CB-02MiRNA EXPRESSION PROFILES OF GLIOMA STEM CELLS AND THEIR ASSOCIATION WITH THE MESENCHYMAL TRANSFORMATION OF THESE CELLS

Glioblastoma, are characterized by increased infiltration into the surrounding brain tissue, resistance to therapies, and poor prognosis. A major pathway that contributes to these characteristics is the mesenchymal phenotype of these tumors. A small subpopulation of cancer stem cells (GSCs) have been implicated in the enhanced infiltration, radio-resistance and tumor recurrence. GSCs share some similarities with neural stem cells (NSCs) but exhibit deregulated differentiation ability and enhanced oncogenic potential. Recent studies documented miRNAs as important regulators of GSC functions and of the malignant and stemness features of these cells. In this study we performed miRNA and mRNA integrated analysis of GSCs compared to human NSCs and mesenchymal stromal cells (MSCs) to identify significant miRNA-mRNA signatures associated with the mesenchymal signature of GSCs, using miRNA and mRNA microarray analysis. The comparison of GSCs and NSCs identified 79 miRNAs that were upregulated in GSCs and 21 miRNAs that were increased in MSCs. Twenty six miRNAs were downregulated in GSCs compared to NSCs and 21 miRNAs from this group were further downregulated in MSCs. The comparison of mRNA expression of GSCs and NSCs identified gene clusters associated with glioma cell invasiveness, axonal guidance signaling and TGF-b signaling. miR-504 is one of the miRNAs that was significantly downregulated in GSCs compared to NSCs. The expression of miR-504 was also decreased in mesenchymal GBM and highly increased in the G-CIMP subset of GBM. miR-504 promoted the neural differentiation of GSC, inhibited their self-renewal, migration and the mesenchymal signature of these cells, by downregulating CD44, BCAN, ZRB1 and ZEB2. In conclusion, these results reveal novel miRNAs and potential target networks that play a role in the oncogenic potential and stemness of GSCs and in their mesenchymal transformation and may lead to the identification of therapeutic targets for the eradication of GSCs and the treatment of GBM.