Bmi1 and cell of origin determinants of brain tumor phenotype
- PMID: 17936553
- DOI: 10.1016/j.ccr.2007.10.003
Bmi1 and cell of origin determinants of brain tumor phenotype
Abstract
Glioblastomas frequently express oncogenic EGFR and loss of the Ink4a/Arf locus. Bmi1, a positive regulator of stem cell self renewal, may be critical to drive brain tumor growth. In this issue of Cancer Cell, Bruggeman and colleagues suggest that brain tumors with these molecular alterations can be initiated in both neural precursor and differentiated cell compartments in the absence of Bmi1; however, tumorigenicity is reduced, and tumors contain fewer precursor cells. Surprisingly, tumors appear less malignant when initiated in precursor cells. Bmi1-deficient tumors also had fewer neuronal lineage cells, suggesting a role for Bmi1 in determination of cell lineage and tumor phenotype.
Comment on
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Bmi1 controls tumor development in an Ink4a/Arf-independent manner in a mouse model for glioma.Cancer Cell. 2007 Oct;12(4):328-41. doi: 10.1016/j.ccr.2007.08.032. Cancer Cell. 2007. PMID: 17936558
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