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Preferential selection of Cys-constrained peptides from a random phage-displayed library by anti-glucitollysine antibodies

✍ Scribed by Gertrudis Rojas; Amaury Pupo; Maria Del Rosario Aleman; Nelson Santiago Vispo


Book ID
105359697
Publisher
John Wiley and Sons
Year
2008
Tongue
English
Weight
104 KB
Volume
14
Category
Article
ISSN
1075-2617

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✦ Synopsis


Abstract

Phage‐displayed peptides recognized by two monoclonal antibodies against glucitollysine were selected. The most prominent feature of the peptide panel was the presence of paired Cys in most of them (21/24 peptides). The availability of a wide variety of peptides having differently spaced paired Cys, as well as truly linear Cys‐free peptides, gave the opportunity to explore the role of disulfide bridges in phage selection. Some Cys‐containing peptides came from a Cys‐flanked cyclic 9‐mer library, but most of them (18/21) were derived from a totally random 12‐mer library, and hence the presence of Cys was dictated by the selector antibodies. Motifs shared by several peptides (potentially involved in binding) often contained or were flanked by Cys residues. Binding of all Cys‐containing phage‐displayed peptides was abolished/decreased after a reducing treatment. Screening a random peptide library (without invariant Cys residues) is powerful enough to clearly reveal the need, preferences, and diversity of Cys‐mediated structural constraints for recognition. Copyright © 2008 European Peptide Society and John Wiley & Sons, Ltd.


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