Molecular Characterization Reveals Subclasses of 1q Gain in Intermediate Risk Wilms Tumors

Author:

van Belzen Ianthe A. E. M.,van Tuil Marc,Badloe Shashi,Strengman EricORCID,Janse AlexORCID,Verwiel Eugène T. P.ORCID,van der Leest Douwe F. M.,de Vos Sam,Baker-Hernandez John,Groenendijk Alissa,de Krijger Ronald,Kerstens Hindrik H. D.,Drost JarnoORCID,van den Heuvel-Eibrink Marry M.,Tops Bastiaan B. J.,Holstege Frank C. P.,Kemmeren PatrickORCID,Hehir-Kwa Jayne Y.

Abstract

Chromosomal alterations have recurrently been identified in Wilms tumors (WTs) and some are associated with poor prognosis. Gain of 1q (1q+) is of special interest given its high prevalence and is currently actively studied for its prognostic value. However, the underlying mutational mechanisms and functional effects remain unknown. In a national unbiased cohort of 30 primary WTs, we integrated somatic SNVs, CNs and SVs with expression data and distinguished four clusters characterized by affected biological processes: muscle differentiation, immune system, kidney development and proliferation. Combined genome-wide CN and SV profiles showed that tumors profoundly differ in both their types of 1q+ and genomic stability and can be grouped into WTs with co-occurring 1p−/1q+, multiple chromosomal gains or CN neutral tumors. We identified 1q+ in eight tumors that differ in mutational mechanisms, subsequent rearrangements and genomic contexts. Moreover, 1q+ tumors were present in all four expression clusters reflecting activation of various biological processes, and individual tumors overexpress different genes on 1q. In conclusion, by integrating CNs, SVs and gene expression, we identified subgroups of 1q+ tumors reflecting differences in the functional effect of 1q gain, indicating that expression data is likely needed for further risk stratification of 1q+ WTs.

Funder

Foundation KiKa

Adessium Foundation

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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