Mutational landscape and clonal architecture in grade II and III gliomas

Suzuki, Hiromichi; Aoki, Kosuke; Chiba, Kenichi; Sato, Yusuke; Shiozawa, Yusuke; Shiraishi, Yuichi; Shimamura, Teppei; Niida, Atsushi; Motomura, Kazuya; Ohka, Fumiharu; Yamamoto, Takashi; Tanahashi, Kuniaki; Ranjit, Melissa; Wakabayashi, Toshihiko; Yoshizato, Tetsuichi; Kataoka, Keisuke; Yoshida, Kenichi; Nagata, Yasunobu; Sato‐Otsubo, Aiko; Tanaka, Hiroko; Sanada, Masashi; Kondo, Yutaka; Nakamura, Hideo; Mizoguchi, Masahiro; Abé, Tatsuya; Muragakı, Yoshihiro; Watanabe, Reiko; Ito, Ichiro; Miyano, Satoru; Natsume, Atsushi; Ogawa, Seishi

doi:10.1038/ng.3273

Cited by 713 publications

(659 citation statements)

References 66 publications

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“…In this GC cohort, 10 of 25 tumors were classified as glioblastoma WHO grade IV by histological analysis while DNA methylation profiling revealed IDH wildtype glioblastoma-associated DNA methylation signatures in 12/23 evaluable tumors. Thus, similar to data recently reported for diffuse and anaplastic astrocytic gliomas [3,16,20,23], 450k beadchip-based DNA methylation profiling may lead to a refined diagnosis of GC tumors. This appears to be both biologically and clinically meaningful, since methylation profiling but not focal histology allowed for the identification of a subgroup of GC with poor prognosis.…”

Section: Discussionsupporting

confidence: 84%

Gliomatosis cerebri: no evidence for a separate brain tumor entity

et al. 2015

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Gliomatosis cerebri (GC) is presently considered a distinct astrocytic glioma entity according to the WHO classification for CNS tumors. It is characterized by widespread, typically bilateral infiltration of the brain involving three or more lobes. Genetic studies of GC have to date been restricted to the analysis of individual glioma-associated genes, which revealed mutations in the isocitrate dehydrogenase 1 (IDH1) and tumor protein p53 (TP53) genes in subsets of patients. Here, we report on a genome-wide analysis of DNA methylation and copy number aberrations in 25 GC patients. Results were compared with those obtained for 105 patients with various types of conventional, i.e., non-GC gliomas including diffuse astrocytic gliomas, oligodendrogliomas and glioblastomas. In addition, we assessed the prognostic role of methylation profiles and recurrent DNA copy number aberrations in GC patients. Our data reveal that the methylation profiles in 23 of the 25 GC tumors corresponded to either IDH mutant astrocytoma (n = 6), IDH mutant and 1p/19q codeleted oligodendroglioma (n = 5), or IDH wild-type glioblastoma including various molecular subgroups, i.e., H3F3A-G34 mutant (n = 1), receptor tyrosine kinase 1 (RTK1, n = 4), receptor tyrosine kinase 2 (classic) (RTK2, n = 2) or mesenchymal (n = 5) glioblastoma groups. Two tumors showed methylation profiles of normal brain tissue due to low tumor cell content. While histological grading (WHO grade IV vs. WHO grade II and III) was not prognostic, the molecular classification as classic/RTK2 or mesenchymal glioblastoma was associated with worse overall survival. Multivariate Cox regression analysis revealed MGMT promoter methylation as a positive prognostic factor. Taken together, DNA-based large-scale molecular profiling indicates that GC comprises a genetically and epigenetically heterogeneous group of diffuse gliomas that carry DNA methylation and copy number profiles closely matching the common molecularly defined glioma entities. These data support the removal of GC as a distinct glioma entity in the upcoming revision of the WHO classification. 3

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Section: Discussionsupporting

confidence: 84%

Gliomatosis cerebri: no evidence for a separate brain tumor entity

et al. 2015

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“…Many potentially confounding factors influence PFS, such as age, extent of removal, histopathologic subtype, and molecular prognostic biomarkers, as well as adjuvant therapy. Because it has become clear that grade II and grade III gliomas exhibit different clinical courses according to their molecular subtypes, 46,47 future studies should incorporate this information when conducting survival analysis on the basis of radiologic findings. Finally, prognostic values of imaging parameters should be analyzed not only with PFS but also with overall survival, which requires further future investigation.…”

Section: Discussionmentioning

confidence: 99%

Diagnostic and Prognostic Value of¹¹C-Methionine PET for Nonenhancing Gliomas

Takano

Kinoshita

Arita³

et al. 2015

AJNR Am J Neuroradiol

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“…Importantly, they have been shown to be clonal mutations in gliomas (11) and are likely to play a role in tumor initiation (12). Using clonal pTERT mutations as the defining characteristic of a GBM tumor cell, we established a convenient PCR-based assay to systematically study clinical and molecular consequences of varying tumor purity.…”

Section: Defining Tumor Puritymentioning

confidence: 99%

Prognostic Relevance of Tumor Purity and Interaction with MGMT Methylation in Glioblastoma

Heuling

Knab

Radke

et al. 2017

Molecular Cancer Research

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Promoter methylation status of O-6-methylguanine-DNA methyltransferase (MGMT), a DNA repair enzyme, is a critical biomarker in glioblastoma (GBM), as treatment decisions and clinical trial inclusion rely on its accurate assessment. However, interpretation of results is complicated by poor interassay reproducibility as well as a weak correlation between methylation status and expression levels of MGMT. This study systematically investigates the influence of tumor purity on tissue subjected to MGMT analysis. A quantitative, allele-specific realtime PCR (qAS-PCR) assay was developed to determine genotype and mutant allele frequency of telomerase promoter (pTERT) mutations as a direct measure of tumor purity. We studied tumor purity, pTERT mutation by Sanger sequencing, MGMT methylation by pyrosequencing, IDH1 mutation status, and clinical parameters in a cohort of high-grade gliomas (n ¼ 97). The qAS-PCR reliably predicted pTERT genotype and tumor purity compared with independent methods. Tumor purity positively and significantly correlated with the extent of methylation in MGMT methylated GBMs. Extent of MGMT methylation differed significantly with respect to pTERT mutation hotspot (C228T vs. C250T). Interestingly, frontal lobe tumors showed greater tumor purity than those in other locations. Above all, tumor purity was identified as an independent prognostic factor in GBM. In conclusion, we determined mutual associations of tumor purity with MGMT methylation and pTERT mutations and found that the extent of MGMT methylation reflects tumor purity. In turn, tumor purity is prognostic in IDH1 wild-type GBM.Implications: Tumor purity is an independent prognostic marker in glioblastoma and is associated with the extent of MGMT methylation. Mol Cancer Res; 15(5); 532-40. Ó2017 AACR.

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Mutational landscape and clonal architecture in grade II and III gliomas

Cited by 713 publications

References 66 publications

Gliomatosis cerebri: no evidence for a separate brain tumor entity

Gliomatosis cerebri: no evidence for a separate brain tumor entity

Diagnostic and Prognostic Value of¹¹C-Methionine PET for Nonenhancing Gliomas

Prognostic Relevance of Tumor Purity and Interaction with MGMT Methylation in Glioblastoma

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Mutational landscape and clonal architecture in grade II and III gliomas

Cited by 713 publications

References 66 publications

Gliomatosis cerebri: no evidence for a separate brain tumor entity

Gliomatosis cerebri: no evidence for a separate brain tumor entity

Diagnostic and Prognostic Value of11C-Methionine PET for Nonenhancing Gliomas

Prognostic Relevance of Tumor Purity and Interaction with MGMT Methylation in Glioblastoma

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Diagnostic and Prognostic Value of¹¹C-Methionine PET for Nonenhancing Gliomas