Delayed Lymphoid Repopulation with Defects in IL-4–Driven Responses Produced by Inactivation of NF-ATc

The NF-AT family of transcription factors activates early immune response genes such as cytokines. In the adult, NF-ATc is expressed exclusively in the lymphoid system and is induced upon lymphocyte activation. NF-ATc null mutant mice die in utero of cardiac failure, precluding analysis of the role...

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Veröffentlicht in:Immunity (Cambridge, Mass.) Mass.), 1998, Vol.8 (1), p.125-134
Hauptverfasser: Ranger, Ann M, Hodge, Martin R, Gravallese, Ellen M, Oukka, Mohammed, Davidson, Laurie, Alt, Frederick W, de la Brousse, Fabienne C, Hoey, Timothy, Grusby, Michael, Glimcher, Laurie H
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Sprache:eng
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Zusammenfassung:The NF-AT family of transcription factors activates early immune response genes such as cytokines. In the adult, NF-ATc is expressed exclusively in the lymphoid system and is induced upon lymphocyte activation. NF-ATc null mutant mice die in utero of cardiac failure, precluding analysis of the role of NF-ATc in lymphocyte activation. By using RAG-2–deficient blastocyst complementation, we now demonstrate that young, highly chimeric mice lacking NF-ATc have impaired repopulation of both thymus and peripheral lymphoid organs. Furthermore, NF-ATc deficiency impaired T lymphocyte activation and secretion of IL-4. B lymphocytes displayed reduced proliferation and a selective loss of IL-4–driven immunoglobulin isotypes both in vivo and in vitro. Our data demonstrate that NF-ATc is essential for the optimal generation and function of mature T and B lineage cells, with an especially profound effect on IL-4–driven responses.
ISSN:1074-7613
1097-4180
DOI:10.1016/S1074-7613(00)80465-3