Chromatin association of Rad17 is required for an ataxia telangiectasia and Rad-related kinase-mediated S-phase checkpoint in response to low-dose ultraviolet radiation
Activation of the S-phase checkpoint results in an inhibition of DNA synthesis in response to DNA damage. This is an active cellular response that may enhance cell survival and limit heritable genetic abnormalities. While much attention has been paid to elucidating signal transduction pathways regulating the ionizing radiation-induced S-phase checkpoint, less is known about whether UV radiation initiates the process and the mechanism controlling it. Here, we demonstrate that low-dose UV radiation activates an S-phase checkpoint that requires the ataxia telanglectasia and Rad-related kinase (ATR). ATR regulates the S-phase checkpoint through phosphorylation of the downstream target structural maintenance of chromosomal protein 1. Furthermore, the ATPase activity of Rad17 is crucial for its chromatin association and for the functional effects of ATR activation in response to low-dose UV radiation. These results suggest that low-dose UV radiation activates an S-phase checkpoint requiring ATR-mediated signal transduction pathway.
- Publisher
- AMER ASSOC CANCER RESEARCH
- Issue Date
- 2004-06
- Language
- English
- Article Type
- Article
- Keywords
ATM-DEPENDENT PHOSPHORYLATION; DNA-DAMAGE CHECKPOINT; CELL-CYCLE CONTROL; IN-VITRO; REPLICATION CHECKPOINT; IONIZING IRRADIATION; GENOTOXIC STRESS; ACTIVATION; P53; COMPLEXES
- Citation
MOLECULAR CANCER RESEARCH, v.2, no.6, pp.362 - 369
- ISSN
- 1541-7786
- Appears in Collection
- BS-Journal Papers(저널논문)
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