Antibacterial lead discovery with D/L-peptide libraries

Objetivo

Nowadays, a multitude of examples for targeting enzymes with small molecules is known, whereas the direkt access to macromolecular interaction, such as DNA/protein, RNA/protein and protein/protein within the cell still waits to be solved by generic methods. We intend to create a toolbox for targeting these interactions with D-/L-peptides, a new class of biostable oligomer ligands. Initially we will establish split-and-pool libraries using postsynthetic dimerization of two orthogonal pairing partners which can be expected to form stable folds of the size of interactive protein subdomains. In a second approach, specific target functions and interaction domains will be used to generate new ligands by design and structural analogy. Folding and secondary structure preference of the most potent constructs will be elucidated (CD, NMR, FRET) to deduce preferences for pairing, minimal sequence length, and composition. Macromolecular targets and activity will be further studied using fluorescence microscopy and protein binding assays.

Ámbito científico

• natural sciencesbiological sciencesgeneticsDNA
• natural sciencesphysical sciencesopticsmicroscopy
• natural sciencesbiological sciencesgeneticsRNA
• natural sciencesbiological sciencesbiochemistrybiomoleculesproteinsenzymes

Palabras clave

• Bioorganic chemistry
• D/L-peptides
• antimicrobial peptides
• library screening
• peptide synthesis
• structure-activity relationships

Programa(s)

• FP7-PEOPLE - Specific programme "People" implementing the Seventh Framework Programme of the European Community for research, technological development and demonstration activities (2007 to 2013)

Tema(s)

• FP7-PEOPLE-IEF-2008 - Marie Curie Action: "Intra-European Fellowships for Career Development"

Convocatoria de propuestas

FP7-PEOPLE-IEF-2008
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Régimen de financiación

Coordinador