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(American Journal of Pathology. 2000;157:571-578.)
© 2000 American Society for Investigative Pathology

Regular Articles

Characterization of Genomic Alterations in Hepatoblastomas

A Role for Gains on Chromosomes 8q and 20 as Predictors of Poor Outcome

Ruthild G. Weber^*, Torsten Pietsch, Dietrich von Schweinitz^§ and Peter Lichter^*

From the Abteilung Organisation komplexer Genome,^*
Deutsches Krebsforschungszentrum, Heidelberg, Germany; the Institut für Humangenetik,
Ruprecht-Karls-Universität, Heidelberg, Germany; the Institut für Neuropathologie,
Rheinische Friedrich-Wilhelms-Universität, Bonn, Germany; and the Abteilung für Kinderchirurgie,^§
Universitäts-Kinderspital Beider Basel, Switzerland

As data on the genomic alterations in hepatoblastoma (HB) are limited, 34 HB tumors and three HB cell lines were screened for DNA copy number changes by comparative genomic hybridization. The average number of chromosomal imbalances per tumor was 2.3 ± 0.5 (mean ± SEM) with gains sevenfold more frequent than losses. The most frequent gains of chromosomal material in HB tumors were on 2q (44%), 1q (41%), 2p (29%), 20 (24%), 22q (18%), 8q (15%), 8p and 12q (9% each), as well as 7q, 12p, and 17 (6% each) and the only recurrent loss was on 4q in 12% of cases. Highly amplified sequences were identified in four tumors and mapped to 2q24 in two cases, to 8q in two cases (once to 8q11.2-q13 and once to 8q11.2-q21.3) as well as to 10q24-q26 in one case. In one cell line, highly amplified DNA sequences were mapped to 7p and 8q. Comparison to previously published data on this series of HB revealed that the number of chromosomal imbalances was significantly higher in HB tumors with loss of heterozygosity on 11p (P = 0.03), whereas in five of 10 HB biopsies without chromosomal imbalances, ß-catenin gene mutations were found. HB patients were divided into a good (no evidence of disease) and a poor (died of disease) outcome group according to their clinical course after standard therapy. Two alterations were found to be significantly associated with poor outcome: gain on 8q (P = 0.007) and gain on 20 (P = 0.009). In summary, our analysis allowed the identification of gains on chromosomes 1q and 2 as hallmark DNA copy number changes in HB with 2q24 as a critical chromosomal band. Furthermore, this study provided evidence that gains on 8q and 20 play a role as markers of prognostic significance in HB.

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