Publication | Closed Access
Enhanced MDR1 Expression and Chemoresistance of Cancer Stem Cells Derived from Glioblastoma
138
Citations
23
References
2009
Year
ImmunologyImmunoeditingCancer BiologyGliomaGbm TherapeuticsCancer StemTumor BiologyNeuro-oncologyEnhanced Mdr1 ExpressionAnti-cancer AgentStem CellsGbm Cs CellsRadiation OncologyCancer ResearchHealth SciencesCancer GeneticsCell BiologyTumor SuppressorMedicine
We established a cancer stem (CS) cell line, U87CS, by means of spheroid culture of U87MG cells derived from glioblastoma (GBM) in neuronal stem cell medium. U87CS cells presented positive immunohistochemical staining for multidrug resistance (MDR)1 and CD133, a marker for a subset of leukemia and GBM CS cells. The gene expression of MDR1 and CD133 on U87CS cells increased by an average of 8.51 and 47.18 times, respectively, compared to the levels on U87MG cells by real-time quantitative RT-PCR. U87CS cells possessed stronger drug-resistance to conventional anti-cancer drugs, such as doxorubicin (Dox), etoposide (VP-16), carboplastin, and BCNU than U87MG cells. Double immunofluoresence staining showed co-expression of MDR1 and CD133 on U87CS cells transplanted into nude mice brains. In addition, we identified the crossreactivity of CD133 and MDR1 in a surgical specimen of GBM. Our results suggest that CS cells may be resistant to current chemotherapy and represent a novel target for GBM therapeutics.
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