PLoS ONE (Jan 2008)

Exploratory analysis of the copy number alterations in glioblastoma multiforme.

  • Pablo Freire,
  • Marco Vilela,
  • Helena Deus,
  • Yong-Wan Kim,
  • Dimpy Koul,
  • Howard Colman,
  • Kenneth D Aldape,
  • Oliver Bogler,
  • W K Alfred Yung,
  • Kevin Coombes,
  • Gordon B Mills,
  • Ana T Vasconcelos,
  • Jonas S Almeida

DOI
https://doi.org/10.1371/journal.pone.0004076
Journal volume & issue
Vol. 3, no. 12
p. e4076

Abstract

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The Cancer Genome Atlas project (TCGA) has initiated the analysis of multiple samples of a variety of tumor types, starting with glioblastoma multiforme. The analytical methods encompass genomic and transcriptomic information, as well as demographic and clinical data about the sample donors. The data create the opportunity for a systematic screening of the components of the molecular machinery for features that may be associated with tumor formation. The wealth of existing mechanistic information about cancer cell biology provides a natural reference for the exploratory exercise.Glioblastoma multiforme DNA copy number data was generated by The Cancer Genome Atlas project for 167 patients using 227 aCGH experiments, and was analyzed to build a catalog of aberrant regions. Genome screening was performed using an information theory approach in order to quantify aberration as a deviation from a centrality without the bias of untested assumptions about its parametric nature. A novel Cancer Genome Browser software application was developed and is made public to provide a user-friendly graphical interface in which the reported results can be reproduced. The application source code and stand alone executable are available at (http://code.google.com/p/cancergenome) and (http://bioinformaticstation.org), respectively.The most important known copy number alterations for glioblastoma were correctly recovered using entropy as a measure of aberration. Additional alterations were identified in different pathways, such as cell proliferation, cell junctions and neural development. Moreover, novel candidates for oncogenes and tumor suppressors were also detected. A detailed map of aberrant regions is provided.