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タイトル: Mini-TCRs: Truncated T cell receptors to generate T cells from induced pluripotent stem cells
著者: Takayanagi, Shin-ichiro
Wang, Bo
Hasegawa, Saki
Nishikawa, Satoshi
Fukumoto, Ken
Nakano, Kohei
Chuganji, Sayaka
Kato, Yuya
Kamibayashi, Sanae
Minagawa, Atsutaka
Kunisato, Atsushi
Nozawa, Hajime
Kaneko, Shin  kyouindb  KAKEN_id
著者名の別形: 高柳, 晋一郎
王, 博
長谷川, 早紀
福本, 健
中観寺, 風香
上林, 早苗
南川, 淳隆
金子, 新
発行日: 14-Dec-2023
出版者: Elsevier BV
誌名: Molecular Therapy - Methods & Clinical Development
巻: 31
論文番号: 101109
抄録: Allogeneic T cell platforms utilizing induced pluripotent stem cell (iPSC) technology exhibit significant promise for the facilitation of adoptive immunotherapies. While mature T cell receptor (TCR) signaling plays a crucial role in generating T cells from iPSCs, the introduction of exogenous mature TCR genes carries a potential risk of causing graft-versus-host disease (GvHD). In this study, we present the development of truncated TCRα and TCRβ chains, termed mini-TCRs, which lack variable domains responsible for recognizing human leukocyte antigen (HLA)-peptide complexes. We successfully induced cytotoxic T lymphocytes (CTLs) from iPSCs by employing mini-TCRs. Combinations of TCRα and TCRβ fragments were screened from mini-TCR libraries based on the surface localization of CD3 proteins and their ability to transduce T cell signaling. Consequently, mini-TCR-expressing iPSCs underwent physiological T cell development, progressing from the CD4 and CD8 double-positive stage to the CD8 single-positive stage. The resulting iPSC-derived CTLs exhibited comparable cytokine production and cytotoxicity in comparison to that of full-length TCR-expressing T lymphocytes when chimeric antigen receptors (CARs) were expressed. These findings demonstrate the potential of mini-TCR-carrying iPSCs as a versatile platform for CAR T cell therapy, offering a promising avenue for advancing adoptive immunotherapies.
著作権等: © 2023 The Authors.
This is an open access article under the CC BY license.
URI: http://hdl.handle.net/2433/287380
DOI(出版社版): 10.1016/j.omtm.2023.101109
PubMed ID: 37822720
出現コレクション:学術雑誌掲載論文等

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