TRIM28 prevents autoinflammatory T cell development in vivo

Shunsuke Chikuma; Naomasa Suita; Il Mi Okazaki; Shiro Shibayama; Tasuku Honjo

doi:10.1038/ni.2293

TRIM28 prevents autoinflammatory T cell development in vivo

Shunsuke Chikuma, Naomasa Suita, Il Mi Okazaki, Shiro Shibayama, Tasuku Honjo

研究成果: Article › 査読

82 被引用数 (Scopus)

抄録

TRIM28 is a component of heterochromatin complexes whose function in the immune system is unknown. By studying mice with conditional T cell-specific deletion of TRIM28 (CKO mice), we found that TRIM28 was phosphorylated after stimulation via the T cell antigen receptor (TCR) and was involved in the global regulation of CD4⁺ T cells. The CKO mice had a spontaneous autoimmune phenotype that was due in part to early lymphopenia associated with a defect in the production of interleukin 2 (IL-2) as well as incomplete cell-cycle progression of their T cells. In addition, CKO T cells showed derepression of the cytokine TGF-β3, which resulted in an altered cytokine balance; this caused the accumulation of autoreactive cells of the T _H17 subset of helper T cells and of Foxp3⁺ T cells. Notably, CKO Foxp3⁺ T cells were unable to prevent the autoimmune phenotype in vivo. Our results show critical roles for TRIM28 in both T cell activation and T cell tolerance.

本文言語	English
ページ（範囲）	596-603
ページ数	8
ジャーナル	Nature Immunology
巻	13
号	6
DOI	https://doi.org/10.1038/ni.2293
出版ステータス	Published - 2012 6月
外部発表	はい

ASJC Scopus subject areas

免疫アレルギー学
免疫学

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10.1038/ni.2293

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title = "TRIM28 prevents autoinflammatory T cell development in vivo",

abstract = "TRIM28 is a component of heterochromatin complexes whose function in the immune system is unknown. By studying mice with conditional T cell-specific deletion of TRIM28 (CKO mice), we found that TRIM28 was phosphorylated after stimulation via the T cell antigen receptor (TCR) and was involved in the global regulation of CD4+ T cells. The CKO mice had a spontaneous autoimmune phenotype that was due in part to early lymphopenia associated with a defect in the production of interleukin 2 (IL-2) as well as incomplete cell-cycle progression of their T cells. In addition, CKO T cells showed derepression of the cytokine TGF-β3, which resulted in an altered cytokine balance; this caused the accumulation of autoreactive cells of the T H17 subset of helper T cells and of Foxp3+ T cells. Notably, CKO Foxp3+ T cells were unable to prevent the autoimmune phenotype in vivo. Our results show critical roles for TRIM28 in both T cell activation and T cell tolerance.",

author = "Shunsuke Chikuma and Naomasa Suita and Okazaki, {Il Mi} and Shiro Shibayama and Tasuku Honjo",

note = "Funding Information: We thank X. Zhou, A. Shimizu, S. Bailey-Bucktrout, K. Ikuta, T. Eagar, K. Ogasawara and M. Aida for discussions; K. Yurimoto for assistance in mouse genotyping; P. Chambon and R. Losson (Institut de G{\'e}n{\'e}tique et de Biologie Mol{\'e}culaire et Cellulaire, France) for mice with loxP-flanked Trim28 alleles; J. Takeda (Osaka University) for mice with Cre expression driven by the Lck promoter; J. Bluestone (University of California-San Francisco) for Foxp3-GFP-Cre–transgenic mice; S. Nagata (Kyoto University) for CD45.1+ mice; K. Kabashima (Kyoto University) for Rag2−/− mice; and J. Bluestone and N. Minato for critical reading of the manuscript. Supported by the Ministry of Education, Culture, Sports, Science and Technology of Japan (KAKENHI Grant-in-Aid for Scientific Research Young Scientist (B) 21790465 and 23790534 to S.C.) and the Program for the Promotion of Fundamental Studies in Health Sciences of the National Institute of Biomedical Innovation (T.H.).",

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AU - Suita, Naomasa

AU - Okazaki, Il Mi

AU - Shibayama, Shiro

AU - Honjo, Tasuku

N1 - Funding Information: We thank X. Zhou, A. Shimizu, S. Bailey-Bucktrout, K. Ikuta, T. Eagar, K. Ogasawara and M. Aida for discussions; K. Yurimoto for assistance in mouse genotyping; P. Chambon and R. Losson (Institut de Génétique et de Biologie Moléculaire et Cellulaire, France) for mice with loxP-flanked Trim28 alleles; J. Takeda (Osaka University) for mice with Cre expression driven by the Lck promoter; J. Bluestone (University of California-San Francisco) for Foxp3-GFP-Cre–transgenic mice; S. Nagata (Kyoto University) for CD45.1+ mice; K. Kabashima (Kyoto University) for Rag2−/− mice; and J. Bluestone and N. Minato for critical reading of the manuscript. Supported by the Ministry of Education, Culture, Sports, Science and Technology of Japan (KAKENHI Grant-in-Aid for Scientific Research Young Scientist (B) 21790465 and 23790534 to S.C.) and the Program for the Promotion of Fundamental Studies in Health Sciences of the National Institute of Biomedical Innovation (T.H.).

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N2 - TRIM28 is a component of heterochromatin complexes whose function in the immune system is unknown. By studying mice with conditional T cell-specific deletion of TRIM28 (CKO mice), we found that TRIM28 was phosphorylated after stimulation via the T cell antigen receptor (TCR) and was involved in the global regulation of CD4+ T cells. The CKO mice had a spontaneous autoimmune phenotype that was due in part to early lymphopenia associated with a defect in the production of interleukin 2 (IL-2) as well as incomplete cell-cycle progression of their T cells. In addition, CKO T cells showed derepression of the cytokine TGF-β3, which resulted in an altered cytokine balance; this caused the accumulation of autoreactive cells of the T H17 subset of helper T cells and of Foxp3+ T cells. Notably, CKO Foxp3+ T cells were unable to prevent the autoimmune phenotype in vivo. Our results show critical roles for TRIM28 in both T cell activation and T cell tolerance.

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TRIM28 prevents autoinflammatory T cell development in vivo

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