Chemical biology of MDR cancer selective cytotoxicity using natural product derivatives

• Project/Area Number: 25670054
• Research Category: Grant-in-Aid for Challenging Exploratory Research
• Allocation Type: Multi-year Fund
• Research Field: Drug development chemistry
• Research Institution: Kanazawa University
• Principal Investigator: Goto Kyoko 金沢大学, 薬学系, 准教授 (50180245)
• Co-Investigator(Renkei-kenkyūsha): TAMAI Ikumi 金沢大学, 医薬保健研究域薬学系, 教授 (20155237)
• Research Collaborator: GOTO Masuo University of North Carolina at Chapel Hill, Eshelman School of Pharmacy, Research Professor
• Project Period (FY): 2013-04-01 – 2016-03-31
• Project Status: Completed (Fiscal Year 2015)
• Budget Amount: ¥3,900,000 (Direct Cost: ¥3,000,000、Indirect Cost: ¥900,000); Fiscal Year 2015: ¥1,170,000 (Direct Cost: ¥900,000、Indirect Cost: ¥270,000); Fiscal Year 2014: ¥1,560,000 (Direct Cost: ¥1,200,000、Indirect Cost: ¥360,000); Fiscal Year 2013: ¥1,170,000 (Direct Cost: ¥900,000、Indirect Cost: ¥270,000)
• Keywords: フラボノイド / TEDB / 多剤耐性がん / Collateral sensitivity / 多剤耐性がん細胞 / フラボノイド誘導体 / 異所性P-糖タンパク / 有糸分裂阻害効果

Outline of Final Research Achievements

TEDB, a derivative of natural flavonoid desmosdumotin B, selectively inhibits multidrug resistant (MDR) tumor cell growth without any cytotoxicity against normal cells as well as non-MDR cells. Despite its unique antiproliferative activity, the mechanism of action is totally unclear. Using medicinal chemistry as well as chemical biological approaches of TEDB derivatives, we have discovered that TEDB with an artificial benzothiophene ring-B system induced a unique antimitotic bioactivity. The resulting antimitotic agent showed a wide spectrum against multiple cancer cell lines including MDR cells. Based on this finding, a series of new antimitotic flavonoids was designed and synthesized. We have also identified a cellular protein overexpressed in MDR cells as a novel candidate for overcoming MDR tumor using TEDB derivatives.

Research Products

• [Int'l Joint Research] ノースカロライナ大学/米国国立がん研究所(米国)
• [Int'l Joint Research] 国立台湾大学(台湾)
• [Journal Article] Development of a novel class of tubulin inhibitor from desmosdumotin B with a hydroxylated bicyclic B-ring (2015)
  • Author(s): Nakagawa-Goto K, Oda A, Hamel E, Ohkoshi E, Bastow KF, Lee KH, Goto M
  • Journal Title: J Med Chem Volume: 58 Issue: 5 Pages: 2378-2389
  • DOI: 10.1021/jm501859j
  • Peer Reviewed / Acknowledgement Compliant
• [Presentation] ベンゾチオフェンフラボノイド誘導体の抗腫瘍活性と構造活性相関 (2016)
  • Author(s): 谷口由花子、釣本浩行、斎藤洋平、後藤益生、後藤（中川）享子
  • Organizer: 日本薬学会第136年会
  • Place of Presentation: 横浜
  • Year and Date: 2016-03-27
• [Presentation] TEDB-TB窒素置換誘導体の合成と抗腫瘍活性評価 (2016)
  • Author(s): 小林佑希子、斎藤洋平、後藤益生、後藤（中川）享子
  • Organizer: 日本薬学会第136年会
  • Place of Presentation: 横浜
  • Year and Date: 2016-03-27
• [Presentation] Benzothiophenyl flavones as new classes of mitotic inhibitors (2015)
  • Author(s): Taniguchi Y, Tsurimoto H, Saito Y, Hamel E, Goto M, Nakagawa-Goto K
  • Organizer: 250th ACS National Meeting & Exposition
  • Place of Presentation: アメリカ、ボストン
  • Year and Date: 2015-08-16
  • Int'l Joint Research
• [Presentation] 新規抗腫瘍活性ベンゾチオフェンフラボノイドの合成と構造活性相関研究 (2015)
  • Author(s): 谷口由花子、釣本浩行、齋藤洋平、後藤益生、後藤（中川）享子
  • Organizer: 日本薬学会第135年会
  • Place of Presentation: 神戸
  • Year and Date: 2015-03-26 – 2015-03-28
  • Invited
• [Presentation] TEDB-TB Analogs as New Classes of Tubulin Inhibitors (2013)
  • Author(s): 後藤享子
  • Organizer: 第246回アメリカ化学会ナショナルミーティング
  • Place of Presentation: インディアナポリス、アメリカ