Issue 17, 2009

Towards the conformational mimicry of the measles virus HNE loop: design, synthesis and biological evaluation of a cyclic bile acid–peptide conjugate

Abstract

The current article reports the design, synthesis and biochemical evaluation of a cyclic bile acid–peptide conjugate as a mimic of the loop-like structure of the measles virus haemagglutinin noose epitope (HNE). This macrocyclic structure was assembled by solid phase synthesis. Scaffold-peptide ring closure was achieved via the introduction of a succinate linker. After disulfide bridge formation with iodine, the desired 14 amino acid cyclic conjugate was obtained with overall yields between 15 and 35%. NMR analysis supports the presence of a helical conformation in the Q384-G388 pentapeptide portion, in agreement with the organisation of this chain in the native protein. The compound was found to have increased biostability compared to stabilised linear peptides, displayed good binding towards monoclonal antibodies known to bind to HNE and thus has potential in an alternative peptide-based measles vaccine.

Graphical abstract: Towards the conformational mimicry of the measles virus HNE loop: design, synthesis and biological evaluation of a cyclic bile acid–peptide conjugate

Supplementary files

Article information

Article type
Paper
Submitted
14 Apr 2009
Accepted
03 Jun 2009
First published
07 Jul 2009

Org. Biomol. Chem., 2009,7, 3391-3399

Towards the conformational mimicry of the measles virus HNE loop: design, synthesis and biological evaluation of a cyclic bile acid–peptide conjugate

C. A. Bodé, T. Bechet, E. Prodhomme, K. Gheysen, P. Gregoir, J. C. Martins, C. P. Muller and A. Madder, Org. Biomol. Chem., 2009, 7, 3391 DOI: 10.1039/B907395G

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