New peptide and protein-conjugates will be in the focus of the project B5 to target multivalent receptors in vitro and in vivo. Large protein structures, for instance viral capsids and flagella-filaments, will be employed in the design of multivalent scaffolds for the interaction with viral glycoproteins. Additionally, new multivalent ligands including PEGylated or structurally stabilized peptides as well as oligosaccharides will be conjugated to protein scaffolds and polymers using chemoselective reactions, which also includes an affinity-driven dynamic ligation. These functional conjugates will be used to address biologically and pharmacologically relevant C-type lectin receptors and membrane-bound scavenger receptors and will be furthermore applied to medicinally relevant virus-host cell-interactions in highly pathogenic viruses.

DFG Programme Collaborative Research Centres

Subproject of SFB 765:  Multivalency as Chemical Organisation and Action Principle: New Architectures, Functions and Applications

Applicant Institution Freie Universität Berlin

Co-Applicant Institution Leibniz-Forschungsinstitut für Molekulare Pharmakologie (FMP)
im Forschungsverbund Berlin e.V.; Technische Universität Berlin

Project Heads Professor Dr. Nediljko Budisa; Professor Dr. Christian Hackenberger