Immunologic Self-Tolerance Maintained by Cd25+Cd4+Regulatory T Cells Constitutively Expressing Cytotoxic T Lymphocyte–Associated Antigen 4

T Takahashi, T Tagami, S Yamazaki, T Uede… - The Journal of …, 2000 - rupress.org
T Takahashi, T Tagami, S Yamazaki, T Uede, J Shimizu, N Sakaguchi, TW Mak…
The Journal of experimental medicine, 2000rupress.org
This report shows that cytotoxic T lymphocyte–associated antigen 4 (CTLA-4) plays a key
role in T cell–mediated dominant immunologic self-tolerance. In vivo blockade of CTLA-4 for
a limited period in normal mice leads to spontaneous development of chronic organ-specific
autoimmune diseases, which are immunopathologically similar to human counterparts. In
normal naive mice, CTLA-4 is constitutively expressed on CD25+ CD4+ T cells, which
constitute 5–10% of peripheral CD4+ T cells. When the CD25+ CD4+ T cells are stimulated …
This report shows that cytotoxic T lymphocyte–associated antigen 4 (CTLA-4) plays a key role in T cell–mediated dominant immunologic self-tolerance. In vivo blockade of CTLA-4 for a limited period in normal mice leads to spontaneous development of chronic organ-specific autoimmune diseases, which are immunopathologically similar to human counterparts. In normal naive mice, CTLA-4 is constitutively expressed on CD25+CD4+ T cells, which constitute 5–10% of peripheral CD4+ T cells. When the CD25+CD4+ T cells are stimulated via the T cell receptor in vitro, they potently suppress antigen-specific and polyclonal activation and proliferation of other T cells, including CTLA-4–deficient T cells, and blockade of CTLA-4 abrogates the suppression. CD28-deficient CD25+CD4+ T cells can also suppress normal T cells, indicating that CD28 is dispensable for activation of the regulatory T cells. Thus, the CD25+CD4+ regulatory T cell population engaged in dominant self-tolerance may require CTLA-4 but not CD28 as a costimulatory molecule for its functional activation. Furthermore, interference with this role of CTLA-4 suffices to elicit autoimmune disease in otherwise normal animals, presumably through affecting CD25+CD4+ T cell–mediated control of self-reactive T cells. This unique function of CTLA-4 could be exploited to potentiate T cell–mediated immunoregulation, and thereby to induce immunologic tolerance or to control autoimmunity.
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