| Literature DB >> 16765653 |
Paola Porcedda1, Valentina Turinetto, Erica Lantelme, Enrico Fontanella, Krystyna Chrzanowska, Riccardo Ragona, Mario De Marchi, Domenico Delia, Claudia Giachino.
Abstract
The repair of DNA double-strand breaks is critical for genome integrity and tumor suppression. Here we show that following treatment with the DNA-intercalating agent actinomycin D (ActD), normal quiescent T cells accumulate double-strand breaks and die, whereas T cells from ataxia telangiectasia (AT) and Nijmegen breakage syndrome (NBS) patients are resistant to this death pathway despite a comparable amount of DNA damage. We demonstrate that the ActD-induced death pathway in quiescent T lymphocytes follows DNA damage and H2AX phosphorylation, is ATM- and NBS1-dependent and due to p53-mediated cellular apoptosis. In response to genotoxic 2-Gy gamma-irradiation, on the other hand, quiescent T cells from normal donors survive following complete resolution of the damage thus induced. T cells from AT and NBS patients also survive, but retain foci of phosphorylated H2AX due to a subtle double-strand break (DSB) repair defect. A common consequence of these two genetic defects in the DSB response is the apparent tolerance of cells containing DNA breaks. We suggest that this tolerance makes a major contribution to the oncogenic risk of patients with chromosome instability syndromes.Entities:
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Year: 2006 PMID: 16765653 DOI: 10.1016/j.dnarep.2006.05.002
Source DB: PubMed Journal: DNA Repair (Amst) ISSN: 1568-7856