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Publication : Telomere maintenance by recombination in human cells.

First Author  Dunham MA Year  2000
Journal  Nat Genet Volume  26
Issue  4 Pages  447-50
PubMed ID  11101843 Mgi Jnum  J:194515
Mgi Id  MGI:5474061 Doi  10.1038/82586
Citation  Dunham MA, et al. (2000) Telomere maintenance by recombination in human cells. Nat Genet 26(4):447-50
abstractText  Telomeres of eukaryotic chromosomes contain many tandem repeats of a G-rich sequence (for example, TTAGGG in vertebrates). In most normal human cells, telomeres shorten with each cell division, and it is proposed that this limits the number of times these cells can replicate. Telomeres may be maintained in germline cells, and in many immortalized cells and cancers, by the telomerase holoenzyme (first discovered in the ciliate Tetrahymena), which uses an RNA subunit as template for synthesis of telomeric DNA by the reverse transcriptase catalytic subunit. Some immortalized human cell lines and some tumours maintain their telomeres in the absence of any detectable telomerase activity by a mechanism referred to as alternative lengthening of telomeres (ALT). Here we show that DNA sequences are copied from telomere to telomere in an immortalized human ALT cell line, indicating that ALT occurs by means of homologous recombination and copy switching.
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