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The Journal of Immunology, 1999, 162: 6401-6409.
Copyright © 1999 by The American Association of Immunologists

Induction of T Cell Anergy by Low Numbers of Agonist Ligands1

Laura C. Korb, Saied Mirshahidi, Kasra Ramyar, Amir A. Sadighi Akha and Scheherazade Sadegh-Nasseri2

Department of Pathology and Graduate Program in Immunology, School of Medicine/Johns Hopkins University, Baltimore, MD 21205

Engagement of TCR by its ligand, the MHC/peptide complex, causes T cell activation. T cells respond positively to stimulation with agonists, and are inhibited by antagonist MHC/peptide ligands. Failure to induce proper conformational changes in the TCR or fast TCR/MHC dissociation are the leading models proposed to explain anergy induction by antagonist ligands. In this study, we demonstrate that presentation of between 1 and 10 complexes of agonist/MHC II by unfixed APC induces T cell anergy that persists up to 7 days and has characteristics similar to anergy induced by antagonist ligand or TCR occupancy without costimulation. Furthermore, anergy-inducing doses of hemagglutinin 306–318 peptide led to the engagement of less than 1000 TCR/CD3 complexes. Thus, engagement of a subthreshold number of TCR by either a low density of agonist/MHC or a 2–3 orders of magnitude higher density of antagonist/MHC causes anergy. Moreover, we show that anergy induced by low agonist concentrations is inhibited in the presence of IL-2 or cyclosporin A, suggesting involvement of the calcineurin signaling pathway.




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