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dc.contributor.authorUeda, Tatsukien
dc.contributor.authorShiina, Saraen
dc.contributor.authorIriguchi, Shoichien
dc.contributor.authorTerakura, Seitaroen
dc.contributor.authorKawai, Yoheien
dc.contributor.authorKabai, Ryotaroen
dc.contributor.authorSakamoto, Satokoen
dc.contributor.authorWatanabe, Akiraen
dc.contributor.authorOhara, Koheien
dc.contributor.authorWang, Boen
dc.contributor.authorXu, Huaigengen
dc.contributor.authorMinagawa, Atsutakaen
dc.contributor.authorHotta, Akitsuen
dc.contributor.authorWoltjen, Knuten
dc.contributor.authorUemura, Yasushien
dc.contributor.authorKodama, Yuzoen
dc.contributor.authorSeno, Hiroshien
dc.contributor.authorNakatsura, Tetsuyaen
dc.contributor.authorTamada, Kojien
dc.contributor.authorKaneko, Shinen
dc.contributor.alternative上田, 樹ja
dc.contributor.alternative椎名, 沙羅ja
dc.contributor.alternative入口, 翔一ja
dc.contributor.alternative寺倉, 精太郎ja
dc.contributor.alternative河合, 洋平ja
dc.contributor.alternative樺井, 良太朗ja
dc.contributor.alternative坂本, 智子ja
dc.contributor.alternative渡辺, 亮ja
dc.contributor.alternative小原, 紘平ja
dc.contributor.alternative王, 博ja
dc.contributor.alternative南川, 淳隆ja
dc.contributor.alternative堀田, 秋津ja
dc.contributor.alternative植村, 靖史ja
dc.contributor.alternative児玉, 裕三ja
dc.contributor.alternative妹尾, 浩ja
dc.contributor.alternative中面, 哲也ja
dc.contributor.alternative玉田, 耕治ja
dc.contributor.alternative金子, 新ja
dc.date.accessioned2023-01-24T02:00:10Z-
dc.date.available2023-01-24T02:00:10Z-
dc.date.issued2023-01-
dc.identifier.urihttp://hdl.handle.net/2433/278799-
dc.descriptionCARシグナルを補完する遺伝子改変により *iCAR-T細胞の固形がん治療効果が改善される. 京都大学プレスリリース. 2022-12-13.ja
dc.descriptionGenetic modifications boosting CAR signaling improve the therapeutic efficacy of iPSC-derived CAR-T cells against solid tumors. 京都大学プレスリリース. 2022-12-13.en
dc.description.abstractThe effectiveness of chimaeric antigen receptor (CAR) T-cell immunotherapies against solid tumours relies on the accumulation, proliferation and persistency of T cells at the tumour site. Here we show that the proliferation of CD8αβ cytotoxic CAR T cells in solid tumours can be enhanced by deriving and expanding them from a single human induced-pluripotent-stem-cell clone bearing a CAR selected for efficient differentiation. We also show that the proliferation and persistency of the effector cells in the tumours can be further enhanced by genetically knocking out diacylglycerol kinase, which inhibits antigen-receptor signalling, and by transducing the cells with genes encoding for membrane-bound interleukin-15 (IL-15) and its receptor subunit IL-15Rα. In multiple tumour-bearing animal models, the engineered hiPSC-derived CAR T cells led to therapeutic outcomes similar to those of primary CD8 T cells bearing the same CAR. The optimization of effector CAR T cells derived from pluripotent stem cells may aid the development of long-lasting antigen-specific T-cell immunotherapies for the treatment of solid tumours.en
dc.language.isoeng-
dc.publisherSpringer Natureen
dc.rights© The Author(s) 2022en
dc.rightsThis article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder.en
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/-
dc.subjectCancer immunotherapyen
dc.subjectStem-cell biotechnologyen
dc.titleOptimization of the proliferation and persistency of CAR T cells derived from human induced pluripotent stem cellsen
dc.typejournal article-
dc.type.niitypeJournal Article-
dc.identifier.jtitleNature Biomedical Engineeringen
dc.identifier.volume7-
dc.identifier.issue1-
dc.identifier.spage24-
dc.identifier.epage37-
dc.relation.doi10.1038/s41551-022-00969-0-
dc.textversionpublisher-
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto University; Department of Gastroenterology and Hepatology, Kyoto University Graduate School of Medicineen
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto University; Takeda-CiRA Joint Program (T-CiRA)en
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto University; Takeda-CiRA Joint Program (T-CiRA)en
dc.addressDepartment of Hematology and Oncology, Nagoya University Graduate School of Medicineen
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto Universityen
dc.addressMedical Innovation Center, Kyoto University Graduate School of Medicineen
dc.addressMedical Innovation Center, Kyoto University Graduate School of Medicineen
dc.addressMedical Innovation Center, Kyoto University Graduate School of Medicineen
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto Universityen
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto University; Takeda-CiRA Joint Program (T-CiRA)en
dc.addressDepartment of Clinical Application, Center for iPS Cell Research and Application (CiRA), Kyoto Universityen
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto Universityen
dc.addressDepartment of Clinical Application, Center for iPS Cell Research and Application (CiRA), Kyoto Universityen
dc.addressDepartment of Life Science Frontiers, Center for iPS Cell Research and Application (CiRA), Kyoto Universityen
dc.addressDivision of Cancer Immunotherapy, Exploratory Oncology Research and Clinical Trial Center, National Cancer Centeren
dc.addressDepartment of Gastroenterology, Kobe University Graduate School of Medicineen
dc.addressDepartment of Gastroenterology and Hepatology, Kyoto University Graduate School of Medicineen
dc.addressDivision of Cancer Immunotherapy, Exploratory Oncology Research and Clinical Trial Center, National Cancer Centeren
dc.addressDepartment of Immunology, Yamaguchi University Graduate School of Medicineen
dc.addressShin Kaneko Laboratory, Department of Cell Growth and Differentiation, Center for iPS Cell Research and Application (CiRA), Kyoto University; Takeda-CiRA Joint Program (T-CiRA)en
dc.identifier.pmid36509913-
dc.relation.urlhttps://www.cira.kyoto-u.ac.jp/j/pressrelease/news/221213-010000.html-
dc.relation.urlhttps://www.cira.kyoto-u.ac.jp/e/pressrelease/news/221213-170000.html-
dcterms.accessRightsopen access-
dc.identifier.eissn2157-846X-
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