4.6 Article

Glioblastoma with an oligodendroglioma component: distinct clinical behavior, genetic alterations, and outcome

Journal

NEURO-ONCOLOGY
Volume 14, Issue 4, Pages 518-525

Publisher

OXFORD UNIV PRESS INC
DOI: 10.1093/neuonc/nor232

Keywords

glioblastoma with an oligodendroglioma component; IDH1 mutation; LOH 1p 19q; prognostic; therapeutic response

Funding

  1. National Key Project of Science and Technology Supporting Programs of China [2007BAI05B08]
  2. National Basic Research Program of China (973 Program) [2010CB529406, 2011CB707804]

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Glioblastomas (GBMs) containing foci that resemble oligodendroglioma are defined as GBM with oligodendroglioma component (GBMO). However, whether GBMO is a distinct clinicopathological variant of GBM or merely represents a divergent pattern of differentiation remains controversial. We investigated 219 consecutive primary GBMs, of which 40 (18.3%) were confirmed as GBMOs. The clinical features and genetic profiles of the GBMOs were analyzed and compared with the conventional GBMs. The GBMO group showed more frequent tumor-related seizures (P = .027), higher frequency of IDH1 mutation (31% vs. <5%, P = .015), lower MGMT expression (P = .016), and longer survival (19.0 vs. 13.2 months; P = .022). In multivariate Cox regression analyses, presence of an oligodendroglioma component was predictive of longer survival (P = .001), but the extent of the oligodendroglial component appeared not to be linked to prognosis (P = .664). The codeletions of 1p/19q, somewhat surprisingly, were infrequent (<5%) in both GBMO and conventional GBM. In addition, the response to aggressive therapy differed: the GBMO group had no survival advantage associated with aggressive treatment protocols, whereas a clear treatment effect was observed in the conventional GBM group. Collectively, the clinical behavior and genetic alterations of GBMO thus differs from those of conventional GBM. Presence of an oligodendroglial component may therefore be a useful classification and stratification variable in therapeutic trials of GBMs.

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