Adenosine A2B receptor antagonist suppresses differentiation to regulatory T cells without suppressing activation of T cells |
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| Authors: | Hiroko Nakatsukasa Mitsutoshi Tsukimoto Hitoshi Harada Shuji Kojima |
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| Affiliation: | aDepartment of Radiation Biosciences, Faculty of Pharmaceutical Sciences, Tokyo University of Science, 2641 Yamazaki, Noda-shi, Chiba 278-8510, Japan;bFaculty of Pharmaceutical Sciences, Suzuka University of Medical Science, 3500-3 Minamitamagaki-cho, Suzuka-shi, Mie 513-8670, Japan |
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| Abstract: | Extracellular adenosine activates P1 receptors (A1, A2A, A2B, A3) on cellular membranes. Here, we investigated the involvement of P1 receptor-mediated signaling in differentiation to regulatory T cells (Treg). Treg were induced in vitro by incubating isolated CD4+CD62L+ naïve murine T cells under Treg-skewing conditions. Antagonists of A1 and A2B receptors suppressed the expression of Foxp3, a specific marker of Treg, and the production of IL-10, suggesting the involvement of A1 and A2B receptors in differentiation to Treg. We also investigated the effect of these antagonists on T cell activation, which is essential for differentiation to Treg, and found that A1 antagonist, but not A2B antagonist, suppressed T cell activation. We conclude that A1 and A2B receptors are both involved in differentiation to Treg, but through different mechanisms. Since A2B antagonist blocked differentiation to Treg without suppressing T cell activation, it is possible that blockade of A2B receptor would facilitate tumor immunity. |
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| Keywords: | Abbreviations: [Ca2+]i, cytosolic Ca2+ concentration Foxp3, Forkhead box P3 IL, interleukin mAb, monoclonal antibody TCR, T cell receptor TGF-β, transforming growth factor-β Treg, regulatory T cells |
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