Targeting self-renewal in high-grade brain tumors leads to loss of brain tumor stem cells and prolonged survival.

نویسندگان

  • Zhe Zhu
  • Muhammad Amir Khan
  • Markus Weiler
  • Jonas Blaes
  • Leonie Jestaedt
  • Madeleine Geibert
  • Peng Zou
  • Jan Gronych
  • Olga Bernhardt
  • Andrey Korshunov
  • Verena Bugner
  • Peter Lichter
  • Bernhard Radlwimmer
  • Sabine Heiland
  • Martin Bendszus
  • Wolfgang Wick
  • Hai-Kun Liu
چکیده

Cancer stem cells (CSCs) have been suggested as potential therapeutic targets for treating malignant tumors, but the in vivo supporting evidence is still missing. Using a GFP reporter driven by the promoter of the nuclear receptor tailless (Tlx), we demonstrate that Tlx(+) cells in primary brain tumors are mostly quiescent. Lineage tracing demonstrates that single Tlx(+) cells can self-renew and generate Tlx(-) tumor cells in primary tumors, suggesting that they are brain tumor stem cells (BTSCs). After introducing a BTSC-specific knock-out of the Tlx gene in primary mouse tumors, we observed a loss of self-renewal of BTSCs and prolongation of animal survival, accompanied by induction of essential signaling pathways mediating cell-cycle arrest, cell death, and neural differentiation. Our study demonstrates the feasibility of targeting glioblastomas and indicates the suitability of BTSCs as therapeutic targets, thereby supporting the CSC hypothesis.

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عنوان ژورنال:
  • Cell stem cell

دوره 15 2  شماره 

صفحات  -

تاریخ انتشار 2014