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E2F1 Responds to Ultraviolet Radiation by Directly Stimulating DNA Repair and Suppressing Carcinogenesis.

Cancer Res.. 2014-04; 
Biswas AK1, Mitchell DL, Johnson DG. Department of Molecular Carcinogenesis, University of Texas MD Anderson Cancer Center, Science Park
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摘要

In response to DNA damage the E2F1 transcription factor is phosphorylated at serine 31 (serine 29 in mouse) by the ATM or ATR kinases, which promotes E2F1 protein stabilization. Phosphorylation of E2F1 also leads to the recruitment of E2F1 to sites of DNA damage where it functions to enhance DNA repair. To study the role of this E2F1 phosphorylation event in vivo, a knock-in mouse model was generated in which serine 29 was mutated to alanine. The S29A mutation impairs E2F1 stabilization in response to ultraviolet (UV) radiation and doxorubicin treatment but has little effect on the expression of E2F target genes. The apoptotic and proliferative responses to acute UV radiation exposure is also similar between wi... More

关键词

E2F1; ATR; GCN5; nucleotide excision repair; skin carcinogenesis