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Nucleic Acids Research, 2003, Vol. 31, No. 16 4779-4790
© 2003 Oxford University Press

Cell cycle arrest and apoptosis provoked by UV radiation-induced DNA damage are transcriptionally highly divergent responses

Massimiliano Gentile, Leena Latonen and Marikki Laiho*

Haartman Institute, University of Helsinki and Helsinki University Central Hospital, FIN-00014 Helsinki, Finland

*To whom correspondence should be addressed. Tel: +358 9 1912 5540; Fax: +358 9 1912 5554; Email: marikki.laiho{at}helsinki.fi
The authors wish it to be known that, in their opinion, the first two authors should be regarded as joint First Authors

DNA damage caused by UV radiation initiates cellular recovery mechanisms, which involve activation of DNA damage response pathways, cell cycle arrest and apoptosis. To assess cellular transcriptional responses to UVC-induced DNA damage we compared time course responses of human skin fibroblasts to low and high doses of UVC radiation known to induce a transient cellular replicative arrest or apoptosis, respectively. UVC radiation elicited >3-fold changes in 460 out of 12 000 transcripts and 89% of these represented downregulated transcripts. Only 5% of the regulated genes were common to both low and high doses of radiation. Cells inflicted with a low dose of UVC exhibited transcription profiles demonstrating transient regulation followed by recovery, whereas the responses were persistent after the high dose. A detailed clustering analysis and functional classification of the targets implied regulation of biologically divergent responses and suggested involvement of transcriptional and translational machinery, inflammatory, anti-proliferative and anti-angiogenic responses. The data support the notion that UVC radiation induces prominent, dose-dependent downregulation of transcription. However, the data strongly suggest that transcriptional repression is also target gene selective. Furthermore, the results demonstrate that dose-dependent induction of cell cycle arrest and apoptosis by UVC radiation are transcriptionally highly distinct responses.


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