Synthetic Strategies to Prepare Bioactive Lysine and Peptide Conjugates With Triazolium Derivatives

Author:

Ledwoń Patrycja12ORCID,Jewginski Michał1ORCID,Bello Claudia3ORCID,Nuti Francesca3ORCID,Rovero Paolo1ORCID,Latajka Rafal2ORCID,Papini Anna Maria3ORCID

Affiliation:

1. Interdepartmental Research Unit of Peptide and Protein Chemistry and Biology Department of NeuroFarBa University of Florence Via Ugo Schiff 6 50019 Sesto Fiorentino Italy

2. Department of Bioorganic Chemistry Faculty of Chemistry Wrocław University of Science and Technology Wybrzeze Wyspianskiego 27 50370 Wrocław Poland

3. Interdepartmental Research Unit of Peptide and Protein Chemistry and Biology Department of Chemistry “Ugo Schiff” University of Florence Via della Lastruccia 13 50019 Sesto Fiorentino Italy

Abstract

AbstractPeptides conjugated with organic molecules can be useful tools for the development of novel bioactive compounds. The lysine side‐chain is an interesting functional group to act as a linker to connect small molecules in peptide conjugates. Herein we present the design and synthesis of four Safirinium derivatives, their facile conjugation to lysine in solid phase, and incorporation in peptides. The compounds differing in the functionalization of nitrogen N2 of the condensed triazolyl moiety are novel building blocks to design conjugates to perform structure‐activity relationship studies of elastase inhibitors. Consequently, structural investigations of the lysine building blocks and of the corresponding peptide conjugates were performed. We present herein the potential of the Safirinium analogs to act as elastase inhibitors in assays performed on porcine pancreas elastase.

Publisher

Wiley

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