Comparison of bacterial and phage display peptide libraries in search of target-binding motif |
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Authors: | Mojca Lunder Tomaž Bratkovič Bojan Doljak Samo Kreft Uroš Urleb Borut Štrukelj Nadja Plazar |
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Affiliation: | (1) Department of Pharmaceutical Biology, Faculty of Pharmacy, University of Ljubljana, Aškerčeva 7, SI-1000 Ljubljana, Slovenia;(2) Lek Pharmaceutical Company, Verovškova 57, SI-1000 Ljubljana, Slovenia;(3) Jožef Stefan Institute, Jamova 39, SI-1000 Ljubljana, Slovenia;(4) College of Health Care of Izola, University of Primorska, Polje 42, SI-6310 Izola, Slovenia |
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Abstract: | Genetic engineering allows modification of bacterial and bacteriophage genes, which code for surface proteins, enabling display of random peptides on the surface of these microbial vectors. Biologic peptide libraries thus formed are used for high-throughput screening of clones bearing peptides with high affinity for target proteins. There are reports of many successful affinity selections performed with phage display libraries and substantially fewer cases describing the use of bacterial display systems. In theory, bacterial display has some advantages over phage display, but the two systems have never been experimentally compared. We tested both techniques in selecting streptavidin-binding peptides from two commercially available libraries. Under similar conditions, selection of phage-displayed peptides to model protein streptavidin proved convincingly better. |
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Keywords: | Phage display library bacterial display library affinity selection ligand peptide streptavidin |
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