Aspirin inhibits cancer stem cells properties and growth of glioblastoma multiforme through Rb1 pathway modulation.
Date
2019-01-01Author
Pozzoli, GiacomoMarei, Hany E
Althani, Asma
Boninsegna, Alma
Casalbore, Patrizia
Marlier, Lionel N J L
Lanzilli, Giulia
Zonfrillo, Manuela
Petrucci, Giovanna
Rocca, Bianca
Navarra, Pierluigi
Sgambato, Alessandro
Cenciarelli, Carlo
...show more authors ...show less authors
Metadata
Show full item recordAbstract
Several clinical studies indicated that the daily use of aspirin or acetylsalicylic acid reduces the cancer risk via cyclooxygenases (Cox-1 and Cox-2) inhibition. In addition, aspirin-induced Cox-dependent and -independent antitumor effects have also been described. Here we report, for the first time, that aspirin treatment of human glioblastoma cancer (GBM) stem cells, a small population responsible for tumor progression and recurrence, is associated with reduced cell proliferation and motility. Aspirin did not interfere with cell viability but induced cell-cycle arrest. Exogenous prostaglandin E significantly increased cell proliferation but did not abrogate the aspirin-mediated growth inhibition, suggesting a Cox-independent mechanism. These effects appear to be mediated by the increase of p21 and p27 , associated with a reduction of Cyclin D1 and Rb1 protein phosphorylation, and involve the downregulation of key molecules responsible for tumor development, that is, Notch1, Sox2, Stat3, and Survivin. Our results support a possible role of aspirin as adjunctive therapy in the clinical management of GBM patients.
Collections
- Biomedical Research Center Research [740 items ]