Issue 11, 2013
From the journal:

Organic & Biomolecular Chemistry

Helical peptides from VEGF and Vammin hotspots for modulating the VEGF–VEGFR interaction

María Isabel García-Aranda,a   Susana González-López,a   Clara María Santiveri,b   Nathalie Gagey-Eilstein,c   Marie Reille-Seroussi,c   Mercedes Martín-Martínez,a   Nicolas Inguimbert,cd   Michel Vidal,ce   María Teresa García-López,a   María Angeles Jiménez,b   Rosario González-Muñiza  and  María Jesús Pérez de Vega*a  

* Corresponding authors

a Instituto de Química Médica, CSIC, C/Juan de la Cierva 3, 28006 Madrid, Spain
E-mail: pdevega@iqm.csic.es

b Instituto de Química-Física Rocasolano, CSIC, C/Serrano 119, 28006 Madrid, Spain

c Université Paris Descartes, UFR des Sciences Pharmaceutiques et Biologiques, UMR CNRS 8638, 4 Avenue de l'Observatoire, Paris F-75270, France

d Université de Perpignan Via Domitia, Laboratoire de Chimie des Biomolécules et de l'Environnement, EA 4215, 52 Avenue P. Alduy, Perpignan F-66860, France

e UF Pharmacinétique et Pharmacochimie, GH Cochin – Hôtel Dieu – Broca, Hôpital Cochin, AP-HP, Paris, France

Abstract

The design, synthesis, conformational studies and binding affinity for VEGF receptors of a collection of linear and cyclic peptide analogues of the N-terminal α-helix fragments 13–25 of VEGF and 1–13 of Vammin are described. Linear 13(14)-mer peptides were designed with the help of an AGADIR algorithm and prepared following peptide solid-phase synthetic protocols. Cyclic peptide derivatives were prepared on-resin from linear precursors with conveniently located Glu and Lys residues, by the formation of amide linkages. Conformational analysis, CD and NMR, showed that most synthesized peptides have a clear tendency to be structured as α-helices in solution. Some of the peptides were able to bind a VEGFR-1 receptor with moderate affinity. In addition to the described key residues (Phe17, Tyr21 and Tyr25), Val14 and Val20 seem to be relevant for affinity.

Graphical abstract: Helical peptides from VEGF and Vammin hotspots for modulating the VEGF–VEGFR interaction

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Article information

DOI
https://doi.org/10.1039/C3OB27312A
Article type
Paper
Submitted
28 Nov 2012
Accepted
18 Jan 2013
First published
18 Jan 2013

Org. Biomol. Chem., 2013,11, 1896-1905

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Helical peptides from VEGF and Vammin hotspots for modulating the VEGF–VEGFR interaction

M. I. García-Aranda, S. González-López, C. M. Santiveri, N. Gagey-Eilstein, M. Reille-Seroussi, M. Martín-Martínez, N. Inguimbert, M. Vidal, M. T. García-López, M. A. Jiménez, R. González-Muñiz and M. J. Pérez de Vega, Org. Biomol. Chem., 2013, 11, 1896 DOI: 10.1039/C3OB27312A

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