Molecular, Histologic, and Clinical Characterization of Methylation Class Pleomorphic Xanthoastrocytoma: An Analysis of 469 Tumors

Authors

• Christopher H Dampier
• Niharika Shah
• Kristyn Galbraith
• Azadeh Ebrahimi
• Osorio Lopes Abath Neto
• Zied Abdullaev
• Sanda Alexandrescu
• Felipe Andreiuolo
• Terri Armstrong
• Tiffany Baker
• Sahara Cathcart
• Hye-Jung Chung
• Patrick J Cimino
• Kyle S Conway
• Jennifer Cotter
• Felipe D'Almeida Costa
• Karen Dazelle
• Nima Etminam
• Sima Esther Ferman
• Igor Fernandes
• Christina K Ferrone
• Ahmed Gilani
• Mark Gilbert
• Jason Gregory
• Courtney Ketchum
• Han Sung Lee
• Ina Lee
• Maria Beatriz S Lopes
• Qinwen Mao
• Michael S Marshall
• Matthew McCord
• Stewart G Neill
• Jeffrey J Nirschl
• Byram H Ozer
• Werner Paulus
• Marta Penas-Prado
• Marco Prinz
• Peter Pytel
• Martha Quezado
• Mark Raffeld
• Sharika Rajan
• Miriam Ratliff
• Guido Reifenberger
• Lorraina Robinson
• Jens Schittenhelm
• Daniel Schrimpf
• Omkar Singh
• Christian Thomas
• Diana Thomas
• Jaiyeola Thomas-Ogunniyi
• Angus Toland
• Rust Turakulov
• Rachael Vaubel
• Nitin Wadhwani
• Jing Wu
• Caterina Giannini
• Matija Snuderl
• Sebastian Brandner
• Andreas von Deimling
• Kenneth Aldape

Language

English

Publication Date

1-1-2025

Journal

Neuro-Oncology Advances

DOI

10.1093/noajnl/vdaf089

PMID

40735274

PMCID

PMC12305539

PubMedCentral® Posted Date

6-19-2025

PubMedCentral® Full Text Version

Post-print

Abstract

Background: Methylation class pleomorphic xanthoastrocytoma (mcPXA) comprises tumors with the DNA methylation signature of classical PXA but with a wider histologic spectrum, including overlap with glioblastoma (GBM).

Methods: To clarify the histologic and molecular scope of mcPXA and characterize its clinical behavior, a cohort of 469 tumor samples from 458 patients matching to mcPXA by the DKFZ classifier (v12.6 score ≥0.85) was interrogated.

Results: Patient median age was 23 years (range 1-73 years) with a female predominance (259 female/199 male). CDKN2A/B homozygous deletion was observed in 406 of 469 (87%) samples. In samples tested for BRAF p.V600E mutations (n = 279), 240 (86%) harbored the mutation. A chr7+/chr10- pattern was observed in 103 of 469 (22%) samples. Among samples tested for TERT promoter mutations (n = 143), 32 (22%) harbored the mutation. Progression-free and overall survival of patients with mcPXA were comparable to patients with methylation class IDH-mutant astrocytoma, low grade, but a GBM-like subset (ie, cases with a pre-methylation working diagnosis of GBM) showed shorter survival. Histologic features of high grade, including palisading necrosis and microvascular proliferation, were prognostic in mcPXA. Compared to patients with BRAF p.V600E-altered GBM, patients with mcPXA were younger and had a lower frequency of TERT promoter mutations.

Conclusion: Tumors in mcPXA share molecular characteristics with histologically defined PXA, and high-grade histologic features can help predict their clinical behavior. The use of an epigenetic classification of PXA reveals that this group of tumors is more common than previously appreciated and warrants in-depth study to identify efficacious therapeutic options.

Keywords

BRAF p.V600E, CDKN2A/B deletion, DNA methylation classification, epithelioid glioblastoma, pleomorphic xanthoastrocytoma

Published Open-Access

yes

Recommended Citation

Dampier, Christopher H; Shah, Niharika; Galbraith, Kristyn; et al., "Molecular, Histologic, and Clinical Characterization of Methylation Class Pleomorphic Xanthoastrocytoma: An Analysis of 469 Tumors" (2025). Faculty, Staff and Student Publications. 4081.
https://digitalcommons.library.tmc.edu/uthmed_docs/4081