Significant increase of high-risk chromosome 1q gain and 6q loss at recurrence in posterior fossa group A ependymoma: A multicenter study

Author:

Donson Andrew M12ORCID,Bertrand Kelsey C3ORCID,Riemondy Kent A4ORCID,Gao Dexiang15ORCID,Zhuang Yonghua15ORCID,Sanford Bridget1ORCID,Norris Gregory A12ORCID,Chapman Rebecca J6ORCID,Fu Rui7,Willard Nicholas8ORCID,Griesinger Andrea M12ORCID,Ribeiro de Sousa Graziella12ORCID,Amani Vladimir12ORCID,Grimaldo Enrique12,Hankinson Todd C29ORCID,Booker Ffyona6,Sill Martin1011ORCID,Grundy Richard G6ORCID,Pajtler Kristian W101112ORCID,Ellison David W3,Foreman Nicholas K12ORCID,Ritzmann Timothy A6ORCID

Affiliation:

1. Department of Pediatrics, University of Colorado Anschutz Medical Campus, Aurora , Colorado , USA

2. Morgan Adams Foundation Pediatric Brain Tumor Research Program, Children’s Hospital Colorado , Aurora, Colorado , USA

3. St. Jude Children’s Research Hospital , Memphis, TN , USA

4. RNA Biosciences Initiative, University of Colorado Anschutz Medical Campus , Aurora, Colorado , USA

5. University of Colorado Cancer Center Biostatistics and Bioinformatics Shared Resource, University of Colorado Anschutz Medical Campus , Aurora, Colorado , USA

6. Children’s Brain Tumor Research Centre, University of Nottingham , Nottingham , UK

7. Computational Biology, New York Genome Center , New York, New York , USA

8. Department of Pathology, University of Colorado Denver , Aurora, Colorado , USA

9. Department of Neurosurgery, University of Colorado Denver , Aurora, Colorado , USA

10. Hopp-Children’s Cancer Center Heidelberg (KiTZ) , Heidelberg , Germany

11. Division of Pediatric Neurooncology, German Cancer Research Center (DKFZ) and German Cancer Consortium (DKTK) , Heidelberg , Germany

12. Department of Pediatric Oncology, Hematology, and Immunology and Pulmonology, Heidelberg University Hospital , Heidelberg , Germany

Abstract

AbstractBackgroundEpendymoma (EPN) posterior fossa group A (PFA) has the highest rate of recurrence and the worst prognosis of all EPN molecular groups. At relapse, it is typically incurable even with re-resection and re-irradiation. The biology of recurrent PFA remains largely unknown; however, the increasing use of surgery at first recurrence has now provided access to clinical samples to facilitate a better understanding of this.MethodsIn this large longitudinal international multicenter study, we examined matched samples of primary and recurrent disease from PFA patients to investigate the biology of recurrence.ResultsDNA methylome derived copy number variants (CNVs) revealed large-scale chromosome gains and losses at recurrence in PFA. CNV changes were dominated by chromosome 1q gain and/or 6q loss, both previously identified as high-risk factors in PFA, which were present in 23% at presentation but increased to 61% at first recurrence. Multivariate survival analyses of this cohort showed that cases with 1q gain or 6q loss at first recurrence were significantly more likely to recur again. Predisposition to 1q+/6q− CNV changes at recurrence correlated with hypomethylation of heterochromatin-associated DNA at presentation. Cellular and molecular analyses revealed that 1q+/6q− PFA had significantly higher proportions of proliferative neuroepithelial undifferentiated progenitors and decreased differentiated neoplastic subpopulations.ConclusionsThis study provides clinically and preclinically actionable insights into the biology of PFA recurrence. The hypomethylation predisposition signature in PFA is a potential risk-classifier for trial stratification. We show that the cellular heterogeneity of PFAs evolves largely because of genetic evolution of neoplastic cells.

Funder

University of Colorado School of Medicine

University of Colorado

Tanner Seebaum Foundation

Morgan Adams Foundation

James Tudor Foundation

Publisher

Oxford University Press (OUP)

Subject

Cancer Research,Neurology (clinical),Oncology

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