Journals of Gerontology Series A: Biological Sciences and Medical Sciences, Vol 53, Issue 1 B11-B17, Copyright © 1998 by The Gerontological Society of America
Accelerated aging of dermal fibroblast-like cells from the senescence- accelerated mouse (SAM): acceleration of changes in DNA ploidy associated with in vitro cellular aging
H Fujisawa, T Nishikawa, BH Zhu, N Takeda, H Jujo, K Higuchi and M Hosokawa
Department of Senescence Biology, Faculty of Medicine, Kyoto University, Japan.
Accelerated changes in the DNA ploidy associated with in vitro aging were
examined in fibroblast-like cells isolated from the dorsal dermis of
newborn SAMP11 (accelerated senescence-prone, short-lived) mice, and were
compared to changes observed in cell lines from SAMR1 (accelerated
senescence-resistant, long-lived) mice. Flow cytometric analysis of the DNA
content in confluent cells and chromosome analysis in mitoses revealed that
the diploid cells were being replaced with tetraploid cells until a growth
crisis; thereafter, hypotetraploid cells became predominant, accompanied by
immortalization. The number of mitoses decreased as the crisis ensued, then
increased. Although these changes were observed in the cell lines from both
strains of mice, the changes occurred more rapidly and at earlier
population doublings in the cell lines from the SAMP11 mice. These results
suggest that the cell lines from SAMP11 mice might have higher
susceptibility to factors that cause polyploidization, including oxidative
stress.
