Résumé
Background: Although cure rates for Wilms tumours (WT) are high, many patients receive therapy with attendant long-term complications. Our goal was to stratify WT using genome-wide analyses to identify candidate molecular features for patients who would benefit from a reduction in therapy. Methods: We generated DNA methylation and exome sequencing data on WT–kidney pairs (n = 57) and unpaired tumours (n = 27) collected either at our centre or by the Children’s Oncology Group. Samples were divided into a discovery set (n = 32) and validation set (n = 52). Results: Analysis of DNA methylation revealed two subgroups of WT with distinct features. Subgroup A has a similar DNA methylation profile to mature kidney, while Subgroup B has genome-wide dysregulation of DNA methylation. The rate of non-synonymous missense mutations and segmental chromosomal aberrations was higher in Subgroup B tumours, suggesting that this group has genome instability related to its epigenetic state. Subgroup A had a higher proportion of cases of bilateral disease. Tumours with high-risk histology or from patients who relapsed were only found in Subgroup B. Conclusion: We have identified subgroup-specific molecular events that could inform future work supporting more targeted therapeutic approaches and patient stratification. We propose a novel developmental tumour model based on these findings.
Langue d'origine | English |
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Pages (de-à) | 437-446 |
Nombre de pages | 10 |
Journal | British Journal of Cancer |
Volume | 124 |
Numéro de publication | 2 |
DOI | |
Statut de publication | Published - janv. 19 2021 |
Note bibliographique
Funding Information:Funding information This study was supported by grants from the C17 Canadian Childhood Cancer network (1000039113) and from the Sick Kids Foundation (9535144613).
Publisher Copyright:
© 2020, The Author(s), under exclusive licence to Cancer Research UK.
ASJC Scopus Subject Areas
- Oncology
- Cancer Research
PubMed: MeSH publication types
- Journal Article
- Research Support, N.I.H., Extramural