The Curcumin Analog GO-Y030 Controls the Generation and Stability of Regulatory T Cells

Takashi MaruYama; Shuhei Kobayashi; Hiroko Nakatsukasa; Yuki Moritoki; Daiki Taguchi; Yoichi Sunagawa; Tatsuya Morimoto; Atsuko Asao; Wenwen Jin; Yuji Owada; Naoto Ishii; Yoshiharu Iwabuchi; Akihiko Yoshimura; Wan Jun Chen; Hiroyuki Shibata

doi:10.3389/fimmu.2021.687669

The Curcumin Analog GO-Y030 Controls the Generation and Stability of Regulatory T Cells

Takashi MaruYama, Shuhei Kobayashi, Hiroko Nakatsukasa, Yuki Moritoki, Daiki Taguchi, Yoichi Sunagawa, Tatsuya Morimoto, Atsuko Asao, Wenwen Jin, Yuji Owada, Naoto Ishii, Yoshiharu Iwabuchi, Akihiko Yoshimura, Wan Jun Chen, Hiroyuki Shibata

微生物学・免疫学

研究成果: Article › 査読

13 被引用数 (Scopus)

抄録

Regulatory T cells (Tregs) play a crucial role in preventing antitumor immune responses in cancer tissues. Cancer tissues produce large amounts of transforming growth factor beta (TGF-β), which promotes the generation of Foxp3⁺ Tregs from naïve CD4⁺ T cells in the local tumor microenvironment. TGF-β activates nuclear factor kappa B (NF-κB)/p300 and SMAD signaling, which increases the number of acetylated histones at the Foxp3 locus and induces Foxp3 gene expression. TGF-β also helps stabilize Foxp3 expression. The curcumin analog and antitumor agent, GO-Y030, prevented the TGF-β-induced generation of Tregs by preventing p300 from accelerating NF-κB-induced Foxp3 expression. Moreover, the addition of GO-Y030 resulted in a significant reduction in the number of acetylated histones at the Foxp3 promoter and at the conserved noncoding sequence 1 regions that are generated in response to TGF-β. In vivo tumor models demonstrated that GO-Y030-treatment prevented tumor growth and reduced the Foxp3⁺ Tregs population in tumor-infiltrating lymphocytes. Therefore, GO-Y030 exerts a potent anticancer effect by controlling Treg generation and stability.

本文言語	English
論文番号	687669
ジャーナル	Frontiers in Immunology
巻	12
DOI	https://doi.org/10.3389/fimmu.2021.687669
出版ステータス	Published - 2021 6月 23

ASJC Scopus subject areas

免疫アレルギー学
免疫学

UN SDG

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MaruYama, T., Kobayashi, S., Nakatsukasa, H., Moritoki, Y., Taguchi, D., Sunagawa, Y., Morimoto, T., Asao, A., Jin, W., Owada, Y., Ishii, N., Iwabuchi, Y., Yoshimura, A., Chen, W. J., & Shibata, H. (2021). The Curcumin Analog GO-Y030 Controls the Generation and Stability of Regulatory T Cells. Frontiers in Immunology, 12, Article 687669. https://doi.org/10.3389/fimmu.2021.687669

@article{acfab0b02aa44d5089ba774415d365e8,

title = "The Curcumin Analog GO-Y030 Controls the Generation and Stability of Regulatory T Cells",

abstract = "Regulatory T cells (Tregs) play a crucial role in preventing antitumor immune responses in cancer tissues. Cancer tissues produce large amounts of transforming growth factor beta (TGF-β), which promotes the generation of Foxp3+ Tregs from na{\"i}ve CD4+ T cells in the local tumor microenvironment. TGF-β activates nuclear factor kappa B (NF-κB)/p300 and SMAD signaling, which increases the number of acetylated histones at the Foxp3 locus and induces Foxp3 gene expression. TGF-β also helps stabilize Foxp3 expression. The curcumin analog and antitumor agent, GO-Y030, prevented the TGF-β-induced generation of Tregs by preventing p300 from accelerating NF-κB-induced Foxp3 expression. Moreover, the addition of GO-Y030 resulted in a significant reduction in the number of acetylated histones at the Foxp3 promoter and at the conserved noncoding sequence 1 regions that are generated in response to TGF-β. In vivo tumor models demonstrated that GO-Y030-treatment prevented tumor growth and reduced the Foxp3+ Tregs population in tumor-infiltrating lymphocytes. Therefore, GO-Y030 exerts a potent anticancer effect by controlling Treg generation and stability.",

keywords = "Foxp3, GO-Y030, TGF-beta 1, gene regulating, regulatory T cell",

author = "Takashi MaruYama and Shuhei Kobayashi and Hiroko Nakatsukasa and Yuki Moritoki and Daiki Taguchi and Yoichi Sunagawa and Tatsuya Morimoto and Atsuko Asao and Wenwen Jin and Yuji Owada and Naoto Ishii and Yoshiharu Iwabuchi and Akihiko Yoshimura and Chen, {Wan Jun} and Hiroyuki Shibata",

note = "Funding Information: This research was supported in part by the Fund for the Promotion of Joint International Research [Fostering Joint International Research (B)] (18KK0257) to TMa, the Intramural Research Program of NIDCR to WC, and a Grant-in-Aid for Scientific Research (C) (20K11643) to HS. Funding Information: We are grateful to Dr. Muta Tatsushi (63) for providing critical reagents for this study. This research was supported (in part) by the NIDCR (Technical research center). The authors would like to thank the NIDCR animal facility staff very much for maintaining the mouse colony while the NIH was closed for COVID-19 (particularly from March/23/2020 to June/22/2020). Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2021 MaruYama, Kobayashi, Nakatsukasa, Moritoki, Taguchi, Sunagawa, Morimoto, Asao, Jin, Owada, Ishii, Iwabuchi, Yoshimura, Chen and Shibata.",

year = "2021",

month = jun,

day = "23",

doi = "10.3389/fimmu.2021.687669",

language = "English",

volume = "12",

journal = "Frontiers in Immunology",

issn = "1664-3224",

publisher = "Frontiers Media S. A.",

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T1 - The Curcumin Analog GO-Y030 Controls the Generation and Stability of Regulatory T Cells

AU - MaruYama, Takashi

AU - Kobayashi, Shuhei

AU - Nakatsukasa, Hiroko

AU - Moritoki, Yuki

AU - Taguchi, Daiki

AU - Sunagawa, Yoichi

AU - Morimoto, Tatsuya

AU - Asao, Atsuko

AU - Jin, Wenwen

AU - Owada, Yuji

AU - Ishii, Naoto

AU - Iwabuchi, Yoshiharu

AU - Yoshimura, Akihiko

AU - Chen, Wan Jun

AU - Shibata, Hiroyuki

N1 - Funding Information: This research was supported in part by the Fund for the Promotion of Joint International Research [Fostering Joint International Research (B)] (18KK0257) to TMa, the Intramural Research Program of NIDCR to WC, and a Grant-in-Aid for Scientific Research (C) (20K11643) to HS. Funding Information: We are grateful to Dr. Muta Tatsushi (63) for providing critical reagents for this study. This research was supported (in part) by the NIDCR (Technical research center). The authors would like to thank the NIDCR animal facility staff very much for maintaining the mouse colony while the NIH was closed for COVID-19 (particularly from March/23/2020 to June/22/2020). Publisher Copyright: © Copyright © 2021 MaruYama, Kobayashi, Nakatsukasa, Moritoki, Taguchi, Sunagawa, Morimoto, Asao, Jin, Owada, Ishii, Iwabuchi, Yoshimura, Chen and Shibata.

PY - 2021/6/23

Y1 - 2021/6/23

N2 - Regulatory T cells (Tregs) play a crucial role in preventing antitumor immune responses in cancer tissues. Cancer tissues produce large amounts of transforming growth factor beta (TGF-β), which promotes the generation of Foxp3+ Tregs from naïve CD4+ T cells in the local tumor microenvironment. TGF-β activates nuclear factor kappa B (NF-κB)/p300 and SMAD signaling, which increases the number of acetylated histones at the Foxp3 locus and induces Foxp3 gene expression. TGF-β also helps stabilize Foxp3 expression. The curcumin analog and antitumor agent, GO-Y030, prevented the TGF-β-induced generation of Tregs by preventing p300 from accelerating NF-κB-induced Foxp3 expression. Moreover, the addition of GO-Y030 resulted in a significant reduction in the number of acetylated histones at the Foxp3 promoter and at the conserved noncoding sequence 1 regions that are generated in response to TGF-β. In vivo tumor models demonstrated that GO-Y030-treatment prevented tumor growth and reduced the Foxp3+ Tregs population in tumor-infiltrating lymphocytes. Therefore, GO-Y030 exerts a potent anticancer effect by controlling Treg generation and stability.

AB - Regulatory T cells (Tregs) play a crucial role in preventing antitumor immune responses in cancer tissues. Cancer tissues produce large amounts of transforming growth factor beta (TGF-β), which promotes the generation of Foxp3+ Tregs from naïve CD4+ T cells in the local tumor microenvironment. TGF-β activates nuclear factor kappa B (NF-κB)/p300 and SMAD signaling, which increases the number of acetylated histones at the Foxp3 locus and induces Foxp3 gene expression. TGF-β also helps stabilize Foxp3 expression. The curcumin analog and antitumor agent, GO-Y030, prevented the TGF-β-induced generation of Tregs by preventing p300 from accelerating NF-κB-induced Foxp3 expression. Moreover, the addition of GO-Y030 resulted in a significant reduction in the number of acetylated histones at the Foxp3 promoter and at the conserved noncoding sequence 1 regions that are generated in response to TGF-β. In vivo tumor models demonstrated that GO-Y030-treatment prevented tumor growth and reduced the Foxp3+ Tregs population in tumor-infiltrating lymphocytes. Therefore, GO-Y030 exerts a potent anticancer effect by controlling Treg generation and stability.

KW - Foxp3

KW - GO-Y030

KW - TGF-beta 1

KW - gene regulating

KW - regulatory T cell

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The Curcumin Analog GO-Y030 Controls the Generation and Stability of Regulatory T Cells

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ASJC Scopus subject areas

UN SDG

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