Molecular Profiling Identifies Prognostic Subgroups of Pediatric Glioblastoma and Shows Increased YB-1 Expression in Tumors

Damien Faury , André Nantel , Sandra E. Dunn , Damien Faury , André Nantel , Sandra E. Dunn , Marie-Christine Guiot , Takrima Haque , Péter Hauser , Miklós Garami , László Bognár , Zoltán Hanzély , Paweł P. Liberski , Enrique López‐Aguilar , Elvis Terci Valera , Luíz Gonzaga Tone , Anne-Sophie Carret , Rolando F. Del Maestro , Martin Gleave , J.L. Martínez Montes , Torsten Pietsch , Stephen Albrecht , Nada Jabado
2007 Journal of Clinical Oncology 216 citations

Abstract

Purpose Pediatric glioblastoma (pGBM) is a rare, but devastating brain tumor. In contrast to GBM in adults (aGBM), little is known about the mechanisms underlying its development. Our aim is to gain insight into the molecular pathways of pGBM. Materials and Methods Thirty-two pGBM and seven aGBM samples were investigated using biochemical and transcriptional profiling. Ras and Akt pathway activation was assessed through the phosphorylation of downstream effectors, and gene expression profiles were generated using the University Health Network Human 19K cDNA arrays. Results were validated using real-time polymerase chain reaction and immunohistochemistry and compared with existing data sets on aGBM. Results There are at least two subsets of pGBM. One subset, associated with Ras and Akt pathway activation, has very poor prognosis and exhibits increased expression of genes related to proliferation and to a neural stem-cell phenotype, similar to findings in aggressive aGBM. This subset was still molecularly distinguishable from aGBM after unsupervised and supervised analysis of expression profiles. A second subset, with better prognosis, is not associated with activation of Akt and Ras pathways, may originate from astroglial progenitors, and does not express gene signatures and markers shown to be associated with long-term survival in aGBM. Both subsets of pGBM show overexpression of Y-box-protein-1 that may help drive oncogenesis in this tumor. Conclusion Our work, the first study of gene expression profiles in pGBM, provides valuable insight into active pathways and targets in a cancer with minimal survival, and suggests that these tumors cannot be understood exclusively through studies of aGBM.

Keywords

Gene expression profilingCarcinogenesisCancer researchProtein kinase BPhenotypeGene expressionGeneMedicineImmunohistochemistryBiologySignal transductionPathologyGenetics

MeSH Terms

AdolescentAdultAgedAged80 and overApoptosisBrain NeoplasmsChildChildPreschoolDNA-Binding ProteinsErbB ReceptorsFemaleGene Expression ProfilingGlioblastomaHumansInfantMaleMiddle AgedNuclear ProteinsPhosphorylationPrognosisProto-Oncogene Proteins c-aktProto-Oncogene Proteins p21(ras)Signal TransductionY-Box-Binding Protein 1

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Publication Info

Year
2007
Type
article
Volume
25
Issue
10
Pages
1196-1208
Citations
216
Access
Closed

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Damien Faury, André Nantel, Sandra E. Dunn et al. (2007). Molecular Profiling Identifies Prognostic Subgroups of Pediatric Glioblastoma and Shows Increased YB-1 Expression in Tumors. Journal of Clinical Oncology , 25 (10) , 1196-1208. https://doi.org/10.1200/jco.2006.07.8626

Identifiers

DOI
10.1200/jco.2006.07.8626
PMID
17401009

Data Quality

Data completeness: 86%