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. 2009 Jul 1;17(13):4825-32.
doi: 10.1016/j.bmc.2009.03.054. Epub 2009 Apr 1.

Phage display screening against a set of targets to establish peptide-based sugar mimetics and molecular docking to predict binding site

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Phage display screening against a set of targets to establish peptide-based sugar mimetics and molecular docking to predict binding site

Limin Yu et al. Bioorg Med Chem. .

Abstract

A novel selection approach is presented to screen phage display peptide libraries against sets of receptors that share specificity for the same ligand. This strategy was applied to the discovery of glycomimetic peptides. Through these screens, a number of peptide clones were discovered that bind the lectins used in the screen, in a sugar competitive manner. In addition, the majority of the selected peptides demonstrate sugar type mimicry consistent with lectin specificity. Docking studies were conducted to establish whether the mimetic peptides bind to the lectin ConA at the sugar binding site or to a nearby, alternative site shown to bind to YPY-containing peptides previously discovered from single-target screens. Of the three cyclic peptides subjected to computational docking, CNTPLTSRC had the highest predicted affinity and CSRILTAAC demonstrated specificity for the sugar binding site comparable to the natural ligand itself.

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