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Age‐dependent accumulation of genomic aberrations and deregulation of cell cycle and telomerase genes in metastatic neuroblastoma
Author(s) -
Coco Simona,
Theissen Jessica,
Scaruffi Paola,
Stigliani Sara,
Moretti Stefano,
Oberthuer André,
Valdora Francesca,
Fischer Matthias,
Gallo Fabio,
Hero Barbara,
Bonassi Stefano,
Berthold Frank,
Tonini Gian Paolo
Publication year - 2012
Publication title -
international journal of cancer
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.475
H-Index - 234
eISSN - 1097-0215
pISSN - 0020-7136
DOI - 10.1002/ijc.27432
Subject(s) - neuroblastoma , telomerase , cell cycle , cancer research , biology , oncogene , gene , stage (stratigraphy) , medicine , oncology , genetics , cell culture , paleontology
About 50% of children with neuroblastoma (NB) show a metastatic disease and have a poor prognosis. However, disease progression is greatly variable and depends on patients' age and MYCN oncogene amplification. To investigate the role of patients' age in tumor aggressiveness, we performed array‐CGH and gene expression profiles of three groups (G) of metastatic NBs: G1, stage 4S patients and MYCN single copy ( MYCN −) tumors; G2, stage 4 patients, ≤18 months of age, MYCN − tumors and favorable outcome and G3, Stage 4 patients, ≥19 months with unfavorable outcome. G1 was characterized by numerical aberrations prevalently; on the contrary, all G3 tumors had structural rearrangements, whereas G2 showed an intermediate pattern. The average of numerical alterations decreased significantly from G1 to G2 to G3 ( p < 0.01). Contrarily, the number of structural aberrations increased from G1 to G2 to G3 ( p < 2.35 E−05). Noteworthy, G3/ MYCN − NBs were characterized by several complex intrachromosome rearrangements. Expression analysis of the three groups showed significant differences in genes of Rho and Ras signaling pathways, development and adhesion, cell cycle regulation and telomerase activity. Accumulation of structural alterations increased with patients' age and was associated with a more aggressive disease. Abnormal expression of genes involved in cell cycle and telomerase in G3 may be responsible for the genomic instability in this cohort of patients. The higher DNA instability observed in G3/ MYCN − NBs than in MYCN ‐amplified G3 may also explain why patients ≥19 months have a poor outcome independently by MYCN status.

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