Literature DB >> 33457097

Generation of GM-CSF-producing antigen-presenting cells that induce a cytotoxic T cell-mediated antitumor response.

Hiroaki Mashima1,2, Rong Zhang1, Tsuyoshi Kobayashi2, Yuichiro Hagiya3, Hirotake Tsukamoto4, Tianyi Liu5, Tatsuaki Iwama1, Masateru Yamamoto1,2, Chiahsuan Lin1, Ryusuke Nakatsuka6, Yuta Mishima7, Noriko Watanabe8, Takashi Yamada8, Satoru Senju9, Shin Kaneko7, Alimjan Idiris3, Tetsuya Nakatsura1, Hideki Ohdan2, Yasushi Uemura1.   

Abstract

Immunotherapy using dendritic cells (DCs) is a promising treatment modality for cancer. However, the limited number of functional DCs from peripheral blood has been linked to the unsatisfactory clinical efficacies of current DC-based cancer immunotherapies. We previously generated proliferating antigen-presenting cells (APCs) by genetically engineering myeloid cells derived from induced pluripotent stem cells (iPSC-pMCs), which offer infinite functional APCs for broad applications in cancer therapy. Herein, we aimed to further enhance the antitumor effect of these cells by genetic modification. GM-CSF gene transfer did not affect the morphology, or surface phenotype of the original iPSC-pMCs, however, it did impart good viability to iPSC-pMCs. The resultant cells induced GM-CSF-dependent CD8+ T cell homeostatic proliferation, thereby enhancing antigen-specific T cell priming in vitro. Administration of the tumor antigen-loaded GM-CSF-producing iPSC-pMCs (GM-pMCs) efficiently stimulated antigen-specific T cells and promoted effector cell infiltration of the tumor tissues, leading to an augmented antitumor effect. To address the potential tumorigenicity of iPSC-derived products, irradiation was applied and found to restrict the proliferation of GM-pMCs, while retaining their T cell-stimulatory capacity. Furthermore, the irradiated cells exerted an antitumor effect equivalent to that of bone marrow-derived DCs obtained from immunocompetent mice. Additionally, combination with immune checkpoint inhibitors increased the infiltration of CD8+ or NK1.1+ effector cells and decreased CD11b+/Gr-1+ cells without causing adverse effects. Hence, although GM-pMCs have certain characteristics that differ from endogenous DCs, our findings suggest the applicability of these cells for broad clinical use and will provide an unlimited source of APCs with uniform quality.
© 2020 The Author(s). Published with license by Taylor & Francis Group, LLC.

Entities:  

Keywords:  Cancer immunotherapy; GM-CSF; cancer vaccine; dendritic cell; induced pluripotent stem cell

Mesh:

Substances:

Year:  2020        PMID: 33457097      PMCID: PMC7781730          DOI: 10.1080/2162402X.2020.1814620

Source DB:  PubMed          Journal:  Oncoimmunology        ISSN: 2162-4011            Impact factor:   8.110


  54 in total

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Authors:  Rong Zhang; Tian-Yi Liu; Satoru Senju; Miwa Haruta; Narumi Hirosawa; Motoharu Suzuki; Minako Tatsumi; Norihiro Ueda; Hiroyuki Maki; Ryusuke Nakatsuka; Yoshikazu Matsuoka; Yutaka Sasaki; Shinobu Tsuzuki; Hayao Nakanishi; Ryoko Araki; Masumi Abe; Yoshiki Akatsuka; Yasushi Sakamoto; Yoshiaki Sonoda; Yasuharu Nishimura; Kiyotaka Kuzushima; Yasushi Uemura
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Journal:  Cell Stem Cell       Date:  2018-02-15       Impact factor: 24.633

Review 7.  Granulocyte-macrophage colony-stimulating factor (GM-CSF) and T-cell responses: what we do and don't know.

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9.  Moderated estimation of fold change and dispersion for RNA-seq data with DESeq2.

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10.  Immune cell dysfunctions in breast cancer patients detected through whole blood multi-parametric flow cytometry assay.

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3.  Improved safety of induced pluripotent stem cell-derived antigen-presenting cell-based cancer immunotherapy.

Authors:  Hiroaki Mashima; Rong Zhang; Tsuyoshi Kobayashi; Hirotake Tsukamoto; Tianyi Liu; Tatsuaki Iwama; Yuichiro Hagiya; Masateru Yamamoto; Satoshi Fukushima; Seiji Okada; Alimjan Idiris; Shin Kaneko; Tetsuya Nakatsura; Hideki Ohdan; Yasushi Uemura
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