Projects per year
Personal profile
Campus career
展開ゲノム薬学系 教授 2017/10/01-2019/09/30
薬学・和漢系 教授 2019/10/01-
薬学科 教授 2019/10/01-
薬学部薬学科 基幹教員
学部運営への参画状況・・・有-教授会他
担当授業科目に係る状況・・・主要授業科目担当
Research interests
Novel immune regulatory mechanisms of cytokines that are controlled by TRAF and TNF family molecules
The mammalian tumor necrosis factor receptor (TNFR)-associated factor (TRAF) is composed of seven family molecules numbered sequentially from TRAF1 to TRAF7. TRAF family molecules control the signaling activity of receptors for tumor necrosis factor-α (TNF-α), a representative pro-inflammatory cytokine, and related TNF family cytokines. Moreover, recent studies have demonstrated that TRAFs associate with immune receptors other than TNFRs and exhibit immune regulatory activities toward these unconventional receptors. However, the molecular mechanisms by which TRAFs regulate these receptors remain obscure.
TRAF5 was discovered as a signaling adaptor of several TNFR family molecules. CD4+ helper T cells help B cells to produce antibodies and play important roles in adaptive immunity. We have identified a novel attribute of TRAF5 in the receptor for interleukin-6 (IL-6), another pro-inflammatory cytokine critically involving CD4+ T cells. Furthermore, TRAF5 displays a regulatory role in Toll-like receptor signaling. We aim to understand novel and uncharacterized cellular functions of TRAF5 in the context of inflammation and immune-mediated diseases.
Collectively, we aim to uncover uncharacterized immune regulatory mechanisms of cytokines to develop novel therapeutic strategies for immune-mediated diseases.
Expertise related to UN Sustainable Development Goals
In 2015, UN member states agreed to 17 global Sustainable Development Goals (SDGs) to end poverty, protect the planet and ensure prosperity for all. This person’s work contributes towards the following SDG(s):
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Collaborations and top research areas from the last five years
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OX40アゴニストの創製から T 細胞免疫療法への展開
So, T. (Principal Investigator)
Japan Society for the Promotion of Science
2025/04/01 → 2028/03/31
Project: Research Project
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Development of a method for activation of costimulatory immune receptors by using their corresponding multimerized ligands
So, T. (Principal Investigator) & 石井直人 (Co-Investigator(Kenkyū-buntansha))
Japan Society for the Promotion of Science
2023/06/30 → 2025/03/31
Project: Research Project
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副腎白質ジストロフィーはコレステロール代謝障害による免疫応答の破綻が原因か?
Morita, M. (Principal Investigator) & So, T. (Co-Investigator(Kenkyū-buntansha))
Japan Society for the Promotion of Science
2022/04/01 → 2025/03/31
Project: Research Project
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Characterization of multifunctional roles of TRAF5 in pro-inflammatory cytokine receptor signaling
So, T. (PI)
2018/04/01 → 2021/03/31
Project: Research
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Regulation of inflammatory cytokine signaling by TRAF5
So, T. (PI)
2015/04/01 → 2018/03/31
Project: Research
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ABCD1欠損ヒトアストロサイトーマU87細胞株のNLRP3インフラマソーム活性化機構の解析.
守田 雅志, 松沢 紗良, 國石 (彦坂) 茉里 & 宗 孝紀., 2024.Research output: Contribution to conference › Presentation
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Basic characterization of TNF ligand-based agonists targeting OX40, 4-1BB, CD27, and GITR expressed by T cells.
So, T., Nagai, H., Azuma, M., Sato, A., Suzuki, A., Ito, A., Morita, M., Hikosaka-Kuniishi, M. & Ishii., N., 2024.Research output: Contribution to conference › Presentation
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B細胞におけるTRAF5の高発現はTLRシグナルを介した IgM 抗体産生能の抑制に重要か?
東充輝, 斉藤弘晃, 若泉知美, 岩谷航洋, 小澤勇介, 守田雅志, 國石(彦坂)茉里 & 宗孝紀., 2024.Research output: Contribution to conference › Presentation
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Functional characterization of antibody fusion-single-chain TNF proteins that agonize costimulatory TNFR expressed by T cells.
Nagai, H., Azuma, M., Sato, A., Ogawara, S., Tsutsui, Y., Suzuki, A., Matsuyama, S., Wakaizumi, T., Morita, M., Hikosaka-Kuniishi, M., Ishii, N. & So., T., 2024.Research output: Contribution to conference › Presentation
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Generation and characterization of OX40-ligand fusion protein that agonizes OX40 on T-Lymphocytes
Sato, A., Nagai, H., Suzuki, A., Ito, A., Matsuyama, S., Shibui, N., Morita, M., Hikosaka-Kuniishi, M., Ishii, N. & So, T., 2024, In: Frontiers in Immunology. 15, 1473815.Research output: Contribution to journal › Article › peer-review
Open Access
Activities
- 15 Oral presentation
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TRAF5 による CD4+ T 細胞の IL-27 受容体シグナル調節機構.
So, T. (Speaker)
2021/03/26 → 2021/03/29Activity: Talk or presentation › Oral presentation
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TNFR-associated factor (TRAF) 5 expressed by intestinal epithelial cells promotes NF-kB-mediated inflammation via controlling TRAF2 stability in dextran sulfate sodium-induced colitis.
So, T. (Speaker)
2019/12/11 → 2019/12/13Activity: Talk or presentation › Oral presentation
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IQGAP1 regulates ILC2 apoptosis in the lung.
So, T. (Speaker)
2019/12/11 → 2019/12/13Activity: Talk or presentation › Oral presentation
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TNF receptor-associated factor 5 inhibits IL-27 receptor signaling in CD4+ T-lymphocytes.
So, T. (Speaker)
2019/12/11 → 2019/12/13Activity: Talk or presentation › Oral presentation
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Understanding the role of TRAF family proteins in gp130 signaling.
So, T. (Speaker)
2019/12/11 → 2019/12/13Activity: Talk or presentation › Oral presentation
Courses
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先端生命薬学
Tabuchi, A., Hirose, Y., Morita, M., Kuniishi, M., Tanaka, A., So, T., Ihara, D., Yokoyama, S. & Sakurai, H. 2024/10/01 → 2025/03/31
Course
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