| Literature DB >> 29687258 |
Mitsuaki Shirahata1,2, Takahiro Ono1,3, Damian Stichel4, Daniel Schrimpf1,4, David E Reuss1,4, Felix Sahm1,4, Christian Koelsche1,4, Annika Wefers1,4, Annekathrin Reinhardt1,4, Kristin Huang1,4, Philipp Sievers1,4, Hiroaki Shimizu3, Hiroshi Nanjo5,6, Yusuke Kobayashi2, Yohei Miyake2, Tomonari Suzuki2, Jun-Ichi Adachi2, Kazuhiko Mishima2, Atsushi Sasaki7, Ryo Nishikawa2, Melanie Bewerunge-Hudler8, Marina Ryzhova9, Oksana Absalyamova9, Andrey Golanov9, Peter Sinn10, Michael Platten11, Christine Jungk12, Frank Winkler13,14, Antje Wick13,14, Daniel Hänggi15, Andreas Unterberg12, Stefan M Pfister16,17,18, David T W Jones16,17, Martin van den Bent19, Monika Hegi20,21, Pim French19, Brigitta G Baumert22, Roger Stupp23, Thierry Gorlia24, Michael Weller25, David Capper1,26,27,28, Andrey Korshunov1,4, Christel Herold-Mende12, Wolfgang Wick13,14, David N Louis29, Andreas von Deimling30,31,32.
Abstract
According to the 2016 World Health Organization Classification of Tumors of the Central Nervous System (2016 CNS WHO), IDH-mutant astrocytic gliomas comprised WHO grade II diffuse astrocytoma, IDH-mutant (AIIIDHmut), WHO grade III anaplastic astrocytoma, IDH-mutant (AAIIIIDHmut), and WHO grade IV glioblastoma, IDH-mutant (GBMIDHmut). Notably, IDH gene status has been made the major criterion for classification while the manner of grading has remained unchanged: it is based on histological criteria that arose from studies which antedated knowledge of the importance of IDH status in diffuse astrocytic tumor prognostic assessment. Several studies have now demonstrated that the anticipated differences in survival between the newly defined AIIIDHmut and AAIIIIDHmut have lost their significance. In contrast, GBMIDHmut still exhibits a significantly worse outcome than its lower grade IDH-mutant counterparts. To address the problem of establishing prognostically significant grading for IDH-mutant astrocytic gliomas in the IDH era, we undertook a comprehensive study that included assessment of histological and genetic approaches to prognosis in these tumors. A discovery cohort of 211 IDH-mutant astrocytic gliomas with an extended observation was subjected to histological review, image analysis, and DNA methylation studies. Tumor group-specific methylation profiles and copy number variation (CNV) profiles were established for all gliomas. Algorithms for automated CNV analysis were developed. All tumors exhibiting 1p/19q codeletion were excluded from the series. We developed algorithms for grading, based on molecular, morphological and clinical data. Performance of these algorithms was compared with that of WHO grading. Three independent cohorts of 108, 154 and 224 IDH-mutant astrocytic gliomas were used to validate this approach. In the discovery cohort several molecular and clinical parameters were of prognostic relevance. Most relevant for overall survival (OS) was CDKN2A/B homozygous deletion. Other parameters with major influence were necrosis and the total number of CNV. Proliferation as assessed by mitotic count, which is a key parameter in 2016 CNS WHO grading, was of only minor influence. Employing the parameters most relevant for OS in our discovery set, we developed two models for grading these tumors. These models performed significantly better than WHO grading in both the discovery and the validation sets. Our novel algorithms for grading IDH-mutant astrocytic gliomas overcome the challenges caused by introduction of IDH status into the WHO classification of diffuse astrocytic tumors. We propose that these revised approaches be used for grading of these tumors and incorporated into future WHO criteria.Entities:
Keywords: Astrocytoma; CDKN2A/B; Glioblastoma; Grading; IDH
Mesh:
Substances:
Year: 2018 PMID: 29687258 DOI: 10.1007/s00401-018-1849-4
Source DB: PubMed Journal: Acta Neuropathol ISSN: 0001-6322 Impact factor: 17.088