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Effects on in vitro and in vivo angiogenesis induced by small peptides carrying adhesion sequences
Authors:Maria Teresa Conconi  Francesca Ghezzo  Monica Dettin  Luca Urbani  Claudio Grandi  Diego Guidolin  Beatrice Nico  Carlo Di Bello  Domenico Ribatti  Pier Paolo Parnigotto
Affiliation:1. Department of Pharmaceutical Sciences, School of Pharmacy, University of Padua, via Marzolo 5, 35131 Padua, Italy;2. Department of Chemical Process Engineering, School of Engineering, University of Padua, via Marzolo 9, 35131 Padua, Italy;3. Department of Human Anatomy and Physiology, School of Medicine, University of Padua, via Gabelli 65, 35121 Padua, Italy;4. Department of Human Anatomy and Histology, School of Medicine, University of Bari, Piazza G. Cesare 11, Bari, Italy
Abstract:It is well known that tumor growth is strictly dependent on neo‐vessel formation inside the tumor mass and that cell adhesion is required to allow EC proliferation and migration inside the tumor. In this work, we have evaluated the in vitro and in vivo effects on angiogenesis of some peptides, originally designed to promote cell adhesion on biomaterials, containing RGD motif mediating cell adhesion via integrin receptors [RGD, GRGDSPK, and (GRGDSP)4K] or the heparin‐binding sequence of human vitronectin that interacts with HSPGs [HVP(351–359)]. Cell adhesion, proliferation, migration, and capillary‐like tube formation in Matrigel were determined on HUVECs, whereas the effects on in vivo angiogenesis were evaluated using the CAM assay. (GRGDSP)4K linear sequence inhibited cell adhesion, decreased cell proliferation, migration and morphogenesis in Matrigel, and induced anti‐angiogenic responses on CAM at higher degree than that determined after incubation with RGD or GRGDSPK. Moreover, it counteracted both in vitro and in vivo the pro‐angiogenic effects induced by the Fibroblast growth factor (FGF‐2). On the other hand, HVP was not able to affect cell adhesion and appeared less effective than (GRGDSP)4K. Our data indicate that the activity of RGD‐containing peptides is related to their adhesive properties, and their effects are modulated by the number of cell adhesion motifs and the aminoacidic residues next to these sequences. The anti‐angiogenic properties of (GRGDSP)4K seem to depend on its interaction with integrins, whereas the effects of HVP may be partially due to an impairment of HSPGs/FGF‐2. Copyright © 2010 European Peptide Society and John Wiley & Sons, Ltd.
Keywords:angiogenesis  cell adhesion  RGD  heparin‐binding motif  FGF‐2
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