TOLERANCE OF T-CELL RECEPTOR GAMMA-DELTA-CELLS IN THE INTESTINE

The present study examined the mechanism(s) of tolerance induction for intestinal intraepithelial lymphocytes (iIELs) using an alloantigen ( Ag)-specific gamma/delta T cell receptor (TCR gamma/delta) transgenic (Tg) model. In Tg Ag-bearing H-2b/d mice (Tg(b/d)), Tg iIELs were Thy- 1-, CD44+, CD45R (B220)+, and CD5+, whereas in syngeneic Tg(d/d) mice, iIELs were Thy-1+, CD44-, and CD45R- with a subset of CD5+ cells. Pre viously, we had shown that tolerance for Tg(b/d) iIELs involved functi onal anergy and deletion (Barrett, T A., M. L. Delvy, D. M. Kennedy, L . Lefrancois, L. A. Matis, A. L. Dent, S. M. Hedrick, and J. A. Bluest one. 1992. J. Exp. Med. 175:65). In this study we demonstrate that Tg( b/d) iIELs expressing dull levels of Thy-1 proliferated in the presenc e of exogenous rIL-2. A direct precursor-product relationship between the Thy-1+-responsive iIELs and the tolerant Thy-1dul/- iIELs was demo nstrated by adoptive transfer into severe combined immunodeficient (SC ID) mice. Tg Thy-1+ iIELs reconstituting Ag+ but not Ag- SCID mice dow nregulated Thy-1 after Ag exposure in vivo. Analysis of bone marrow (B M) chimeras demonstrated the persistence of Tg IELs in all Ag+ chimera s although a modest degree of clonal deletion was apparent. The greate st percentage of Tg IELs were detected when Ag was restricted to radio resistant cells (e.g., epithelial cells) compared with BM-derived anti gen-presenting cells (APC). This was especially apparent in thymectomi zed chimeric mice. Consistent with the notion that Ag-bearing epitheli al cells may be poor APC, isolated intestinal epithelial cells from Ag -bearing mice failed to stimulate Tg iIELs compared with splenic APC. These studies suggest that the major population of TCR gamma/delta iIE Ls were probably extrathymically derived and encountered self-Ag on in testinal epithelial cells. The induction of tolerance likely involved an activation event resulting in downregulation of Thy-1. These mechan isms of tolerance for TCR gamma/delta iIELs led to the persistence of a reservoir of self-reactive T cells with the potential for mediating autoimmune disease.