| Literature DB >> 35320876 |
Jason Chiang1, Daniel C Moreira2,3, Nicholas J Pytel3, Yen-Chun Liu1, Patrick R Blackburn1, Zonggao Shi4, Maria Cardenas4, David A Wheeler4, Larissa V Furtado1.
Abstract
Recent advancements in molecular characterisation have identified four principal molecular groups of medulloblastoma: WNT, SHH, group 3 and group 4. Each has its characteristic clinical features, signature genetic alterations and distinct DNA methylome profiles. Thus far, CTNNB1 mutations have been considered pathognomonic of WNT-activated medulloblastoma. Furthermore, it has been shown that CTNNB1 mutations dominantly drive the WNT-activated phenotype in medulloblastoma, even in the presence of alterations in the SHH pathway. We herein report an illustrative case that challenges this belief-a medulloblastoma with a pathogenic CTNNB1 mutation that otherwise showed the histopathology, immunophenotype and methylation and transcriptomic profiles of an SHH-activated medulloblastoma. Detailed molecular analyses, including whole exome sequencing, transcriptome analysis and DNA methylation profiling with DKFZ brain tumour classifier and St. Jude MLPnet neural network classifier analyses, have been performed on the tumour. Our example emphasises the diagnostic value of the immunohistochemistry panel with YAP1, GAB1 and β-catenin and DNA methylation profiling, combined with exome sequencing, in the characterisation of medulloblastoma. CTNNB1 mutations are not specific for WNT-activated medulloblastoma, and different CTNNB1 mutations have diverse oncogenic potential.Entities:
Keywords: CTNNB1 S45; DNA methylation; SHH-activated; WNT-activated; immunophenotype; medulloblastoma; transcriptomic profile
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Year: 2022 PMID: 35320876 PMCID: PMC9295902 DOI: 10.1111/nan.12815
Source DB: PubMed Journal: Neuropathol Appl Neurobiol ISSN: 0305-1846 Impact factor: 6.250