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OX40 ligand expressed in glioblastoma modulates adaptive immunity depending on the microenvironment : a clue for successful immunotherapy

http://hdl.handle.net/20.500.12000/45952
http://hdl.handle.net/20.500.12000/45952
e7901fe3-c78c-4028-a7f1-9bc836ccdfc4
名前 / ファイル ライセンス アクション
s12943-015-0307-3.pdf s12943-015-0307-3.pdf
Item type デフォルトアイテムタイプ(フル)(1)
公開日 2020-05-29
タイトル
タイトル OX40 ligand expressed in glioblastoma modulates adaptive immunity depending on the microenvironment : a clue for successful immunotherapy
言語 en
作成者 Shibahara, Ichiyo

× Shibahara, Ichiyo

en Shibahara, Ichiyo
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Saito, Ryuta

× Saito, Ryuta

en Saito, Ryuta
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Zhang, Rong

× Zhang, Rong

en Zhang, Rong
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Chonan, Masashi

× Chonan, Masashi

en Chonan, Masashi
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Shoji, Takuhiro

× Shoji, Takuhiro

en Shoji, Takuhiro
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Kanamori, Masayuki

× Kanamori, Masayuki

en Kanamori, Masayuki
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Sonoda, Yukihiko

× Sonoda, Yukihiko

en Sonoda, Yukihiko
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Kumabe, Toshihiro

× Kumabe, Toshihiro

en Kumabe, Toshihiro
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Kanehira, Masahiko

× Kanehira, Masahiko

en Kanehira, Masahiko
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Kikuchi, Toshiaki

× Kikuchi, Toshiaki

en Kikuchi, Toshiaki
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So, Takanori

× So, Takanori

en So, Takanori
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Watanebe, Takashi

× Watanebe, Takashi

en Watanebe, Takashi
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Takahashi, Hiroaki

× Takahashi, Hiroaki

en Takahashi, Hiroaki
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Iwabuchi, Erina

× Iwabuchi, Erina

en Iwabuchi, Erina
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Tanaka, Yuetsu

× Tanaka, Yuetsu

en Tanaka, Yuetsu
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Shibahara, Yukiko

× Shibahara, Yukiko

en Shibahara, Yukiko
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Sasano, Hironobu

× Sasano, Hironobu

en Sasano, Hironobu
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Ishii, Naoto

× Ishii, Naoto

en Ishii, Naoto
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Tominaga, Teiji

× Tominaga, Teiji

en Tominaga, Teiji
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アクセス権
アクセス権 open access
アクセス権URI http://purl.org/coar/access_right/c_abf2
権利情報
言語 en
権利情報 Creative Commons Attribution 4.0
権利情報
言語 en
権利情報Resource https://creativecommons.org/licenses/by/4.0/
権利情報 https://creativecommons.org/licenses/by/4.0/
主題
言語 en
主題Scheme Other
主題 Glioblastoma
主題
言語 en
主題Scheme Other
主題 OX40
主題
言語 en
主題Scheme Other
主題 OX40 ligand
主題
言語 en
主題Scheme Other
主題 Immunotherapy
主題
言語 en
主題Scheme Other
主題 Hypoxia
主題
言語 en
主題Scheme Other
主題 Regulatory T cell
内容記述
内容記述タイプ Other
内容記述 Background: Glioblastoma is the most malignant human brain tumor and has a dismal prognosis; however, some patients show long-term survival. The interaction between the costimulatory molecule OX40 and its ligand OX40L generates key signals for T-cell activation. The augmentation of this interaction enhances antitumor immunity. In this present study, we explored whether OX40 signaling is responsible for antitumor adaptive immunity against glioblastoma and also established therapeutic antiglioma vaccination therapy. Methods: Tumor specimens were obtained from patients with primary glioblastoma (n = 110) and grade III glioma (n = 34). Quantitative polymerase chain reaction (PCR), flow cytometry, and immunohistochemistry were used to analyze OX40L expression in human glioblastoma specimens. Functional consequences of OX40 signaling were studied using glioblastoma cell lines, mouse models of glioma, and T cells isolated from human subjects and mice. Cytokine production assay with mouse regulatory T cells was conducted under hypoxic conditions (1.5% O_2). Results: OX40L mRNA was expressed in glioblastoma specimens and higher levels were associated with prolonged progression-free survival of patients with glioblastoma, who had undergone gross total resection. In this regard, OX40L protein was expressed in A172 human glioblastoma cells and its expression was induced under hypoxia, which mimics the microenvironment of glioblastoma. Notably, human CD4 T cells were activated when cocultured in anti-CD3-coated plates with A172 cells expressing OX40L, as judged by the increased production of interferon-γ. To confirm the survival advantage of OX40L expression, we then used mouse glioma models. Mice bearing glioma cells forced to express OX40L did not die during the observed period after intracranial transplantation, whereas all mice bearing glioma cells lacking OX40L died. Such a survival benefit of OX40L was not detected in nude mice with an impaired immune system. Moreover, compared with systemic intraperitoneal injection, the subcutaneous injection of the OX40 agonist antibody together with glioma cell lysates elicited stronger antitumor immunity and prolonged the survival of mice bearing glioma or glioma-initiating cell-like cells. Finally, OX40 triggering activated regulatory T cells cultured under hypoxia led to the induction of the immunosuppressive cytokine IL10. Conclusion: Glioblastoma directs immunostimulation or immunosuppression through OX40 signaling, depending on its microenvironment.
内容記述
内容記述タイプ Other
内容記述 論文
出版者
出版者 BioMed Central
言語 en
言語
言語 eng
資源タイプ
資源タイプ識別子 http://purl.org/coar/resource_type/c_6501
資源タイプ journal article
出版タイプ
出版タイプ VoR
出版タイプResource http://purl.org/coar/version/c_970fb48d4fbd8a85
識別子
識別子 http://hdl.handle.net/20.500.12000/45952
識別子タイプ HDL
関連情報
識別子タイプ DOI
関連識別子 https://doi.org/10.1186/s12943-015-0307-3
関連情報
識別子タイプ DOI
関連識別子 https://doi.org/10.1186/s12943-015-0307-3
収録物識別子
収録物識別子タイプ ISSN
収録物識別子 1476-4598
収録物名
収録物名 Molecular Cancer
言語 en
書誌情報
巻 14, 発行日 2015-02-15
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