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Flexibility-tuning of dual-display DNA-encoded chemical libraries facilitates cyclic peptide ligand discovery

Dimitar Petrov, Louise Plais, Kristina Schira, Junyu Cai, Michelle Keller, Alice Lessing, Gabriele Bassi, Samuele Cazzamalli, Dario Neri, Andreas Gloger, Jörg Scheuermann

2025Nature Communications19 citationsDOIOpen Access PDF

Abstract

Cyclic peptides constitute an important drug modality since they offer significant advantages over small molecules and macromolecules. However, access to diverse chemical sets of cyclic peptides is difficult on a large library scale. DNA-encoded Chemical Libraries (DELs) provide a suitable tool to obtain large chemical diversity, but cyclic DELs made by standard DEL implementation cannot efficiently explore their conformational diversity. On the other hand, dual-display Encoded Self-Assembling Chemical (ESAC) Libraries can be used for modulating macrocycle flexibility since the two displayed peptides can be connected in an incremental fashion. In this work, we construct a 56 million dual-display ESAC library using a two-step cyclization strategy. We show that varying the level of conformational restraint is essential for the discovery of specific ligands for the three protein targets thrombin, human alkaline phosphatase and streptavidin.

Topics & Concepts

Flexibility (engineering)Drug discoveryCyclic peptideComputational biologyComputer scienceConstruct (python library)Dual (grammatical number)Combinatorial chemistryOligonucleotideChemistryPeptideSmall moleculeDNABiochemistryBiologyLiteratureStatisticsArtMathematicsProgramming languageChemical Synthesis and AnalysisMonoclonal and Polyclonal Antibodies ResearchBiochemical and Structural Characterization
Flexibility-tuning of dual-display DNA-encoded chemical libraries facilitates cyclic peptide ligand discovery | Litcius