Literature DB >> 26558781

Mir-21-Sox2 Axis Delineates Glioblastoma Subtypes with Prognostic Impact.

Pratheesh Sathyan1, Pascal O Zinn2, Anantha L Marisetty2, Bin Liu2, Mohamed Mostafa Kamal2, Sanjay K Singh2, Pierre Bady3, Li Lu2, Khalida M Wani4, Bethany L Veo2, Joy Gumin5, Dina Hamada Kassem2, Frederick Robinson2, Connie Weng2, Veerabhadran Baladandayuthapani6, Dima Suki7, Howard Colman8, Krishna P Bhat9, Erik P Sulman10, Ken Aldape11, Rivka R Colen12, Roel G W Verhaak13, Zhimin Lu14, Gregory N Fuller15, Suyun Huang7, Frederick F Lang7, Raymond Sawaya7, Monika Hegi3, Sadhan Majumder16.   

Abstract

Glioblastoma (GBM) is the most aggressive human brain tumor. Although several molecular subtypes of GBM are recognized, a robust molecular prognostic marker has yet to be identified. Here, we report that the stemness regulator Sox2 is a new, clinically important target of microRNA-21 (miR-21) in GBM, with implications for prognosis. Using the MiR-21-Sox2 regulatory axis, approximately half of all GBM tumors present in the Cancer Genome Atlas (TCGA) and in-house patient databases can be mathematically classified into high miR-21/low Sox2 (Class A) or low miR-21/high Sox2 (Class B) subtypes. This classification reflects phenotypically and molecularly distinct characteristics and is not captured by existing classifications. Supporting the distinct nature of the subtypes, gene set enrichment analysis of the TCGA dataset predicted that Class A and Class B tumors were significantly involved in immune/inflammatory response and in chromosome organization and nervous system development, respectively. Patients with Class B tumors had longer overall survival than those with Class A tumors. Analysis of both databases indicated that the Class A/Class B classification is a better predictor of patient survival than currently used parameters. Further, manipulation of MiR-21-Sox2 levels in orthotopic mouse models supported the longer survival of the Class B subtype. The MiR-21-Sox2 association was also found in mouse neural stem cells and in the mouse brain at different developmental stages, suggesting a role in normal development. Therefore, this mechanism-based classification suggests the presence of two distinct populations of GBM patients with distinguishable phenotypic characteristics and clinical outcomes. SIGNIFICANCE STATEMENT: Molecular profiling-based classification of glioblastoma (GBM) into four subtypes has substantially increased our understanding of the biology of the disease and has pointed to the heterogeneous nature of GBM. However, this classification is not mechanism based and its prognostic value is limited. Here, we identify a new mechanism in GBM (the miR-21-Sox2 axis) that can classify ∼50% of patients into two subtypes with distinct molecular, radiological, and pathological characteristics. Importantly, this classification can predict patient survival better than the currently used parameters. Further, analysis of the miR-21-Sox2 relationship in mouse neural stem cells and in the mouse brain at different developmental stages indicates that miR-21 and Sox2 are predominantly expressed in mutually exclusive patterns, suggesting a role in normal neural development.
Copyright © 2015 the authors 0270-6474/15/3515098-16$15.00/0.

Entities:  

Keywords:  SOX2; glioblastoma; microRNA-21; neuronal subtype

Mesh:

Substances:

Year:  2015        PMID: 26558781      PMCID: PMC4642241          DOI: 10.1523/JNEUROSCI.1265-15.2015

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


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