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哺乳類脳神経幹細胞の特性の経時変化を制御するエピゲノム修飾と細胞間シグナルの研究

Research Project

Project/Area Number 15F15083
Research Category

Grant-in-Aid for JSPS Fellows

Allocation TypeSingle-year Grants
Section外国
Research Field Developmental biology
Research InstitutionInstitute of Physical and Chemical Research

Principal Investigator

松崎 文雄  国立研究開発法人理化学研究所, 多細胞システム形成研究センター, チームリーダー (10173824)

Co-Investigator(Kenkyū-buntansha) WU QUAN  国立研究開発法人理化学研究所, 多細胞システム形成研究センター, 外国人特別研究員
Project Period (FY) 2015-07-29 – 2017-03-31
Project Status Completed (Fiscal Year 2016)
Budget Amount *help
¥2,300,000 (Direct Cost: ¥2,300,000)
Fiscal Year 2016: ¥1,100,000 (Direct Cost: ¥1,100,000)
Fiscal Year 2015: ¥1,200,000 (Direct Cost: ¥1,200,000)
Keywords神経発生 / 翻訳調節 / Notchシグナル / RNA メチル基転移酵素 / リボゾーム プロファイリング / 神経幹細胞 / 対称分裂 / 非対称分裂 / エピジェネティクス / 単一遺伝子発現解析
Outline of Annual Research Achievements

In the last year, Wu continued to analyze the function of Fibrillarin in temporal fate change of neural stem cells (NSCs). As a result, Wu found that RNAi-mediated knockdown of Fibrillarin to ~50% at proliferative stage promoted premature neuronal differentiation of NSCs. Consistently, the activity of Notch signaling which is important for self-renewal of NSCs was strongly reduced after knockdown of Fibrillarin. In contrast, overexpression of Fibrillarin increased the population of NSCs. These results suggest that Fibrillarin is essential for proliferation of NSCs. Next, Wu tried to uncover the mechanism by which Fibrillarin affects the fate of NSCs. Because Fibrillarin is a methyltransferase of rRNA and methylation level of rRNA may affect translation, Wu asked that whether knockdown of Fibrillarin affects global protein translation or only impacts on specific targets. Using chemical probe to trace newly synthesized protein, Wu confirmed that RNAi-mediated knockdown of Fibrillarin to ~50% did not affect global protein translation. These results imply that Fibrillarin regulates cell fate through preferentially translating of target mRNAs. Then, to search the targets of Fibrillarin, Wu, cooperating with Dr. Iwasaki Shitano, performed ribosome profiling, a novel method to detect translating mRNAs based on deep-sequencing. Even this experiment is still ongoing, I think that results of this experiment will help us to better understand how NSC fate is precisely controlled. After finish of JSPS fellowship, Wu will continue to complete this project in my lab.

Research Progress Status

28年度が最終年度であるため、記入しない。

Strategy for Future Research Activity

28年度が最終年度であるため、記入しない。

Report

(2 results)
  • 2016 Annual Research Report
  • 2015 Annual Research Report
  • Research Products

    (3 results)

All 2017 2016

All Journal Article (1 results) (of which Int'l Joint Research: 1 results,  Peer Reviewed: 1 results,  Open Access: 1 results,  Acknowledgement Compliant: 1 results) Presentation (2 results)

  • [Journal Article] Sexual Fate Change of XX Germ Cells Caused by the Deletion of SMAD4 and STRA8 Independent of Somatic Sex Reprogramming.2016

    • Author(s)
      Wu Q, Fukuda K, Kato Y, Zhou Z, Deng CX, Saga Y
    • Journal Title

      PLoS Bio

      Volume: 14(9) Issue: 9 Pages: e1002553-e1002553

    • DOI

      10.1371/journal.pbio.1002553

    • Related Report
      2016 Annual Research Report
    • Peer Reviewed / Open Access / Int'l Joint Research / Acknowledgement Compliant
  • [Presentation] Fibrillarin-dependent rRNA methylation couples temporal fate transition of embryonic neural stem cells2017

    • Author(s)
      Quan Wu
    • Organizer
      RIKEN Epigenetics 2017
    • Place of Presentation
      理化学研究所・筑波研究所(茨城県)
    • Related Report
      2016 Annual Research Report
  • [Presentation] Study of Intrinsic clocks controlling temporal identity of neural stem cells2017

    • Author(s)
      Quan Wu
    • Organizer
      RIKEN Single Cell Workshop 2017
    • Place of Presentation
      理化学研究所・横浜研究所(神奈川県)
    • Related Report
      2016 Annual Research Report

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Published: 2015-11-26   Modified: 2024-03-26  

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