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Promiscuity mapping of the S100 protein family using a high-throughput holdup assay

Márton A. Simon, Éva Bartus, Beáta Mag, Eszter Boros, Lea Roszjár, Gergő Gógl, Gilles Travé, Tamás A. Martinek, László Nyitray

2022Scientific Reports17 citationsDOIOpen Access PDF

Abstract

-dependent protein-protein interactions in the intra- and extracellular environment and are overexpressed in various pathologies. There are about 20 distinct human S100 proteins with numerous potential partner proteins. Here, we used a quantitative holdup assay to measure affinity profiles of most members of the S100 protein family against a library of chemically synthetized foldamers. The profiles allowed us to quantitatively map the binding promiscuity of each member towards the foldamer library. Since the library was designed to systematically contain most binary natural amino acid side chain combinations, the data also provide insight into the promiscuity of each S100 protein towards all potential naturally occurring S100 partners in the human proteome. Such information will be precious for future drug design to interfere with S100 related pathologies.

Topics & Concepts

PromiscuityProteomeHuman proteome projectComputational biologyAmino acidDrug discoveryFoldamerS100 proteinProtein familyBiologyChemistryBiochemistryProteomicsGeneImmunologyEcologyImmunohistochemistryS100 Proteins and AnnexinsAntimicrobial Peptides and ActivitiesMachine Learning in Bioinformatics
Promiscuity mapping of the S100 protein family using a high-throughput holdup assay | Litcius