<i>SOX2</i> Silencing in Glioblastoma Tumor-Initiating Cells Causes Stop of Proliferation and Loss of Tumorigenicity

Rosaria Gangemi; Fabrizio Griffero; Daniela Marubbi; Marzia Perera; Maria Capra; Paolo Malatesta; Gian Luigi Ravetti; Gianluigi Zona; Antonio Daga; Giorgio Corte

doi:10.1634/stemcells.2008-0493

<i>SOX2</i> Silencing in Glioblastoma Tumor-Initiating Cells Causes Stop of Proliferation and Loss of Tumorigenicity

Rosaria Gangemi(Alleanza Contro il Cancro), Fabrizio Griffero(Alleanza Contro il Cancro), Daniela Marubbi(Alleanza Contro il Cancro), Marzia Perera(Alleanza Contro il Cancro), Maria Capra(Alleanza Contro il Cancro), Paolo Malatesta(Alleanza Contro il Cancro), Gian Luigi Ravetti(Ospedale Policlinico San Martino), Gianluigi Zona(University of Genoa), Antonio Daga(Alleanza Contro il Cancro), Giorgio Corte(Alleanza Contro il Cancro)

Stem Cells

October 24, 2008

10.1634/stemcells.2008-0493

Cited by 572Open Access

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Abstract

Glioblastoma, the most aggressive cerebral tumor, is invariably lethal. Glioblastoma cells express several genes typical of normal neural stem cells. One of them, SOX2, is a master gene involved in sustaining self-renewal of several stem cells, in particular neural stem cells. To investigate its role in the aberrant growth of glioblastoma, we silenced SOX2 in freshly derived glioblastoma tumor-initiating cells (TICs). Our results indicate that SOX2 silenced glioblastoma TICs, despite the many mutations they have accumulated, stop proliferating and lose tumorigenicity in immunodeficient mice. SOX2 is then also fundamental for maintenance of the self-renewal capacity of neural stem cells when they have acquired cancer properties. SOX2, or its immediate downstream effectors, would then be an ideal target for glioblastoma therapy.

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