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2016 年度 実績報告書

イメージングと時系列統計解析による細胞死制御機構の定量的な解析

研究課題

研究課題/領域番号 15J08196
研究機関京都大学

研究代表者

三浦 晴子  京都大学, 生命科学研究科, 特別研究員(DC1)

研究期間 (年度) 2015-04-24 – 2018-03-31
キーワードp38 / JNK / cell death / crosstalk / live cell imaging
研究実績の概要

The stress activated protein kinases p38 and JNK play important roles in the cellular response to diverse stress conditions. Although p38 and JNK have been studied for decades, it is still unknown how they regulate each other and how they regulate cell fate decisions at the single cell level.
To address these issues, we performed simultaneous imaging of p38 and JNK activities in single living cells using our previously developed multiplexed fluorescent imaging system. Interestingly, we found that p38 negatively regulated JNK in all tested stress conditions, which was mediated by both transcriptional and posttranslational mechanisms.
Furthermore, p38 and JNK activities seem to have both, pro-death and pro-survival roles, which probably depends on the timing and strength of the activities.

現在までの達成度 (区分)
現在までの達成度 (区分)

2: おおむね順調に進展している

理由

I succeeded in multiplexed imaging of JNK, p38, and also caspase 8 activities in single living cells. We used this imaging system in human cancer cell lines stably expressing all reporters and analyzed their activities in response to inflammatory inputs, stresses, and chemotherapeutic drugs. By specific image analysis programs, we successfully extracted activity time courses from the raw image data of each each reporter. Perturbation experiments using inducible expression, small molecule inhibitors, and CRISPR Cas9 knock out revealed regulatory mechanisms between these pathways and implicated complex roles of JNK and p38 in cell death. To study the dual roles of JNK and p38, we performed gene expression studies. In summary, my research made good progress according to the initial plans.

今後の研究の推進方策

In future, I want to address following points.
(1) Statistical analysis of the p38 and JNK activity time-courses will extract parameters which are determinant for cell death.
(2) A synthetic and specific activation system of p38 and JNK should be developed, e.g. based on optogenetics. This will help to clarify the role of p38 and JNK, in especially whether their activities are sufficient to induce cell death.
(3) I want to titrate p38 and JNK activation by drug titration or synthetic activation and analyze the amount of induced cell death, in order to find a putative threshold of p38 and JNK activities, which separates survival and cell death.
(4) Finally, I will summarize my results in two papers, which I will submit to peer-reviewed scientific journals.

  • 研究成果

    (5件)

すべて 2017 2016

すべて 学会発表 (5件) (うち国際学会 2件)

  • [学会発表] Single cell analysis of stress signaling dynamics in a life-death decision2017

    • 著者名/発表者名
      Haruko Miura
    • 学会等名
      5th Annual Winter Q-Bio Meeting
    • 発表場所
      Koloa, HI, USA
    • 年月日
      2017-02-21 – 2017-02-24
    • 国際学会
  • [学会発表] Single cell analysis of stress signaling dynamics in a life death decision2017

    • 著者名/発表者名
      Haruko Miura
    • 学会等名
      Resonance Bio Work Shop ’17
    • 発表場所
      Okazaki, Japan
    • 年月日
      2017-02-18 – 2017-02-18
  • [学会発表] Single cell analysis of stress signaling dynamics in a life-death decision2016

    • 著者名/発表者名
      Haruko Miura
    • 学会等名
      QBiC Symposium 2016 Decoding Organisms by Quantitative Cell Profiling
    • 発表場所
      Osaka, Japan
    • 年月日
      2016-09-05 – 2016-09-07
  • [学会発表] Single cell analysis of stress signaling dynamics in the life-death decision2016

    • 著者名/発表者名
      Haruko Miura
    • 学会等名
      The 68th Annual Meeting of the Japan Society for Cell Biology
    • 発表場所
      Kyoto, Japan
    • 年月日
      2016-06-15 – 2016-06-17
  • [学会発表] Single cell analysis of stress signaling dynamics in the life-death decision2016

    • 著者名/発表者名
      Haruko Miura
    • 学会等名
      FASEB Science Research Conference Cell Signaling in Cancer: From Mechanisms to Therapy
    • 発表場所
      Snowmass Village, CO, USA
    • 年月日
      2016-06-05 – 2016-06-10
    • 国際学会

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公開日: 2018-01-16  

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