Immortal, telomerase-negative cell lines derived from a Li-Fraumeni syndrome patient exhibit telomere length variability and chromosomal and minisatellite instabilities

doi:10.1093/carcin/bgg024

Carcinogenesis Advance Access originally published online on March 28, 2003

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Carcinogenesis, Vol. 24, No. 5, 953-965, May 2003
© 2003 Oxford University Press

CARCINOGENESIS

Immortal, telomerase-negative cell lines derived from a Li-Fraumeni syndrome patient exhibit telomere length variability and chromosomal and minisatellite instabilities

Takeki Tsutsui¹, Shin-ichi Kumakura¹, Yukiko Tamura¹, Takeo W. Tsutsui¹, Mizuki Sekiguchi¹, Tokihiro Higuchi²^,4 and J.Carl Barrett³^,5

¹ Department of Pharmacology, The Nippon Dental University, School of Dentistry at Tokyo, Tokyo, Japan
² Molecular Pathology Group, TSL Inc., Tokyo, Japan
³ National Cancer Institute, National Institutes of Health, Bethesda, Maryland, USA

⁵ To whom correspondence should be addressed Email: barrett{at}mail.nih.gov

Five immortal cell lines derived from a Li-Fraumeni syndromepatient (MDAH 087) with a germline mutant p53 allele were characterizedwith respect to telomere length and genomic instability. Theremaining wild-type p53 allele is lost in the cell lines. Telomeraseactivity was undetectable in all immortal cell lines. Five subclonesof each cell line and five re-subclones of each of the subclonesalso showed undetectable telomerase activity. All five immortalcell lines exhibited variability in the mean length of terminalrestriction fragments (TRFs). Subclones of each cell line, andre-subclones of the subclones also showed TRF variability, indicatingthat the variability is owing to clonal heterogeneity. Chromosomeaberrations were observed at high frequencies in these celllines including the subclones and re-subclones, and the principaltypes of aberrations were breaks, double minute chromosomesand dicentric chromosomes. In addition, minisatellite instabilitydetected by DNA fingerprints was observed in the immortal celllines. However, all of the cell lines were negative for microsatelliteinstability. As minisatellite sequences are considered recombinogenicin mammalian cells, these results suggest that recombinationrates can be increased in these cell lines. Tumor-derived humancell lines, HT1080 cells and HeLa cells that also lack p53 function,exhibited little genomic instability involving chromosomal andminisatellite instabilities, indicating that chromosomal andminisatellite instabilities observed in the immortal cell lineslacking telomerase activity could not result from loss of p53function.

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