| Literature DB >> 26054846 |
Hiroyuki Kato1, Koreyuki Kurosawa1, Yui Inoue2, Nobuhiro Tanuma1, Yuki Momoi2, Katsuhisa Hayashi1, Honami Ogoh3, Miyuki Nomura2, Masato Sakayori2, Yoichiro Kakugawa2, Yoji Yamashita2, Koh Miura2, Makoto Maemondo4, Ryuichi Katakura2, Shigemi Ito5, Masami Sato6, Ikuro Sato5, Natsuko Chiba7, Toshio Watanabe3, Hiroshi Shima8.
Abstract
We previously reported that deficiency in the gene encoding the catalytic subunit of protein phosphatase 6 (Ppp6c) predisposes mouse skin tissue to papilloma formation initiated by DMBA. Here, we demonstrate that Ppp6c loss acts as a tumor promoter in UVB-induced squamous cell carcinogenesis. Following UVB irradiation, mice with Ppp6c-deficient keratinocytes showed a higher incidence of skin squamous cell carcinoma than did control mice. Time course experiments showed that following UVB irradiation, Ppp6c-deficient keratinocytes upregulated expression of p53, PUMA, BAX, and cleaved caspase-3 proteins. UVB-induced tumors in Ppp6c-deficient keratinocytes exhibited a high frequency of both p53- and γH2AX-positive cells, suggestive of DNA damage. Epidemiological and molecular data strongly suggest that UVB from sunlight induces p53 gene mutations in keratinocytes and is the primary causative agent of human skin cancers. Our analysis suggests that PP6 deficiency underlies molecular events that drive outgrowth of initiated keratinocytes harboring UVB-induced mutated p53. Understanding PP6 function in preventing UV-induced tumorigenesis could suggest strategies to prevent and treat this condition.Entities:
Keywords: PUMA; Protein phosphatase; UV-induced carcinogenesis; apoptosis; p53; γH2AX
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Year: 2015 PMID: 26054846 DOI: 10.1016/j.canlet.2015.05.022
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679