著作(論文等)

基本情報

氏名 鶴留 優也
氏名(カナ) ツルドメ ユウヤ
氏名(英語) TSURUDOME Yuya

論文名

Circadian Clock in a Mouse Colon Tumor Regulates Intracellular Iron Levels to Promote Tumor Progression

著者名

Fumiyasu Okazaki, Naoya Matsunaga, Hiroyuki Okazaki, Hiroki Azuma, Kengo Hamamura, Akito Tsuruta, Yuya Tsurudome, Takashi Ogino, Yukinori Hara, Takuya Suzuki, Kenji Hyodo, Hiroshi Ishihara, Hiroshi Kikuchi, Hideto To, Hironori Aramaki, Satoru Koyanagi, Shigehiro Ohdo

掲載誌名等

JOURNAL OF BIOLOGICAL CHEMISTRY

掲載年月

2016/03

291

13

開始頁

7017

 

終了頁

7028

出版者(日本語)

 

出版者(英語)

 

発表形態

レフェリー付き学術論文(外国語)

概要

Iron is an important biological catalyst and is critical for DNA synthesis during cell proliferation. Cellular iron uptake is enhanced in tumor cells to support increased DNA synthesis. Circadian variations in DNA synthesis and proliferation have been identified in tumor cells, but their relationship with intracellular iron levels is unclear. In this study, we identified a 24-h rhythm in iron regulatory protein 2 (IRP2) levels in colon-26 tumors implanted in mice. Our findings suggest that IRP2 regulates the 24-h rhythm of transferrin receptor 1 (Tfr1) mRNA expression post-transcriptionally, by binding to RNA stem-loop structures known as iron-response elements. We also found that Irp2 mRNA transcription is promoted by circadian clock genes, including brain and muscle Arnt-like 1 (BMAL1) and the circadian locomotor output cycles kaput (CLOCK) heterodimer. Moreover, growth in colon-26(19) tumors expressing the clock-mutant protein (CLOCK19) was low compared with that in wild-type colon-26 tumor. The time-dependent variation of cellular iron levels, and the proliferation rate in wild-type colon-26 tumor was decreased by CLOCK19 expression. Our findings suggest that circadian organization contributes to tumor cell proliferation by regulating iron metabolism in the tumor.