par Lin, Shuheng 
;Negulescu, Ana;Bulusu, Sirisha;Gibert, Benjamin;Delcros, Jean-Guy;Ducarouge, Benjamin;Rama, Nicolas;Gadot, Nicolas;Treilleux, Isabelle;Saintigny, Pierre;Meurette, Olivier;Mehlen, Patrick
Référence Nature communications, 8, page (16074)
Publication Publié, 2017-07
;Negulescu, Ana;Bulusu, Sirisha;Gibert, Benjamin;Delcros, Jean-Guy;Ducarouge, Benjamin;Rama, Nicolas;Gadot, Nicolas;Treilleux, Isabelle;Saintigny, Pierre;Meurette, Olivier;Mehlen, PatrickRéférence Nature communications, 8, page (16074)
Publication Publié, 2017-07
Article révisé par les pairs
| Résumé : | Notch signalling is a causal determinant of cancer and efforts have been made to develop targeted therapies to inhibit the so-called canonical pathway. Here we describe an unexpected pro-apoptotic role of Notch3 in regulating tumour angiogenesis independently of the Notch canonical pathway. The Notch3 ligand Jagged-1 is upregulated in a fraction of human cancer and our data support the view that Jagged-1, produced by cancer cells, is inhibiting the apoptosis induced by the aberrant Notch3 expression in tumour vasculature. We thus present Notch3 as a dependence receptor inducing endothelial cell death while this pro-apoptotic activity is blocked by Jagged-1. Along this line, using Notch3 mutant mice, we demonstrate that tumour growth and angiogenesis are increased when Notch3 is silenced in the stroma. Consequently, we show that the well-documented anti-tumour effect mediated by γ-secretase inhibition is at least in part dependent on the apoptosis triggered by Notch3 in endothelial cells. |
