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Literature DB >> 24288253

Structure of a complex formed by a protein and a helical aromatic oligoamide foldamer at 2.1 Å resolution.

Jérémie Buratto¹, Cinzia Colombo, Marine Stupfel, Simon J Dawson, Christel Dolain, Béatrice Langlois d'Estaintot, Lucile Fischer, Thierry Granier, Michel Laguerre, Bernard Gallois, Ivan Huc.

Abstract

In the search of molecules that could recognize sizeable areas of protein surfaces, a series of ten helical aromatic oligoamide foldamers was synthesized on solid phase. The foldamers comprise three to five monomers carrying various proteinogenic side chains, and exist as racemic mixtures of interconverting right-handed and left-handed helices. Functionalization of the foldamers by a nanomolar ligand of human carbonic anhydrase II (HCA) ensured that they would be held in close proximity to the protein surface. Foldamer-protein interactions were screened by circular dichroism (CD). One foldamer displayed intense CD bands indicating that a preferred helix handedness is induced upon interacting with the protein surface. The crystal structure of the complex between this foldamer and HCA could be resolved at 2.1 Å resolution and revealed a number of unanticipated protein-foldamer, foldamer-foldamer, and protein-protein interactions.

Entities: Chemical Gene Species

Keywords: circular dichroism; crystallography; foldamers; protein recognition; solid-phase synthesis

Mesh：

Substances：

Year: 2013 PMID： 24288253 DOI： 10.1002/anie.201309160

Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN： 1433-7851 Impact factor: 15.336

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Cited

12 in total

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Journal: Angew Chem Int Ed Engl Date: 2014-10-06 Impact factor: 15.336

Structure of a complex formed by a protein and a helical aromatic oligoamide foldamer at 2.1 Å resolution.

1. Macromolecular Crystallography for Synthetic Abiological Molecules: Combining xMDFF and PHENIX for Structure Determination of Cyanostar Macrocycles.

2. Inhibition of β-catenin/B cell lymphoma 9 protein-protein interaction using α-helix-mimicking sulfono-γ-AApeptide inhibitors.

3. Computational Prediction of the Binding Pose of Metal-Binding Pharmacophores.

4. Optimizing side chains for crystal growth from water: a case study of aromatic amide foldamers.

5. Supramolecular Chemistry Targeting Proteins.

6. Crowning proteins: modulating the protein surface properties using crown ethers.

7. Hexagonal Lyotropic Liquid Crystal from Simple "Abiotic" Foldamers.

8. An α-Helix-Mimicking 12,13-Helix: Designed α/β/γ-Foldamers as Selective Inhibitors of Protein-Protein Interactions.

9. A Binary Bivalent Supramolecular Assembly Platform Based on Cucurbit[8]uril and Dimeric Adapter Protein 14-3-3.

10. Discrimination of supramolecular chirality using a protein nanopore.