Biology and grading of pleomorphic xanthoastrocytoma-what have we learned about it?
astrocytoma
glioma
methylation
pleomorphic xanthoastrocytoma
Journal
Brain pathology (Zurich, Switzerland)
ISSN: 1750-3639
Titre abrégé: Brain Pathol
Pays: Switzerland
ID NLM: 9216781
Informations de publication
Date de publication:
01 2021
01 2021
Historique:
received:
07
05
2020
revised:
09
06
2020
accepted:
16
06
2020
pubmed:
4
7
2020
medline:
21
12
2021
entrez:
4
7
2020
Statut:
ppublish
Résumé
Pleomorphic xanthoastrocytoma (PXA) is a rare astrocytoma predominantly affecting children and young adults. We performed comprehensive genomic characterization on a cohort of 67 patients with histologically defined PXA (n = 53, 79%) or anaplastic PXA (A-PXA, n = 14, 21%), including copy number analysis (ThermoFisher Oncoscan, n = 67), methylation profiling (Illumina EPIC array, n = 43) and targeted next generation sequencing (n = 32). The most frequent alterations were CDKN2A/B deletion (n = 63; 94%) and BRAF p.V600E (n = 51, 76.1%). In 7 BRAF p.V600 wild-type cases, alternative driver alterations were identified involving BRAF, RAF1 and NF1. Downstream phosphorylation of ERK kinase was uniformly present. Additional pathogenic alterations were rare, with TERT, ATRX and TP53 mutations identified in a small number of tumors, predominantly A-PXA. Methylation-based classification of 46 cases utilizing a comprehensive reference tumor allowed assignment to the PXA methylation class in 40 cases. A minority grouped with the methylation classes of ganglioglioma or pilocytic astrocytoma (n = 2), anaplastic pilocytic astrocytoma (n = 2) or control tissues (n = 2). In 9 cases, tissue was available from matched primary and recurrent tumors, including 8 with anaplastic transformation. At recurrence, two tumors acquired TERT promoter mutations and the majority demonstrated additional non-recurrent copy number alterations. Methylation class was preserved at recurrence. For 62 patients (92.5%), clinical follow-up data were available (median follow-up, 5.4 years). Overall survival was significantly different between PXA and A-PXA (5-year OS 80.8% vs. 47.6%; P = 0.0009) but not progression-free survival (5-year PFS 59.9% vs. 39.8%; P = 0.05). WHO grade remained a strong predictor of overall survival when limited to 38 cases defined as PXA by methylation-based classification. Our data confirm the importance of WHO grading in histologically and epigenetically defined PXA. Methylation-based classification may be helpful in cases with ambiguous morphology, but is largely confirmatory in PXA with well-defined morphology.
Identifiants
pubmed: 32619305
doi: 10.1111/bpa.12874
pmc: PMC8018001
doi:
Types de publication
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
20-32Subventions
Organisme : Deutsche Kinderkrebsstiftung (German Children Cancer Foundation)
ID : DKS 2006.03
Organisme : Deutsche Kinderkrebsstiftung (German Children Cancer Foundation)
ID : DKS 2011.01
Organisme : Deutsche Kinderkrebsstiftung (German Children Cancer Foundation)
ID : DKS 2009.19
Organisme : NCI NIH HHS
ID : P30 CA015083
Pays : United States
Organisme : Mayo Clinic
Organisme : Deutsche Kinderkrebsstiftung (German Children Cancer Foundation)
ID : DKS 2014.17
Informations de copyright
© 2020 International Society of Neuropathology.
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