EMBO Molecular Medicine (Apr 2016)

MET inhibition overcomes radiation resistance of glioblastoma stem‐like cells

  • Francesca De Bacco,
  • Antonio D'Ambrosio,
  • Elena Casanova,
  • Francesca Orzan,
  • Roberta Neggia,
  • Raffaella Albano,
  • Federica Verginelli,
  • Manuela Cominelli,
  • Pietro L Poliani,
  • Paolo Luraghi,
  • Gigliola Reato,
  • Serena Pellegatta,
  • Gaetano Finocchiaro,
  • Timothy Perera,
  • Elisabetta Garibaldi,
  • Pietro Gabriele,
  • Paolo M Comoglio,
  • Carla Boccaccio

DOI
https://doi.org/10.15252/emmm.201505890
Journal volume & issue
Vol. 8, no. 5
pp. 550 – 568

Abstract

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Abstract Glioblastoma (GBM) contains stem‐like cells (GSCs) known to be resistant to ionizing radiation and thus responsible for therapeutic failure and rapidly lethal tumor recurrence. It is known that GSC radioresistance relies on efficient activation of the DNA damage response, but the mechanisms linking this response with the stem status are still unclear. Here, we show that the MET receptor kinase, a functional marker of GSCs, is specifically expressed in a subset of radioresistant GSCs and overexpressed in human GBM recurring after radiotherapy. We elucidate that MET promotes GSC radioresistance through a novel mechanism, relying on AKT activity and leading to (i) sustained activation of Aurora kinase A, ATM kinase, and the downstream effectors of DNA repair, and (ii) phosphorylation and cytoplasmic retention of p21, which is associated with anti‐apoptotic functions. We show that MET pharmacological inhibition causes DNA damage accumulation in irradiated GSCs and their depletion in vitro and in GBMs generated by GSC xenotransplantation. Preclinical evidence is thus provided that MET inhibitors can radiosensitize tumors and convert GSC‐positive selection, induced by radiotherapy, into GSC eradication.

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