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Construction of a natural product library composed of azepine alkaloids and determination of their absolute configuration by VCD spectroscopy.

Research Project

Project/Area Number 16K08308
Research Category

Grant-in-Aid for Scientific Research (C)

Allocation TypeMulti-year Fund
Section一般
Research Field Natural medicines
Research InstitutionTokyo University of Pharmacy and Life Science

Principal Investigator

HITOTSUYANAGI Yukio  東京薬科大学, 薬学部, 教授 (80218726)

Research Collaborator FUKAYA Haruhiko  
Project Period (FY) 2016-10-21 – 2019-03-31
Project Status Completed (Fiscal Year 2018)
Budget Amount *help
¥3,640,000 (Direct Cost: ¥2,800,000、Indirect Cost: ¥840,000)
Fiscal Year 2018: ¥780,000 (Direct Cost: ¥600,000、Indirect Cost: ¥180,000)
Fiscal Year 2017: ¥780,000 (Direct Cost: ¥600,000、Indirect Cost: ¥180,000)
Fiscal Year 2016: ¥2,080,000 (Direct Cost: ¥1,600,000、Indirect Cost: ¥480,000)
Keywords赤外円二色性スペク トル / 化合物ライブラリ / アルカロイド / 環状ペプチド / 密度汎関数理論 / Stemona tuberosa / Rubia cordifolia / VCD / N-オキシド / 密度汎関数法 / 中分子 / ステモナアルカロイド / DFT / 配座探索 / アゼピンアルカロイド / VCDスペクトル / 化合物ライブラリー / Stemona
Outline of Final Research Achievements

Eleven new alkaloids were isolated from the roots of Stemona tuberosa to create a natural products library composed of alkaloids possessing an azepine ring, which is often found in the structures of important synthetic drugs. I found conditions to convert the chemically labile azepine alkaloid into its stable N-oxide to restrict the conformational freedom of the parent alkaloid. Vibrational circular dichroism (VCD) spectroscopy was applied to determine the absolute configuration of RA-VII, a bicyclic hexapeptide with an 18-membered ring, indicating that the VCD spectroscopy is applicable to macrocyclic peptides. Three new RA-series cyclopeptide alkaloids were isolated from the roots of Rubia cordifolia and their structures were determined. Conformational analysis and the DFT calculation of those new peptides revealed that the N-methyl group at Tyr-5 is important for RA-VII to preferentially adopt the active conformation.

Academic Significance and Societal Importance of the Research Achievements

Stemona tuberosaより見出したアゼピン骨格を有する新規アルカロイド類はいずれも新奇性の高いユニークな構造を有しており、医薬品開発の活性スクリーニングに供する構造多様性に富む天然化合物ライブラリーを構築するうえで、重要度が高い構成要素となるものである。また、赤外円二色性スペクトル法を分子量の大きいマクロ環状ペプチドアルカロイドに適応し、非晶質性中分子化合物の絶対配置決定に本法が応用できることを示した。

Report

(4 results)
  • 2018 Annual Research Report   Final Research Report ( PDF )
  • 2017 Research-status Report
  • 2016 Research-status Report
  • Research Products

    (9 results)

All 2019 2018 2017 2016

All Journal Article (2 results) (of which Peer Reviewed: 2 results) Presentation (7 results)

  • [Journal Article] RA-XXV and RA-XXVI, bicyclic hexapeptides from Rubia cordifolia L.: Structure, synthesis, and conformation2019

    • Author(s)
      Hitotsuyanagi, Yukio; Hirai, Masahito; Odagiri, Masumi; Komine, Miho; Hasuda, Tomoyo; Fukaya, Haruhiko; Takeya, Koichi
    • Journal Title

      Chemistry - An Asian Journal

      Volume: 14 Issue: 1 Pages: 205-215

    • DOI

      10.1002/asia.201801466

    • Related Report
      2018 Annual Research Report
    • Peer Reviewed
  • [Journal Article] Stemona-amines F and G, new alkaloids from Stemona tuberosa2016

    • Author(s)
      Yukio Hitotsuyanagi, Yoshiyuki Sekiya, Haruhiko Fukaya, Hyun Sun Park, Shu Zhu, Katsuko Komatsu
    • Journal Title

      Tetrahedron Letters

      Volume: 57 Issue: 51 Pages: 5746-5749

    • DOI

      10.1016/j.tetlet.2016.10.096

    • Related Report
      2016 Research-status Report
    • Peer Reviewed
  • [Presentation] タマビャクブ (Stemona tuberosa) から得られたアルカロイドの構造と生物活性について2019

    • Author(s)
      松原 七海, 朴 炫宣, 深谷 晴彦, Zhu Shu, 小松 かつ子, 一栁 幸生
    • Organizer
      日本薬学会 第139年会
    • Related Report
      2018 Annual Research Report
  • [Presentation] 茜草根より単離したフェニルプロパノイド単位を持つRA 系ペプチド化合物の構造(II)2019

    • Author(s)
      深谷 晴彦, 一栁 幸生, 安斉 竜郎, 蓮田 知代, 青柳 裕
    • Organizer
      日本薬学会 第139年会
    • Related Report
      2018 Annual Research Report
  • [Presentation] ビャクブコンから得られた新規 stenine 型および croomine 型アルカロイドについて2018

    • Author(s)
      深谷 晴彦,一栁 幸生,Zhu Shu,小松 かつ子
    • Organizer
      日本生薬学会 第65回年会
    • Related Report
      2018 Annual Research Report
  • [Presentation] 茜草根より単離したフェニルプロパノイド単位を持つ RA 系ペプチド化合物の構造 (I)2018

    • Author(s)
      深谷晴彦,一栁幸生,安斉竜郎,青柳裕
    • Organizer
      日本薬学会 第138年会
    • Related Report
      2017 Research-status Report
  • [Presentation] Stemona tuberosaから得られる新規アルカロイドに関する構造研究2017

    • Author(s)
      松原 雅生,朴 炫宣,深谷 晴彦,一栁 幸生
    • Organizer
      日本薬学会第137年会
    • Place of Presentation
      富山
    • Year and Date
      2017-03-24
    • Related Report
      2016 Research-status Report
  • [Presentation] 抗腫瘍性環状ペプチドRA-VIIのVCDスペクトル2017

    • Author(s)
      深谷 晴彦,一栁 幸生,青柳 裕
    • Organizer
      日本薬学会第137年会
    • Place of Presentation
      仙台
    • Year and Date
      2017-03-24
    • Related Report
      2016 Research-status Report
  • [Presentation] 茜草根由来新規RA系ペプチド化合物の構造2017

    • Author(s)
      一栁幸生,平井聖仁,小田切増美,深谷晴彦,蓮田知代,竹谷孝一
    • Organizer
      日本生薬学会 第64回年会
    • Related Report
      2017 Research-status Report

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Published: 2016-10-24   Modified: 2020-03-30  

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