Affiliation:
1. Sorbonne Université École Normale Supérieure PSL University CNRS Laboratoire des Biomolécules LBM 75005 Paris France
2. UMR 5247-CNRS-UM-ENSCM Institut des Biomolécules Max Mousseron (IBMM) Université de Montpellier Montpellier France
3. MS3U Platform Fédération de Chimie Moléculaire de Paris Centre – FR2769 Sorbonne Université 4 Place Jussieu 75005 Paris France
Abstract
AbstractTarget‐directed dynamic combinatorial chemistry is a very attractive strategy for the discovery of bioactive peptides. However, its application has not yet been demonstrated, presumably due to analytical challenges that arise from the diversity of a peptide library with combinatorial side‐chains. We previously reported an efficient method to generate, under biocompatible conditions, large dynamic libraries of cyclic peptides grafted with amino acid's side‐chains, by thiol‐to‐thioester exchanges. In this work, we present analytical tools to easily characterize such libraries by HPLC and mass spectrometry, and in particular to simplify the isomers’ distinction requiring sequencing by MS/MS fragmentations. After structural optimization, the cyclic scaffold exhibits a UV‐tag, absorbing at 415 nm, and an ornithine residue which favors the regioselective ring‐opening and simultaneous MS/MS fragmentation, in the gas‐phase.
Subject
Organic Chemistry,Molecular Biology,Molecular Medicine,Biochemistry