1. Influences of p53 deficiency on the apoptotic response, DNA damage removal and mutagenesis in UVB-exposed mouse skin
- Author
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Kiyoji Tanaka, Shingo Nakamura, Hironobu Ikehata, Toshio Mori, Setsuya Aiba, Tetsuya Ono, Ryuhei Okuyama, Atsuko Usami, and Eisaku Ogawa
- Subjects
Genome instability ,Male ,DNA Repair ,DNA repair ,DNA damage ,Ultraviolet Rays ,Health, Toxicology and Mutagenesis ,Apoptosis ,Biology ,Toxicology ,medicine.disease_cause ,Mice ,Genetics ,medicine ,Animals ,skin and connective tissue diseases ,Genetics (clinical) ,Skin ,Mutation ,integumentary system ,Epidermis (botany) ,Mutagenesis ,Molecular biology ,Cancer research ,Tumor Suppressor Protein p53 ,Genotoxicity ,Nucleotide excision repair ,DNA Damage - Abstract
p53 suppresses the genomic instability provoked by genotoxic agents. Ultraviolet (UV) B induces skin cancers by producing DNA damage and mutations in the skin genome, whereas the skin tissue responds to the UVB insult with cell cycle arrest and apoptosis as well as damage exclusion by DNA repair. To address the p53 contribution to these skin responses in vivo, we analyzed the time course of DNA damage removal, apoptosis induction and hyperplasia in the skin after UVB irradiation in p53-knockout mice. We also examined UVB-induced mutations in the skin. We found that p53 deficiency does not abolish the UVB-induced apoptotic response in the epidermis but delays the process and the following hyperplasia 12-24 h. Regardless of the p53 genotype, 1 kJ/m(2) UVB induced a total replacement of the epidermal layer by destroying the damaged epidermis by apoptosis and rebuilding a new one through hyperplasia. We failed to detect a clear defect in removal of UVB-induced DNA photolesions from the genome of the p53-deficient skin except for a delay in the epidermis, which seemed to result from the delay in the apoptotic response. However, we found that p53 deficiency enhanced UVB-induced mutagenesis. Furthermore, in a genetic study using Xpa-knockout mice, we showed that the enhanced mutagenic response depends on the activity of nucleotide excision repair (NER), which was also supported by the mutation spectrum observed in the UVB-exposed p53-knockout mice. These results indicate that p53 protects the skin genome from the UVB genotoxicity by facilitating NER, whereas its contribution to the UVB-induced apoptosis is limited.
- Published
- 2010