Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.

Age is a powerful predictor of survival in glioblastoma multiforme (GBM) yet the biological basis for the difference in clinical outcome is mostly unknown. Discovering genes and pathways that would explain age-specific survival difference could generate opportunities for novel therapeutics for GBM....

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Published in:PLoS ONE
Main Authors: Serdar Bozdag, Aiguo Li, Gregory Riddick, Yuri Kotliarov, Mehmet Baysan, Fabio M Iwamoto, Margaret C Cam, Svetlana Kotliarova, Howard A Fine
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Online Access:http://europepmc.org/articles/PMC3639162?pdf=render
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author Serdar Bozdag
Aiguo Li
Gregory Riddick
Yuri Kotliarov
Mehmet Baysan
Fabio M Iwamoto
Margaret C Cam
Svetlana Kotliarova
Howard A Fine
author_facet Serdar Bozdag
Aiguo Li
Gregory Riddick
Yuri Kotliarov
Mehmet Baysan
Fabio M Iwamoto
Margaret C Cam
Svetlana Kotliarova
Howard A Fine
author_sort Serdar Bozdag
collection DOAJ
container_title PLoS ONE
description Age is a powerful predictor of survival in glioblastoma multiforme (GBM) yet the biological basis for the difference in clinical outcome is mostly unknown. Discovering genes and pathways that would explain age-specific survival difference could generate opportunities for novel therapeutics for GBM. Here we have integrated gene expression, exon expression, microRNA expression, copy number alteration, SNP, whole exome sequence, and DNA methylation data sets of a cohort of GBM patients in The Cancer Genome Atlas (TCGA) project to discover age-specific signatures at the transcriptional, genetic, and epigenetic levels and validated our findings on the REMBRANDT data set. We found major age-specific signatures at all levels including age-specific hypermethylation in polycomb group protein target genes and the upregulation of angiogenesis-related genes in older GBMs. These age-specific differences in GBM, which are independent of molecular subtypes, may in part explain the preferential effects of anti-angiogenic agents in older GBM and pave the way to a better understanding of the unique biology and clinical behavior of older versus younger GBMs.
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spelling doaj-art-fd413d4cfa814ca8a9bba9617c604f492025-08-19T21:16:20ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0184e6298210.1371/journal.pone.0062982Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.Serdar BozdagAiguo LiGregory RiddickYuri KotliarovMehmet BaysanFabio M IwamotoMargaret C CamSvetlana KotliarovaHoward A FineAge is a powerful predictor of survival in glioblastoma multiforme (GBM) yet the biological basis for the difference in clinical outcome is mostly unknown. Discovering genes and pathways that would explain age-specific survival difference could generate opportunities for novel therapeutics for GBM. Here we have integrated gene expression, exon expression, microRNA expression, copy number alteration, SNP, whole exome sequence, and DNA methylation data sets of a cohort of GBM patients in The Cancer Genome Atlas (TCGA) project to discover age-specific signatures at the transcriptional, genetic, and epigenetic levels and validated our findings on the REMBRANDT data set. We found major age-specific signatures at all levels including age-specific hypermethylation in polycomb group protein target genes and the upregulation of angiogenesis-related genes in older GBMs. These age-specific differences in GBM, which are independent of molecular subtypes, may in part explain the preferential effects of anti-angiogenic agents in older GBM and pave the way to a better understanding of the unique biology and clinical behavior of older versus younger GBMs.http://europepmc.org/articles/PMC3639162?pdf=render
spellingShingle Serdar Bozdag
Aiguo Li
Gregory Riddick
Yuri Kotliarov
Mehmet Baysan
Fabio M Iwamoto
Margaret C Cam
Svetlana Kotliarova
Howard A Fine
Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.
title Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.
title_full Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.
title_fullStr Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.
title_full_unstemmed Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.
title_short Age-specific signatures of glioblastoma at the genomic, genetic, and epigenetic levels.
title_sort age specific signatures of glioblastoma at the genomic genetic and epigenetic levels
url http://europepmc.org/articles/PMC3639162?pdf=render
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