@article {152931, title = {A developmental taxonomy of glioblastoma defined and maintained by MicroRNAs.}, journal = {Cancer Res}, volume = {71}, number = {9}, year = {2011}, month = {2011 May 1}, pages = {3387-99}, abstract = { mRNA expression profiling has suggested the existence of multiple glioblastoma subclasses, but their number and characteristics vary among studies and the etiology underlying their development is unclear. In this study, we analyzed 261 microRNA expression profiles from The Cancer Genome Atlas (TCGA), identifying five clinically and genetically distinct subclasses of glioblastoma that each related to a different neural precursor cell type. These microRNA-based glioblastoma subclasses displayed microRNA and mRNA expression signatures resembling those of radial glia, oligoneuronal precursors, neuronal precursors, neuroepithelial/neural crest precursors, or astrocyte precursors. Each subclass was determined to be genetically distinct, based on the significant differences they displayed in terms of patient race, age, treatment response, and survival. We also identified several microRNAs as potent regulators of subclass-specific gene expression networks in glioblastoma. Foremost among these is miR-9, which suppresses mesenchymal differentiation in glioblastoma by downregulating expression of JAK kinases and inhibiting activation of STAT3. Our findings suggest that microRNAs are important determinants of glioblastoma subclasses through their ability to regulate developmental growth and differentiation programs in several transformed neural precursor cell types. Taken together, our results define developmental microRNA expression signatures that both characterize and contribute to the phenotypic diversity of glioblastoma subclasses, thereby providing an expanded framework for understanding the pathogenesis of glioblastoma in a human neurodevelopmental context. }, keywords = {Brain Neoplasms, DNA Modification Methylases, DNA Repair Enzymes, Gene Dosage, Gene Expression Profiling, Glioblastoma, Humans, MicroRNAs, Mutation, Neoplastic Stem Cells, Promoter Regions, Genetic, RNA, Messenger, Tumor Suppressor Proteins}, issn = {1538-7445}, doi = {10.1158/0008-5472.CAN-10-4117}, author = {Kim, Tae-Min and Huang, Wei and Park, Richard and Park, Peter J** and Johnson, Mark D**} }