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6 February 1997, Volume 14, Number 5, Pages 551-560
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Article
20q gain associates with immortalization: 20q13.2 amplification correlates with genome instability in human papillomavirus 16 E7 transformed human uroepithelial cells
Elena Savelieva1,4, Cassandra D Belair3,4, Michael A Newton2, Sandy DeVries5, Joe W Gray5, Frederic Waldman5 and Catherine A Reznikoff1,3,4

1Department of Human Oncology, University of Wisconsin Medical School

2Department of Biostatistics, University of Wisconsin Medical School

3Environmental Toxicology Center and

4Comprehensive Clinical Cancer Centre, Madison, WI 53792

5University of California at San Francisco Dept. of Laboratory Medicine, Laboratory of Cancer Genetics and Division of Molecular Cytometry, San Francisco, California 94143, USA

Correspondence: CA Reznikoff, K6/548 Clinical Science Center, 600 Highland Ave., Madison, WI 53792, USA

Abstract

Breast, bladder, colon, and ovarian carcinomas show frequent low level 20q gain and less frequently high level 20q13.2 amplification, but the significance of these 20q amplifications in transformation has not been defined. Using karyotypic and comparative genomic hybridization (CGH) analyses, chromosome losses and gains were analysed in six newly immortalized human uroepithelial cell (HUC) lines transformed by Human Papillomavirus 16 (HPV16) E7. Results showed clonal chromosomes with 20q11->qter gain in all six lines. CGH revealed a peak of 20q13.2 amplification in two cell lines. FISH with whole chromosome 20 paint showed expanded chromosome regions (ECRs) and double minute chromosomes (DMs) that contained chromosome 20 material in cell lines with 20q13.2 amplification. FISH with probes from the center of the 20q13.2 human breast cancer amplicon showed as many as 24 signals in cells with 20q13.2 amplification. The acquisition of genome instability in these E7-HUCs did not correlate with TP53 mutation, as all E7-HUCs contained only wildtype TP53. These results suggest that low level 20q gain is associated with overcoming cellular senescence in E7 transformed cells (P-value=2´10-7), but does not confer genome instability, while high level 20q13.2 amplification is associated with chromosome instability. Loss of 10p (P-value=3´10-5) was also important in immortalization of E7-transformed HUCs. Thus, these results have profound implications for interpreting the significance of high versus low level 20q gains in human cancers.

Keywords

HPV16 E7; human uroepithelial cells; immortalization; 20q amplification; genome instability

Received 23 July 1999; revised 2 October 1999; accepted 7 October 1999
6 February 1997, Volume 14, Number 5, Pages 551-560
Table of contents    Previous  Abstract  Next   Article  PDF
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