Cell Reports (Jan 2017)

Glioblastoma Cell Malignancy and Drug Sensitivity Are Affected by the Cell of Origin

  • Yiwen Jiang,
  • Voichita Dana Marinescu,
  • Yuan Xie,
  • Malin Jarvius,
  • Naga Prathyusha Maturi,
  • Caroline Haglund,
  • Sara Olofsson,
  • Nanna Lindberg,
  • Tommie Olofsson,
  • Caroline Leijonmarck,
  • Göran Hesselager,
  • Irina Alafuzoff,
  • Mårten Fryknäs,
  • Rolf Larsson,
  • Sven Nelander,
  • Lene Uhrbom

DOI
https://doi.org/10.1016/j.celrep.2017.01.003
Journal volume & issue
Vol. 18, no. 4
pp. 977 – 990

Abstract

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The identity of the glioblastoma (GBM) cell of origin and its contributions to disease progression and treatment response remain largely unknown. We have analyzed how the phenotypic state of the initially transformed cell affects mouse GBM development and essential GBM cell (GC) properties. We find that GBM induced in neural stem-cell-like glial fibrillary acidic protein (GFAP)-expressing cells in the subventricular zone of adult mice shows accelerated tumor development and produces more malignant GCs (mGC1GFAP) that are less resistant to cancer drugs, compared with those originating from more differentiated nestin- (mGC2NES) or 2,′3′-cyclic nucleotide 3′-phosphodiesterase (mGC3CNP)-expressing cells. Transcriptome analysis of mouse GCs identified a 196 mouse cell origin (MCO) gene signature that was used to partition 61 patient-derived GC lines. Human GC lines that clustered with the mGC1GFAP cells were also significantly more self-renewing, tumorigenic, and sensitive to cancer drugs compared with those that clustered with mouse GCs of more differentiated origin.

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