Cancer Cell Biology

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The YSNSG cyclopeptide derived from tumstatin inhibits tumor angiogenesis by down-regulating endothelial cell migration

  1. Jessica Thevenard1,
  2. Laurent Ramont1,
  3. Jérome Devy1,
  4. Bertrand Brassart1,
  5. Aurélie Dupont-Deshorgue1,
  6. Nicolas Floquet1,†,
  7. Laurence Schneider1,
  8. Farid Ouchani1,
  9. Christine Terryn2,
  10. François-Xavier Maquart1,
  11. Jean-Claude Monboisse1,
  12. Sylvie Brassart-Pasco1,‡,*

Article first published online: 23 JUN 2009

DOI: 10.1002/ijc.24688

Issue

International Journal of Cancer

International Journal of Cancer

Volume 126, Issue 5, pages 1055–1066, 1 March 2010

Additional Information

How to Cite

Thevenard, J., Ramont, L., Devy, J., Brassart, B., Dupont-Deshorgue, A., Floquet, N., Schneider, L., Ouchani, F., Terryn, C., Maquart, F.-X., Monboisse, J.-C. and Brassart-Pasco, S. (2010), The YSNSG cyclopeptide derived from tumstatin inhibits tumor angiogenesis by down-regulating endothelial cell migration. Int. J. Cancer, 126: 1055–1066. doi: 10.1002/ijc.24688

Author Information

  1. 1

    CNRS UMR 6237, Université de Reims Champagne-Ardenne, CHU de Reims, Reims, France

  2. 2

    IFR 53, Plateforme Imagerie Cellulaire et Tissulaire, Université de Reims Champagne-Ardenne, Reims, France

  1. Institut des BioMolécules Max Mousseron, CNRS UMR 5247, Université de Montpellier, Montpellier, France

  1. Fax: 33-32-691-8055

*Laboratoire de Biochimie Médicale et de Biologie Moléculaire CNRS UMR 6237, U.F.R. Médecine, 51 Rue Cognacq Jay, REIMS Cedex 51095, France

Publication History

  1. Issue published online: 27 DEC 2009
  2. Article first published online: 23 JUN 2009
  3. Accepted manuscript online: 23 JUN 2009 12:00AM EST
  4. Manuscript Accepted: 12 JUN 2009
  5. Manuscript Received: 11 AUG 2008

Funded by

  • Centre National de la Recherche Scientifique. Grant Number: (UMR 6237)
  • University of Reims Champagne-Ardenne
  • Association pour la Recherche sur le Cancer
  • Ligue Nationale Contre le Cancer (Comités de l'Aisne et de la Haute-Marne)
  • Canceropole Grand Est (ACI 2004, InCa)

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Keywords:

  • tumstatin;
  • angiogenesis;
  • migration;
  • matrix metalloproteinases;
  • plasminogen activation system

Abstract

We previously demonstrated that the CNYYSNS peptide derived from tumstatin inhibited in vivo tumor progression. The YSNS motif formed a β-turn crucial for biological activity. More recently, a YSNSG cyclopeptide with a constrained β-turn on the YSNS residues was designed. Intraperitoneal administration of the YSNSG cyclopeptide inhibited in vivo melanoma progression more efficiently than the native linear peptide. In the present article, we showed that the YSNSG cyclopeptide also triggered an inhibition of in vivo tumor neovascularization and we further analyzed its in vitroantiangiogenic effect. The YSNSG cyclopeptide did not alter endothelial cell proliferation but inhibited cell migration by 83% in an in vitro wound healing model. The inhibition was mediated by a decrease in active MT1-MMP at the migration front as well as a decrease in u-PA and u-PAR expression. The cyclopeptide also altered β1-integrin distribution in endothelial cell lamellipodia, induced a strong decrease in the phosphorylated focal adhesion kinase (p125FAK), disorganized F-actin stress fibers and decreased the number of lamellipodia, resulting in a non migratory phenotype. Our results confirm the YSNSG cyclopeptide as a potent antitumor agent, through both the inhibition of invasive properties of tumor cells and the antiangiogenic activity.

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