Ephrin-B3 supports glioblastoma growth by inhibiting apoptosis induced by the dependence receptor EphA4

نویسندگان

  • Amélie Royet
  • Laura Broutier
  • Marie-May Coissieux
  • Céline Malleval
  • Nicolas Gadot
  • Denis Maillet
  • Lise Gratadou-Hupon
  • Agnès Bernet
  • Pascale Nony
  • Isabelle Treilleux
  • Jérôme Honnorat
  • Daniel Liebl
  • Laurent Pelletier
  • François Berger
  • David Meyronet
  • Marie Castets
  • Patrick Mehlen
چکیده

EphA4, an Ephrins tyrosine kinase receptor, behaves as a dependence receptor (DR) by triggering cell apoptosis in the absence of its ligand Ephrin-B3. DRs act as conditional tumor suppressors, engaging cell death based on ligand availability; this mechanism is bypassed by overexpression of DRs ligands in some aggressive cancers. The pair EphA4/Ephrin-B3 favors survival of neuronal progenitors of the brain subventricular zone, an area where glioblastoma multiform (GBM) are thought to originate. Here, we report that Ephrin-B3 is highly expressed in human biopsies and that it inhibits EphA4 pro-apoptotic activity in tumor cells. Angiogenesis is directly correlated with GBM aggressiveness and we demonstrate that Ephrin-B3 also supports the survival of endothelial cells in vitro and in vivo. Lastly, silencing of Ephrin-B3 decreases tumor vascularization and growth in a xenograft mice model. Interference with EphA4/Ephrin-B3 interaction could then be envisaged as a relevant strategy to slow GBM growth by enhancing EphA4-induced cell death.

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عنوان ژورنال:

دوره 8  شماره 

صفحات  -

تاریخ انتشار 2017