Pseudo-prolines: Reversible, conformational trap of cyclosporin C as novel concept for prodrug design

The selective and reversible insertion of pseudo-proline (PsiPro) Systems in cyclosporin C (CsC) featuring different C(2) substituents at the oxazolidine ring and its impact on the conformational and biological properties is described. The presence of a 5-membered ring exerts drastic effects upon the backbone conformation of CsC as demonstrated by NMR analysis. For example, the number of conformations, in particular in DMSO-d6, is strongly reduced and a cis 1-2 amide bond is induced when dialkylated at the C(2) position, resulting in a complete loss of the binding capacity to its receptor CypA. The reversibility of PsiPro insertion allows the temporary introduction of conformational constraints representing a new strategy in pro-drug design.

Pseudo-prolines: Reversible, conformational trap of cyclosporin C as novel concept for prodrug design

Molten globule-like transition state of protein barnase measured with calorimetric force spectroscopy

Deep learning approaches for conformational flexibility and switching properties in protein design

Towards automating de novo protein design for novel functionalities: controlling protein folds and protein-protein interactions

Towards automating de novo protein design for novel functionalities: controlling protein folds and protein-protein interactions

Deep learning approaches for conformational flexibility and switching properties in protein design

Molten globule-like transition state of protein barnase measured with calorimetric force spectroscopy