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Publication : Normal mammalian cells negatively regulate telomere length by telomere trimming.

First Author  Pickett HA Year  2011
Journal  Hum Mol Genet Volume  20
Issue  23 Pages  4684-92
PubMed ID  21903669 Mgi Jnum  J:177559
Mgi Id  MGI:5295495 Doi  10.1093/hmg/ddr402
Citation  Pickett HA, et al. (2011) Normal mammalian cells negatively regulate telomere length by telomere trimming. Hum Mol Genet 20(23):4684-92
abstractText  In human cancer cells with telomeres that have been over-lengthened by exogenous telomerase activity, telomere shortening can occur by a process that generates circles of double-stranded telomeric DNA (t-circles). Here, we demonstrate that this telomeretrimming process occurs in cells of the male germline and in normal lymphocytes following mitogen-stimulated upregulation of telomerase activity. Mouse tissues also contain abundant t-circles, suggesting that telomere trimming also contributes to telomere length regulation in mice. In cancer cells and stimulated lymphocytes, the mechanism involves the XRCC3 homologous recombination (HR) protein and generates single-stranded C-rich telomeric DNA. This suggests that, in addition to the well-documented gradual telomere attrition that accompanies cellular replication, there is also a more rapid form of negative telomere length control in normal mammalian cells, which most likely involves HR-mediated removal of telomere loops in the form of t-circles. We therefore propose that this telomere trimming mechanism is an additional factor in the balance between telomere lengthening and telomere shortening in normal human germline and somatic cells that may prevent excessive lengthening by processes such as telomerase activity.
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