| Literature DB >> 10784448 |
R P Lanza1, J B Cibelli, C Blackwell, V J Cristofalo, M K Francis, G M Baerlocher, J Mak, M Schertzer, E A Chavez, N Sawyer, P M Lansdorp, M D West.
Abstract
The potential of cloning depends in part on whether the procedure can reverse cellular aging and restore somatic cells to a phenotypically youthful state. Here, we report the birth of six healthy cloned calves derived from populations of senescent donor somatic cells. Nuclear transfer extended the replicative life-span of senescent cells (zero to four population doublings remaining) to greater than 90 population doublings. Early population doubling level complementary DNA-1 (EPC-1, an age-dependent gene) expression in cells from the cloned animals was 3.5- to 5-fold higher than that in cells from age-matched (5 to 10 months old) controls. Southern blot and flow cytometric analyses indicated that the telomeres were also extended beyond those of newborn (<2 weeks old) and age-matched control animals. The ability to regenerate animals and cells may have important implications for medicine and the study of mammalian aging.Entities:
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Year: 2000 PMID: 10784448 DOI: 10.1126/science.288.5466.665
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728