Both Epimutations and Chromosome Aberrations Affect Multiple Imprinted Loci in Aggressive Wilms Tumors

About 7% of all children's malignancies are represented by the embryonal renal cancer Wilms tumor (WT). Since methylation imprinting alterations at multiple loci dictated by chromosome copy-number variations have been recently demonstrated in adult cancers, we investigated the presence of simil...

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Detalles Bibliográficos
Autores: Pignata, Laura|||0000-0001-8835-5567, Palumbo, Orazio|||0000-0001-6583-3482, Cerrato, Flavia|||0000-0003-3794-3021, Acurzio, Basilia|||0000-0002-4703-8511, De Álava, Enrique|||0000-0001-8400-046X, Roma, Josep|||0000-0001-7692-6123, Gallego, Soledad|||0000-0002-4712-9624, Català-Mora, Jaume|||0000-0003-2152-8579, Carella, Massimo|||0000-0002-6830-6829, Riccio, Andrea|||0000-0001-7990-3576, Verde, Gaetano|||0000-0003-4768-0165
Tipo de recurso: artículo
Fecha de publicación:2020
País:España
Institución:Universitat Autònoma de Barcelona
Repositorio:Dipòsit Digital de Documents de la UAB
Idioma:inglés
OAI Identifier:oai:ddd.uab.cat:253110
Acceso en línea:https://ddd.uab.cat/record/253110
https://dx.doi.org/urn:doi:10.3390/cancers12113411
Access Level:acceso abierto
Palabra clave:Nephroblastoma
Genomic imprinting
DNA methylation
Chromosome aberrations
Descripción
Sumario:About 7% of all children's malignancies are represented by the embryonal renal cancer Wilms tumor (WT). Since methylation imprinting alterations at multiple loci dictated by chromosome copy-number variations have been recently demonstrated in adult cancers, we investigated the presence of similar alterations in pediatric malignancies. Our results demonstrated that 35% of WT cases were affected by methylation abnormalities of multiple imprinted loci. However, differently from adult cancers, they were associated with either chromosome aberrations or normal chromosome profiles. Epigenotype-phenotype correlations indicated that these epimutations were more frequent in highly aggressive tumors, suggesting the use of multiple methylation imprinting defects as a new informative marker for WT. The embryonal renal cancer Wilms tumor (WT) accounts for 7% of all children's malignancies. Its most frequent molecular defect is represented by DNA methylation abnormalities at the imprinted 11p15.5 region. Multiple imprinted methylation alterations dictated by chromosome copy-number variations have been recently demonstrated in adult cancers, raising the question of whether multiple imprinted loci were also affected in WT. To address this issue, we analyzed DNA methylation and chromosome profiles of 7 imprinted loci in 48 WT samples. The results demonstrated that methylation abnormalities of multiple imprinted loci occurred in 35% of the cases, but that they were associated with either chromosome aberrations or normal chromosome profiles. Multiple imprinted methylation changes were correlated with tumor stage and presence of metastasis, indicating that these epimutations were more frequent in highly aggressive tumors. When chromosome profiles were affected, these alterations were extended to flanking cancer driver genes. Overall, this study demonstrates the presence of multiple imprinted methylation defects in aggressive WTs and suggests that the mechanism by which they arise in embryonal and adult cancers is different