Peptides as Tools for Identifying Anti-Amyloid Agents

Several amyloid-forming proteins are characterized by the presence of hydrophobic and highly amyloidogenic core sequences that play critical roles in the initiation and progression of amyloid fibril formation. Therefore targeting these sequences represents a viable strategy for identifying candidate...

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Published in:	Chembiochem : a European journal of chemical biology Vol. 9; no. 13; pp. 2104 - 2112
Main Authors:	Camus, Marie-Stéphanie, Dos Santos, Sonia, Chandravarkar, Arunan, Mandal, Bhubaneswar, Schmid, Adrian W, Tuchscherer, Gabriele, Mutter, Manfred, Lashuel, Hilal A
Format:	Journal Article
Language:	English
Published:	Weinheim Wiley-VCH Verlag 01-09-2008 WILEY-VCH Verlag WILEY‐VCH Verlag
Subjects:	aggregation Alzheimer's disease Amino Acid Sequence Amyloid - antagonists & inhibitors Amyloid - metabolism amyloid fibrils conformation analysis Drug Design Drug Evaluation, Preclinical host-guest switch peptides Hydrophobic and Hydrophilic Interactions Kinetics Molecular Sequence Data Peptides - chemical synthesis Peptides - chemistry Peptides - metabolism Protein Binding - drug effects Protein Structure, Secondary Small Molecule Libraries - pharmacology
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Summary:	Several amyloid-forming proteins are characterized by the presence of hydrophobic and highly amyloidogenic core sequences that play critical roles in the initiation and progression of amyloid fibril formation. Therefore targeting these sequences represents a viable strategy for identifying candidate molecules that could interfere with amyloid formation and toxicity of the parent proteins. However, the highly amyloidogenic and insoluble nature of these sequences has hampered efforts to develop high-throughput fibrillization assays. Here we describe the design and characterization of host-guest switch peptides that can be used for in vitro mechanistic and screening studies that are aimed at discovering aggregation inhibitors that target highly amyloidogenic sequences. These model systems are based on a host-guest system where the amyloidogenic sequence (guest peptide) is flanked by two β-sheet-promoting (Leu-Ser)n oligomers as host sequences. Two host-guest peptides were prepared by using the hydrophobic core of Aβ comprising residues 14-24 (HQKLVFFAEDV) as the guest peptide with switch elements inserted within (peptide 1) or at the N and C termini of the guest peptide (peptide 2). Both model peptides can be triggered to undergo rapid self-assembly and amyloid formation in a highly controllable manner and their fibrillization kinetics is tuneable by manipulating solution conditions (for example, peptide concentration and pH). The fibrillization of both peptides reproduces many features of the full-length Aβ peptides and can be inhibited by known inhibitors of Aβ fibril formation. Our results suggest that this approach can be extended to other amyloid proteins and should facilitate the discovery of small-molecule aggregation inhibitors and the development of more efficacious anti-amyloid agents to treat and/or reverse the pathogenesis of neurodegenerative and systemic amyloid diseases.
Bibliography:	http://dx.doi.org/10.1002/cbic.200800245 ArticleID:CBIC200800245 Debiopharm SA, Lausanne ark:/67375/WNG-BCP4VRBL-3 istex:8816570722ACD0E43212C10E7FF41BD26F7848AD National Science Foundation ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23
ISSN:	1439-4227 1439-7633
DOI:	10.1002/cbic.200800245