TY - JOUR
T1 - Prognostic significance of clinical, histopathological, and molecular characteristics of medulloblastomas in the prospective HIT2000 multicenter clinical trial cohort
AU - Pietsch, Torsten
AU - Schmidt, Rene
AU - Remke, Marc
AU - Korshunov, Andrey
AU - Hovestadt, Volker
AU - Jones, David T.W.
AU - Felsberg, Jörg
AU - Kaulich, Kerstin
AU - Goschzik, Tobias
AU - Kool, Marcel
AU - Northcott, Paul A.
AU - Von Hoff, Katja
AU - Von Bueren, André O.
AU - Friedrich, Carsten
AU - Mynarek, Martin
AU - Skladny, Heyko
AU - Fleischhack, Gudrun
AU - Taylor, Michael D.
AU - Cremer, Friedrich
AU - Lichter, Peter
AU - Faldum, Andreas
AU - Reifenberger, Guido
AU - Rutkowski, Stefan
AU - Pfister, Stefan M.
N1 - Funding Information:
Acknowledgments This work was principally funded by the BMBF program “Molecular Diagnostics” (TP, Tg, FC, Pl, AF, gr, Sr, SMP). Mr was funded by the Baden-Württemberg Stiftung. For technical support and expertise we thank Matthias Schick, roger Fischer, Melanie Bewerunge-Hudler and the DKFZ genomics and Proteomics Core Facility and Anja zur Mühlen, Department of Neuropathology, University of Bonn. The HIT2000 trial office (KvH, AvB, CF, Sr) and the DgNN Brain Tumor reference Center (Neuropathology, TP, Tg) was additionally funded by the Deutsche Kinderkrebsstiftung (german Children´s Cancer Foundation).
PY - 2014/7
Y1 - 2014/7
N2 - This study aimed to prospectively evaluate clinical, histopathological and molecular variables for outcome prediction in medulloblastoma patients. Patients from the HIT2000 cooperative clinical trial were prospectively enrolled based on the availability of sufficient tumor material and complete clinical information. This revealed a cohort of 184 patients (median age 7.6 years), which was randomly split at a 2:1 ratio into a training (n = 127), and a test (n = 57) dataset in order to build and test a risk score for this population. Independent validation was performed in a non-overlapping cohort (n = 83). All samples were subjected to thorough histopathological investigation, CTNNB1 mutation analysis, quantitative PCR, MLPA and FISH analyses for cytogenetic variables, and methylome analysis. By univariable analysis, clinical factors (M-stage), histopathological variables (large cell component, endothelial proliferation, synaptophysin pattern), and molecular features (chromosome 6q status, MYC amplification, subgrouping) were found to be prognostic. Molecular consensus subgrouping (WNT, SHH, Group 3, Group 4) was validated as an independent feature to stratify patients into different risk groups. When comparing methods for the identification of WNT-driven medulloblastoma, this study identified CTNNB1 sequencing and methylation profiling to most reliably identify these patients. After removing patients with particularly favorable (CTNNB1 mutation, extensive nodularity) or unfavorable (MYC amplification) markers, a risk score for the remaining "intermediate molecular risk" population dependent on age, M-stage, pattern of synaptophysin expression, and MYCN copy-number status was identified, with speckled synaptophysin expression indicating worse outcome. Test and independent validation of the score confirmed significant discrimination of patients by risk profile. Methylation subgrouping and CTNNB1 mutation status represent robust tools for the risk stratification of medulloblastoma. A simple clinico-pathological risk score was identified, which was confirmed in a test set and by independent clinical validation.
AB - This study aimed to prospectively evaluate clinical, histopathological and molecular variables for outcome prediction in medulloblastoma patients. Patients from the HIT2000 cooperative clinical trial were prospectively enrolled based on the availability of sufficient tumor material and complete clinical information. This revealed a cohort of 184 patients (median age 7.6 years), which was randomly split at a 2:1 ratio into a training (n = 127), and a test (n = 57) dataset in order to build and test a risk score for this population. Independent validation was performed in a non-overlapping cohort (n = 83). All samples were subjected to thorough histopathological investigation, CTNNB1 mutation analysis, quantitative PCR, MLPA and FISH analyses for cytogenetic variables, and methylome analysis. By univariable analysis, clinical factors (M-stage), histopathological variables (large cell component, endothelial proliferation, synaptophysin pattern), and molecular features (chromosome 6q status, MYC amplification, subgrouping) were found to be prognostic. Molecular consensus subgrouping (WNT, SHH, Group 3, Group 4) was validated as an independent feature to stratify patients into different risk groups. When comparing methods for the identification of WNT-driven medulloblastoma, this study identified CTNNB1 sequencing and methylation profiling to most reliably identify these patients. After removing patients with particularly favorable (CTNNB1 mutation, extensive nodularity) or unfavorable (MYC amplification) markers, a risk score for the remaining "intermediate molecular risk" population dependent on age, M-stage, pattern of synaptophysin expression, and MYCN copy-number status was identified, with speckled synaptophysin expression indicating worse outcome. Test and independent validation of the score confirmed significant discrimination of patients by risk profile. Methylation subgrouping and CTNNB1 mutation status represent robust tools for the risk stratification of medulloblastoma. A simple clinico-pathological risk score was identified, which was confirmed in a test set and by independent clinical validation.
KW - Biomarker
KW - Clinical trial cohort
KW - Medulloblastoma
KW - Methylation profiling
KW - Prospective
KW - Risk stratification
UR - http://www.scopus.com/inward/record.url?scp=84903817160&partnerID=8YFLogxK
U2 - 10.1007/s00401-014-1276-0
DO - 10.1007/s00401-014-1276-0
M3 - Article
C2 - 24791927
AN - SCOPUS:84903817160
SN - 0001-6322
VL - 128
SP - 137
EP - 149
JO - Acta Neuropathologica
JF - Acta Neuropathologica
IS - 1
ER -