Artículos de revistas
Combinatorial Library Screening Coupled to Mass Spectrometry toIdentify Valuable Cyclic Peptides
Date
2016-01Registration in:
Camperi, Silvia Andrea; Giudicessi, Silvana Laura; Martínez Ceron, María Camila; Gurevich Messina, Juan Manuel; Saavedra, Soledad Lorena; et al.; Combinatorial Library Screening Coupled to Mass Spectrometry toIdentify Valuable Cyclic Peptides; Wiley; Curr Protoc Chem Biol; 8; 2; 1-2016; 109-130
2160-4762
CONICET Digital
CONICET
Author
Camperi, Silvia Andrea
Giudicessi, Silvana Laura
Martínez Ceron, María Camila
Gurevich Messina, Juan Manuel
Saavedra, Soledad Lorena
Acosta, Gerardo
Cascone, Osvaldo
Erra Balsells, Rosa
Albericio Palomera, Fernando
Abstract
Combinatorial library screening coupled to mass spectrometry (MS) analysis isa practical approach to identify useful peptides. Cyclic peptides can have highbiological activity, selectivity, and affinity for target proteins, and high stabilityagainst proteolytic degradation. Here we describe two strategies to preparecombinatorial libraries suitable for MS analysis to accelerate the discoveryof cyclic peptide structures. Both approaches use ChemMatrix resin and thelinker 4-hydroxymethylbenzoic acid. One strategy involves the synthesis ofa one-bead?two-peptides library in which each bead contains both the cyclicpeptide and its linear counterpart to facilitate MS analysis. The other protocol isbased on the synthesis of a cyclic depsipeptide library in which a glycolamidicester group is incorporated by adding glycolic acid. After library screening, thering is opened and the peptide is released simultaneously for subsequent MSanalysis.