PLoS ONE (Jan 2015)

Array CGH Analysis of Paired Blood and Tumor Samples from Patients with Sporadic Wilms Tumor.

  • Leila Cabral de Almeida Cardoso,
  • Lara Rodriguez-Laguna,
  • María Del Carmen Crespo,
  • Elena Vallespín,
  • María Palomares-Bralo,
  • Rubén Martin-Arenas,
  • Inmaculada Rueda-Arenas,
  • Paulo Antonio Silvestre de Faria,
  • GT-CSGP Working Group,
  • Purificación García-Miguel,
  • Pablo Lapunzina,
  • Fernando Regla Vargas,
  • Hector N Seuanez,
  • Víctor Martínez-Glez

DOI
https://doi.org/10.1371/journal.pone.0136812
Journal volume & issue
Vol. 10, no. 8
p. e0136812

Abstract

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Wilms tumor (WT), the most common cancer of the kidney in infants and children, has a complex etiology that is still poorly understood. Identification of genomic copy number variants (CNV) in tumor genomes provides a better understanding of cancer development which may be useful for diagnosis and therapeutic targets. In paired blood and tumor DNA samples from 14 patients with sporadic WT, analyzed by aCGH, 22% of chromosome abnormalities were novel. All constitutional alterations identified in blood were segmental (in 28.6% of patients) and were also present in the paired tumor samples. Two segmental gains (2p21 and 20q13.3) and one loss (19q13.31) present in blood had not been previously described in WT. We also describe, for the first time, a small, constitutive partial gain of 3p22.1 comprising 2 exons of CTNNB1, a gene associated to WT. Among somatic alterations, novel structural chromosomal abnormalities were found, like gain of 19p13.3 and 20p12.3, and losses of 2p16.1-p15, 4q32.5-q35.1, 4q35.2-q28.1 and 19p13.3. Candidate genes included in these regions might be constitutively (SIX3, SALL4) or somatically (NEK1, PIAS4, BMP2) operational in the development and progression of WT. To our knowledge this is the first report of CNV in paired blood and tumor samples in sporadic WT.