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2021 年度 実績報告書

ストレスメディエーターClaspinによるストレス反応の統合的な制御機構の解明

研究課題

研究課題/領域番号 19K16367
研究機関公益財団法人東京都医学総合研究所

研究代表者

楊 其駿  公益財団法人東京都医学総合研究所, 基礎医科学, 研究員 (80792647)

研究期間 (年度) 2019-04-01 – 2022-03-31
キーワードClaspin / serum stimulation / PI3 kinase / PDK1 / mTOR
研究実績の概要

Claspin plays multiple important roles in regulation of DNA replication as a mediator for the cellular response to replication stress, an integral replication fork factor that facilitates replication fork progression and a factor that promotes initiation by recruiting Cdc7 kinase. Here, we report a novel role of Claspin in growth recovery from serum starvation, which requires the activation of PI3 kinase (PI3K)- PDK1-Akt-mTOR pathways. In the absence of Claspin, cells do not proceed into S phase and eventually die partially in a ROS- and p53-dependent manner. Claspin directly interacts with PI3K and mTOR, and is required for activation of PI3K-PDK1-mTOR and for that of mTOR downstream factors, p70S6K and 4E-BP1, but not for p38 MAPK cascade during the recovery from serum starvation. PDK1 physically interacts with Claspin, notably with CKBD, in a manner dependent on phosphorylation of the latter protein, and is required for interaction of mTOR with Claspin. Thus, Claspin plays a novel role as a key regulator for nutrition-induced proliferation/survival signaling by activating the mTOR pathway. The results also suggest a possibility that Claspin may serve as a common mediator that receives signals from different PI3K-related kinases and transmit them to specific downstream kinases.

  • 研究成果

    (1件)

すべて 2022

すべて 雑誌論文 (1件) (うちオープンアクセス 1件)

  • [雑誌論文] Claspin is required for growth recovery from serum starvation through regulating the PI3K-PDK1-mTOR pathway2022

    • 著者名/発表者名
      Yang Chi-Chun、Masai Hisao
    • 雑誌名

      biorxiv

      巻: 0121 ページ: 475743

    • DOI

      10.1101/2022.01.21.475743

    • オープンアクセス

URL: 

公開日: 2022-12-28  

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