Induction of Specific T Cell Tolerance by Fas Ligand- Expressing Antigen-Presenting Cells

Author:

Zhang Huang-ge1,Su Xiao1,Liu Di1,Liu Weimin1,Yang Pingar1,Wang Zheng1,Edwards Carl K.2,Bluethmann Horst3,Mountz John D.4,Zhou Tong1

Affiliation:

1. *Division of Clinical Immunology and Rheumatology, University of Alabama, Birmingham, AL 35294;

2. †Amgen, Inc., Boulder, CO 80301;

3. ‡F. Hoffmann-La Roche, Ltd., Basel, Switzerland; and

4. §Birmingham Veterans Administration Medical Center, Birmingham, AL 35233

Abstract

AbstractAutocrine interaction of Fas and Fas ligand leads to apoptosis of activated T cells, a process that is critical for the maintenance of peripheral T cell tolerance. Paracrine interactions of Fas ligand with T cells also may play an important role in the maintenance of tolerance, as Fas ligand can create immune-privileged sites and prevent graft rejection by inducing apoptosis in T cells. We surmised that APCs that express Fas ligand might directly induce apoptosis of T cells during presentation of Ag to the T cells, thus inducing Ag-specific, systemic T cell tolerance. Here, we show that profound, specific T cell unresponsiveness to alloantigen was induced by treatment of H-2k mice with H-2b APCs that expressed Fas ligand and that profound T cell unresponsiveness specific for the H-Y Ag was induced by treatment of H-2Db/H-Y TCR transgenic female mice with H-2Db/H-Y APCs that expressed Fas ligand. The induction of this systemic T cell tolerance required the expression of Fas ligand on the APCs as well as the expression of Fas on the T cells. The tolerance was restricted to the Ag presented by the APCs. The rapid and profound clonal deletion of the Ag-specific, peripheral T cells mediated by the Fas ligand-expressing APCs contributed to the induction of tolerance. These findings demonstrate that Ag-specific T cell tolerance can be induced by APCs that express Fas ligand and suggest a novel function for APCs in the induction of T cell apoptosis. Furthermore, they indicate a novel immunointervention strategy for treatment of graft rejection and autoantigen-specific autoimmune diseases.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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