Identification of a CpG Island Methylator Phenotype that Defines a Distinct Subgroup of Glioma

Houtan Noushmehr,Daniel J. Weisenberger,Kristin Diefes,Heidi S. Phillips,Kanan Pujara,Benjamin P. Berman,Fei Pan,Christopher E. Pelloski,Erik Philip Sulman,Krishna P Bhat,Roeland Verhaak,Katherine A. Hoadley,D. Neil Hayes,Charles M. Perou,Heather K. Schmidt,Li Ding,Richard K. Wilson,David Van Den Berg,Hui Shen,Henrik Bengtsson,Pierre Neuvial,Leslie Cope,Jonathan D. Buckley,James G. Herman,Stephen B. Baylin,Peter W. Laird,Kenneth Aldape

Identification of a CpG Island Methylator Phenotype that Defines a Distinct Subgroup of Glioma

2010

Summary We have profiled promoter DNA methylation alterations in 272 glioblastoma tumors in the context of The Cancer Genome Atlas (TCGA). We found that a distinct subset of samples displays concerted hypermethylation at a large number of loci, indicating the existence of a glioma-CpG island methylator phenotype (G-CIMP). We validated G-CIMP in a set of non-TCGA glioblastomas and low-grade gliomas. G-CIMP tumors belong to the proneural subgroup, are more prevalent among lower-grade gliomas, display distinct copy-number alterations, and are tightly associated with IDH1 somatic mutations. Patients with G-CIMP tumors are younger at the time of diagnosis and experience significantly improved outcome. These findings identify G-CIMP as a distinct subset of human gliomas on molecular and clinical grounds.

Keywords:

Methylation
Cancer research
CpG site
Glioma
DNA methylation
Germline mutation
IDH1
Phenotype
CpG Island Methylator Phenotype
Biology
Genetics
Mutation

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