2017 Fiscal Year Annual Research Report

Eliminating residual undifferentiated cells from iPSC-CMs for safer clinical application of iPSCs

Research Project

Project/Area Number	15K10211
Research Institution	Osaka University
Principal Investigator	増田茂夫大阪大学, 医学系研究科, 特任准教授(常勤) (10396749)
Project Period (FY)	2015-04-01 – 2018-03-31
Keywords	ヒトiPS細胞 / 造腫瘍性 / 未分化細胞除去 / 分子標的治療薬
Outline of Annual Research Achievements	ヒトiPS細胞を利用した再生医療の実現に際し、安全性担保、特に腫瘍形成回避が必要条件となる。本研究ではiPS細胞由来未分化細胞を除去することを目的とし、種々の分子標的阻害剤によるex vivo purgingを試みた。まずヒトiPS細胞を対象にEpigenetic修飾薬であるBET阻害剤(JQ1)を添加したところ、同剤が強力なNanog阻害剤として作用することを確認した。次にヒトiPS由来心筋細胞をin vitroで同Nanog阻害剤処理したところ、残存未分化細胞 (Lin28 or TRA-1-60陽性細胞)が効率的に除去されることが判明した。一方ヒトiPS由来心筋細胞はintactであり、選択的標的化が示唆された。さらに未分化細胞除去効果に関し、より深い効果を目指して分子標的阻害剤のスクリーニングを行った結果、CDK阻害剤 (CDK9 or CDK1阻害剤)がBET阻害剤 (Nanog阻害剤)と共に相乗効果を呈することを見出した。BET蛋白BRD4は転写complex (P-TEFb)を形成している。同complexはBRD4の他、CDK9やCYCLIN Tから成ることから、より深いNanog抑制効果が相乗効果を説明すると予想される。さらに近年開発されたPROTACという化合物で、プロテアソーム系で標的タンパク質を特異的に分解する低分子化合物を用いて未分化細胞除去を検証した。BETタンパク質BRD4を標的にしたBRD4 PROTACを用いた結果、BET阻害剤(JQ1)とほぼ同等の高い効果が確認された。本研究で使用された(PROTACを除く)分子標的阻害剤の多くは種々の癌でPhase II試験施行中であり、今後、“ヒトiPS細胞”を対象とした分子標的治療薬としての可能性が示唆された。

Research Products
(10 results)

All 2018 2017

All Journal Article (3 results) (of which Int'l Joint Research: 3 results, Peer Reviewed: 3 results, Open Access: 1 results) Presentation (5 results) (of which Int'l Joint Research: 2 results) Book (2 results)

[Journal Article] Pivotal role of non-cardiomyocytes in electromechanical and therapeutic potential of induced pluripotent stem cell-derived engineered cardiac tissue.2018
- Author(s)
  Iseoka H, Miyagawa S, Fukushima S, Saito A, Masuda S, Yajima S, Ito E, Sougawa N, Takeda M, Harada A, Lee JK, Sawa Y.
- Journal Title
  
  Tissue Eng Part A.
  
  Volume: 24(3-4) Pages: 287-300
- DOI
  10.1089/ten.TEA.2016.0535.
- Peer Reviewed / Int'l Joint Research
[Journal Article] Atherosclerosis: Caused by Mutated Old Blood Cells.2017
- Author(s)
  Masuda S.
- Journal Title
  
  Ann Cardiol Cardiovasc Med.
  
  Volume: 1(1) Pages: 1002
- Peer Reviewed / Open Access / Int'l Joint Research
[Journal Article] A Highly Durable RNAi Therapeutic Inhibitor of PCSK9.2017
- Author(s)
  Masuda S, Miyagawa S, Sawa Y.
- Journal Title
  
  N Engl J Med.
  
  Volume: 376(18) Pages: e38
- DOI
  10.1056/NEJMc1703361.
- Peer Reviewed / Int'l Joint Research
[Presentation] Novel PROTAC-induced BET Protein Degradation is Potent in Ex Vivo Purging of Tumorigenic Cells from iPSC-derived Cardiomyocytes.2018
- Author(s)
  Masuda S, Miyagawa S, Kawaguchi K, Nishitani M, Ishikawa T, Saito A, Sawa Y.
- Organizer
  第82回日本循環器学会学術総会
[Presentation] Novel Factors that Evaluate Safety in iPSC-derived Cardiomyocytes Contaminated with Tumorigenic Cells.2018
- Author(s)
  Masuda S, Miyagawa S, Nishitani M, Kawaguchi K, Ishikawa T, Saito A, Sawa Y.
- Organizer
  第82回日本循環器学会学術総会
[Presentation] Eliminating Residual Undifferentiated Cells from iPSC-derived Cardiomyocytes by Heat Shock Protein 90 Inhibitors in Collaboration with Proteasome Inhibitor.2018
- Author(s)
  Masuda S, Miyagawa S, Nishitani M, Kawaguchi K, Ishikawa T, Saito A, Sawa Y.
- Organizer
  第82回日本循環器学会学術総会
[Presentation] Eliminating Residual Undifferentiated Cells from Human iPS-derived Products by Heat Shock Protein 90 Inhibitors.2017
- Author(s)
  Masuda S, Miyagawa S, Khurram MA, Kawaguchi K, Ishikawa T, Saito A, Sawa Y.
- Organizer
  15th International Society for Stem Cell Research: Annual Meeting
- Int'l Joint Research
[Presentation] Novel Candidate Markers for Evaluating Safety in iPSC-derived Cardiomyocytes Contaminated with Tumorigenic Cells.2017
- Author(s)
  Masuda S, Miyagawa S, Nakamura T, Nishitani M, Kawaguchi K, Ishikawa T, Saito A, Sawa Y.
- Organizer
  American Heart Association Scientific Sessions 2017
- Int'l Joint Research
[Book] 腫瘍内科　「Notchシグナル阻害剤」2018
- Author(s)
  増田茂夫
- Total Pages
  7ページ
- Publisher
  科学評論社
- ISBN
  -
[Book] 日本再生医療学会雑誌2017
- Author(s)
  増田茂夫、宮川繁、澤芳樹
- Total Pages
  1ページ
- Publisher
  メディカルレビュー社
- ISBN
  978-4-7792-1999-3

2017 Fiscal Year Annual Research Report

Eliminating residual undifferentiated cells from iPSC-CMs for safer clinical application of iPSCs

Principal Investigator

増田 茂夫 大阪大学, 医学系研究科, 特任准教授(常勤) (10396749)

Research Products

[Journal Article] Pivotal role of non-cardiomyocytes in electromechanical and therapeutic potential of induced pluripotent stem cell-derived engineered cardiac tissue.2018

Author(s)

Journal Title

DOI

[Journal Article] Atherosclerosis: Caused by Mutated Old Blood Cells.2017

Author(s)

Journal Title

[Journal Article] A Highly Durable RNAi Therapeutic Inhibitor of PCSK9.2017

Author(s)

Journal Title

DOI

[Presentation] Novel PROTAC-induced BET Protein Degradation is Potent in Ex Vivo Purging of Tumorigenic Cells from iPSC-derived Cardiomyocytes.2018

Author(s)

Organizer

[Presentation] Novel Factors that Evaluate Safety in iPSC-derived Cardiomyocytes Contaminated with Tumorigenic Cells.2018

Author(s)

Organizer

[Presentation] Eliminating Residual Undifferentiated Cells from iPSC-derived Cardiomyocytes by Heat Shock Protein 90 Inhibitors in Collaboration with Proteasome Inhibitor.2018

Author(s)

Organizer

[Presentation] Eliminating Residual Undifferentiated Cells from Human iPS-derived Products by Heat Shock Protein 90 Inhibitors.2017

Author(s)

Organizer

[Presentation] Novel Candidate Markers for Evaluating Safety in iPSC-derived Cardiomyocytes Contaminated with Tumorigenic Cells.2017

Author(s)

Organizer

[Book] 腫瘍内科 「Notchシグナル阻害剤」2018

Author(s)

Total Pages

Publisher

ISBN

[Book] 日本再生医療学会雑誌2017

Author(s)

Total Pages

Publisher

ISBN

増田茂夫大阪大学, 医学系研究科, 特任准教授(常勤) (10396749)

[Book] 腫瘍内科　「Notchシグナル阻害剤」2018