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Regulatory mechanisms of the leukemia-associated transcription factor, RUNX1/AML1, through the post-translational modifications.

Research Project

Project/Area Number 24591408
Research Category

Grant-in-Aid for Scientific Research (C)

Allocation TypeMulti-year Fund
Section一般
Research Field Hematology
Research InstitutionKyoto Prefectural University of Medicine

Principal Investigator

TSUKASA Okuda  京都府立医科大学, 医学(系)研究科(研究院), 教授 (30291587)

Co-Investigator(Kenkyū-buntansha) SAKAKURA Chouhei  京都府立医科大学, 大学院医学研究科, 准教授 (10285257)
Project Period (FY) 2012-04-01 – 2015-03-31
Project Status Completed (Fiscal Year 2014)
Budget Amount *help
¥5,460,000 (Direct Cost: ¥4,200,000、Indirect Cost: ¥1,260,000)
Fiscal Year 2014: ¥1,820,000 (Direct Cost: ¥1,400,000、Indirect Cost: ¥420,000)
Fiscal Year 2013: ¥1,820,000 (Direct Cost: ¥1,400,000、Indirect Cost: ¥420,000)
Fiscal Year 2012: ¥1,820,000 (Direct Cost: ¥1,400,000、Indirect Cost: ¥420,000)
Keywords白血病 / 造血幹細胞 / リンパ球 / 転写因子 / 翻訳後修飾 / RUNX1 / AML1 / マウスモデル / Runx1 / ES細胞 / 遺伝子改変マウス / 造血 / ノックイン
Outline of Final Research Achievements

RUNX1 is a leukemia-associated transcription factor that functions in hematopoietic development, proliferation, and differentiation. In this study, biological significance of the methylation of two arginine residues (R206/210) was analyzed. To this end, we made mutant RUNX1 in which both R206 and R210 were substituted to lysine (K) that cannot be methylated by the responsible enzyme. Although this non-methylable mutant protein showed somewhat reduced trans-activating activity in vitro, it still retained the biological ability to rescue the hematopoietic defect found in Runx1-deficient murine ES cells. In addition, engineered mice that homozygously carry these R-to-K mutations showed no obvious defects in myeloid, meg/platelet, or B-cell lineages. However, the mutant mice showed reduced number for CD4-single positive T-cells for peripheral blood and spleen. Thus, our results revealed that methylation of Runx1 is important for homeostasis of the peripheral CD4+ lymphocyte population.

Report

(4 results)
  • 2014 Annual Research Report   Final Research Report ( PDF )
  • 2013 Research-status Report
  • 2012 Research-status Report
  • Research Products

    (15 results)

All 2015 2014 2013 Other

All Journal Article (4 results) (of which Peer Reviewed: 1 results,  Acknowledgement Compliant: 1 results) Presentation (11 results)

  • [Journal Article] Loss of RUNX1/AML1 arginine-methylation impairs peripheral T cell homeostasis.2015

    • Author(s)
      Mizutani S, Yoshida T, Zhao X, Nimer SD, Taniwaki M, and Okuda T.
    • Journal Title

      British Journal of Haematology

      Volume: 印刷中

    • Related Report
      2014 Annual Research Report
    • Peer Reviewed / Acknowledgement Compliant
  • [Journal Article] 血管内皮細胞による造血幹細胞の維持.2014

    • Author(s)
      山元康敏、奥田 司
    • Journal Title

      血液内科

      Volume: 69 Pages: 309-320

    • Related Report
      2014 Annual Research Report
  • [Journal Article] 血球発生と血管分化のcrossroad2013

    • Author(s)
      山元康敏、奥田 司
    • Journal Title

      京都府立医科大学雑誌

      Volume: 122 Pages: 329-340

    • Related Report
      2013 Research-status Report
  • [Journal Article] 血球発生と血管分化のcrossroad2013

    • Author(s)
      山元康敏
    • Journal Title

      京都府立医科大学雑誌

      Volume: 掲載予定

    • Related Report
      2012 Research-status Report
  • [Presentation] AML1/Runx1機能制御に関わる新規共役因子の解析.2014

    • Author(s)
      吉田達士, 中村加世子, 水谷信介, 奥田 司.
    • Organizer
      第87回日本生化学会大会
    • Place of Presentation
      京都
    • Year and Date
      2014-10-16
    • Related Report
      2014 Annual Research Report
  • [Presentation] A candidate co-factor which regulates acute myeloid leukemia 1/runt-related transcription factor 1 (AML1/Runx1) function.2014

    • Author(s)
      Yoshida T, and Okuda T.
    • Organizer
      第73回日本癌学会学術総会
    • Place of Presentation
      横浜
    • Year and Date
      2014-09-27
    • Related Report
      2014 Annual Research Report
  • [Presentation] A cellular and molecular analysis for endothelial/mesenchymal plasticity.2013

    • Author(s)
      Yamamoto Y, Prince LS, Okuda T.
    • Organizer
      第86回日本生化学会大会
    • Place of Presentation
      横浜
    • Related Report
      2013 Research-status Report
  • [Presentation] AML1アルギニンメチル化の喪失は末梢T細胞集団の不均衡を惹起する2013

    • Author(s)
      水谷信介、谷脇雅史、奥田 司
    • Organizer
      第75回日本血液学会学術集会
    • Place of Presentation
      札幌
    • Related Report
      2013 Research-status Report
  • [Presentation] 間葉細胞/血管内皮分化過程を解析可能な新規細胞培養システムの構築2013

    • Author(s)
      山元康敏、Prince LS, 奥田 司
    • Organizer
      第3回 4大学連携研究フォーラム
    • Place of Presentation
      京都
    • Related Report
      2013 Research-status Report
  • [Presentation] Fetal lung vascular progenitor cells exhibit endothelial/mesenchymal plasticity

    • Author(s)
      Yamamoto Y
    • Organizer
      14th International congress of histochemistry and cytochemistry
    • Place of Presentation
      京都
    • Related Report
      2012 Research-status Report
  • [Presentation] Biological significance of AML1 arginine-methylation revealed by generation of targeted-knock-in mice.

    • Author(s)
      Mizutani S
    • Organizer
      第71回日本癌学会学術総会
    • Place of Presentation
      札幌
    • Related Report
      2012 Research-status Report
  • [Presentation] Generation of genome-modified mouse lines which carry knocked-in allele for AML1 arginine-mutant.

    • Author(s)
      Mizutani S
    • Organizer
      第74回日本血液学会学術集会
    • Place of Presentation
      京都
    • Related Report
      2012 Research-status Report
  • [Presentation] A Gene-Targeting Approach for the Biological Significance of AML1/Runx1 Arginine-Methylation.

    • Author(s)
      Mizutani S
    • Organizer
      第54回米国血液学会年次総会
    • Place of Presentation
      アトランタ、米国
    • Related Report
      2012 Research-status Report
  • [Presentation] ジーンターゲティングアプローチによるAML1のアルギニンメチル化修飾の生物学的意義の検討.

    • Author(s)
      水谷信介
    • Organizer
      第85回日本生化学会大会
    • Place of Presentation
      博多
    • Related Report
      2012 Research-status Report
  • [Presentation] A novel cell culture model for endothelial/mesenchymal plasticity.

    • Author(s)
      Yamamoto Y
    • Organizer
      第85回日本生化学会大会
    • Place of Presentation
      博多
    • Related Report
      2012 Research-status Report

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Published: 2013-05-31   Modified: 2019-07-29  

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