par Thijssen, Victor L;Barkan, Batya;Shoji, Hiroki;Aries, Ingrid M;Mathieu, Véronique 
;Deltour, Louise;Hackeng, Tilman M;Kiss, Robert ;Kloog, Yoel;Poirier, Françoise;Griffioen, Arjan W
Référence Cancer research, 70, 15, page (6216-6224)
Publication Publié, 2010-08
;Deltour, Louise;Hackeng, Tilman M;Kiss, Robert ;Kloog, Yoel;Poirier, Françoise;Griffioen, Arjan WRéférence Cancer research, 70, 15, page (6216-6224)
Publication Publié, 2010-08
Article révisé par les pairs
| Résumé : | Tumor angiogenesis is a key event in cancer progression. Here, we report that tumors can stimulate tumor angiogenesis by secretion of galectin-1. Tumor growth and tumor angiogenesis of different tumor models are hampered in galectin-1-null (gal-1(-/-)) mice. However, tumor angiogenesis is less affected when tumor cells express and secrete high levels of galectin-1. Furthermore, tumor endothelial cells in gal-1(-/-) mice take up galectin-1 that is secreted by tumor cells. Uptake of galectin-1 by cultured endothelial cells specifically promotes H-Ras signaling to the Raf/mitogen-activated protein kinase/extracellular signal-regulated kinase (Erk) kinase (Mek)/Erk cascade and stimulates endothelial cell proliferation and migration. Moreover, the activation can be blocked by galectin-1 inhibition as evidenced by hampered membrane translocation of H-Ras.GTP and impaired Raf/Mek/Erk phosphorylation after treatment with the galectin-1-targeting angiogenesis inhibitor anginex. Altogether, these data identify galectin-1 as a proangiogenic factor. These findings have direct implications for current efforts on galectin-1-targeted cancer therapies. |
