| Literature DB >> 25605732 |
Atsushi Naito1, Hirofumi Yamamoto2, Yoshinori Kagawa3, Yoko Naito4, Daisuke Okuzaki5, Keisuke Otani6, Yoriko Iwamoto6, Sakae Maeda3, Junichi Kikuta7, Keizo Nishikawa7, Mamoru Uemura2, Junichi Nishimura2, Taishi Hata2, Ichiro Takemasa2, Tsunekazu Mizushima2, Hideshi Ishii8, Yuichiro Doki2, Masaki Mori9, Masaru Ishii10.
Abstract
Cell cycle-arrested cancer cells are resistant to conventional chemotherapy that acts on the mitotic phases of the cell cycle, although the molecular mechanisms involved in halting cell cycle progression remain unclear. Here, we demonstrated that RFPL4A, an uncharacterized ubiquitin ligase, induced G1 retention and thus conferred decreased sensitivity to chemotherapy in the human colorectal cancer cell line, HCT116. Long term time lapse observations in HCT116 cells bearing a "fluorescence ubiquitin-based cell cycle indicator" identified a characteristic population that is viable but remains in the G1 phase for an extended period of time (up to 56 h). Microarray analyses showed that expression of RFPL4A was significantly up-regulated in these G1-arrested cells, not only in HCT116 cells but also in other cancer cell lines, and overexpression of RFPL4A increased the G1 population and decreased sensitivity to chemotherapy. However, knockdown of RFPL4A expression caused the cells to resume mitosis and induced their susceptibility to anti-cancer drugs in vitro and in vivo. These results indicate that RFPL4A is a novel factor that increases the G1 population and decreases sensitivity to chemotherapy and thus may be a promising therapeutic target for refractory tumor conditions.Entities:
Keywords: Anticancer Drug; Cell Cycle; Colon Cancer; E3 Ubiquitin Ligase; G1 Maintenance; Microarray; RFPL4A
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Year: 2015 PMID: 25605732 PMCID: PMC4358269 DOI: 10.1074/jbc.M114.614859
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157