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Altered thymic T-cell selection due to a mutation of the ZAP-70 gene causes autoimmune arthritis in mice

Author

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  • Noriko Sakaguchi

    (Kyoto University
    RIKEN Research Center for Allergy and Immunology)

  • Takeshi Takahashi

    (Kyoto University)

  • Hiroshi Hata

    (Kyoto University)

  • Takashi Nomura

    (Kyoto University)

  • Tomoyuki Tagami

    (Kyoto University)

  • Sayuri Yamazaki

    (Kyoto University)

  • Toshiko Sakihama

    (Kyoto University)

  • Takaji Matsutani

    (Shionogi Institute for Medical Science)

  • Izumi Negishi

    (Gunma University Hospital)

  • Syuichi Nakatsuru

    (Kyoto University)

  • Shimon Sakaguchi

    (Kyoto University
    RIKEN Research Center for Allergy and Immunology)

Abstract

Rheumatoid arthritis (RA), which afflicts about 1% of the world population, is a chronic systemic inflammatory disease of unknown aetiology that primarily affects the synovial membranes of multiple joints1,2,3. Although CD4+ T cells seem to be the prime mediators of RA, it remains unclear how arthritogenic CD4+ T cells are generated and activated1,2,3. Given that highly self-reactive T-cell clones are deleted during normal T-cell development in the thymus, abnormality in T-cell selection has been suspected as one cause of autoimmune disease4,5. Here we show that a spontaneous point mutation of the gene encoding an SH2 domain of ZAP-70, a key signal transduction molecule in T cells6, causes chronic autoimmune arthritis in mice that resembles human RA in many aspects. Altered signal transduction from T-cell antigen receptor through the aberrant ZAP-70 changes the thresholds of T cells to thymic selection, leading to the positive selection of otherwise negatively selected autoimmune T cells. Thymic production of arthritogenic T cells due to a genetically determined selection shift of the T-cell repertoire towards high self-reactivity might also be crucial to the development of disease in a subset of patients with RA.

Suggested Citation

  • Noriko Sakaguchi & Takeshi Takahashi & Hiroshi Hata & Takashi Nomura & Tomoyuki Tagami & Sayuri Yamazaki & Toshiko Sakihama & Takaji Matsutani & Izumi Negishi & Syuichi Nakatsuru & Shimon Sakaguchi, 2003. "Altered thymic T-cell selection due to a mutation of the ZAP-70 gene causes autoimmune arthritis in mice," Nature, Nature, vol. 426(6965), pages 454-460, November.
    • Handle: RePEc:nat:nature:v:426:y:2003:i:6965:d:10.1038_nature02119
    DOI: 10.1038/nature02119
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    Cited by:

    1. Hirofumi Nakaoka & Tailin Cui & Atsushi Tajima & Akira Oka & Shigeki Mitsunaga & Koichi Kashiwase & Yasuhiko Homma & Shinji Sato & Yasuo Suzuki & Hidetoshi Inoko & Ituro Inoue, 2011. "A Systems Genetics Approach Provides a Bridge from Discovered Genetic Variants to Biological Pathways in Rheumatoid Arthritis," PLOS ONE, Public Library of Science, vol. 6(9), pages 1-16, September.
    2. Christopher Szeto & Pirooz Zareie & Rushika C. Wirasinha & Justin B. Zhang & Andrea T. Nguyen & Alan Riboldi-Tunnicliffe & Nicole L. Gruta & Stephanie Gras & Stephen R. Daley, 2022. "Covalent TCR-peptide-MHC interactions induce T cell activation and redirect T cell fate in the thymus," Nature Communications, Nature, vol. 13(1), pages 1-12, December.

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