What question did this study set out to answer?

The study aims to explore genetic characteristics of Wilms tumor among Asian patients and their association with clinical outcomes.

March 25, 2026Open Access

Gain of Chromosome 1q and MYCN Characterize Unique Subgroups of Asian Wilms Tumor Patients

Key Points

The study aims to explore genetic characteristics of Wilms tumor among Asian patients and their association with clinical outcomes.
Analyzed chromosomal changes in 87 Wilms tumors from Singapore hospitals and an Asian validation set.
Profiled six relapsed tumors using whole-exome sequencing to identify mutational signatures.
Conducted clustering analysis to differentiate subgroups based on relapse rates and genomic features.
Identified a subgroup of predominantly non-Asian patients with higher relapse rates associated with 1p and 16q loss.
Found that gain of MYCN and 1q is linked to lower relapse rates in Asian patients.
Relapsed tumors showed no recurrent mutations, highlighting the persistence of resistant clones.

Abstract

• Risk stratification of Wilms tumor does not consider its inter-ethnic variations • 1p/16q loss and relapse are more frequent in a predominantly non-Asian subgroup • 1q gain rather than 1p/16q loss of heterozygosity associated with relapse in Asians • MYCN and PAX3 gain is associated with good outcome and more prevalent among Asians Wilms tumors in Asian populations demonstrate uniquely favorable biological characteristics and are not appropriately stratified by current risk markers like loss of heterozygosity of 1p and 16q. We analyzed the prognostic associations of copy number changes at other genomic loci in a population-based cohort of Wilms tumor and explored genomic profiles of relapsed cases. Chromosomal aberrations of targeted loci were evaluated in 61 Wilms tumors treated with National Wilms Tumor Study regimens in Singapore hospitals from 2001-2022, and 26 tumors from a separate Asian validation set, and correlated with clinical variables. Mutational signatures of 6 relapsed patients’ tumors were profiled using whole-exome sequencing. Clustering analysis identified a subgroup (65.6%) of predominantly non-Asian patients with higher frequency of relapse, 1p and 16q loss and 1q gain. A smaller predominantly-Asian subgroup (21.0%) with low stage and few relapses was characterized by gain of MYCN and minimal 1p, 1q and 16q aberrations. MYCN exon 2 gain was present in 23.0% of the discovery set and 37.5% of the validation set. Loss of IGF2 and 1p gene ABCA4, and gain of 1q genes, were associated with relapse. Notably, relapsed tumors demonstrated no recurrent somatic mutations; instead, in 2 patients with 1q gain clonal deconvolution showed persistence of chemo-refractory clones without metachronous pathogenic variants. Among Asian Wilms tumor patients, 1q gain is prognostic for relapse. Gain of MYCN features uniquely in Asian patients and may represent a favorable prognostic marker. These results identify distinct molecular subgroups associated with varying prognosis and relapse among Asian patients.

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Cite This Study

Wong et al. (Sun,) studied this question.

synapsesocial.com/papers/69c37acab34aaaeb1a67c9cd https://doi.org/https://doi.org/10.1016/j.ctarc.2026.101191

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