Peripheral clonal deletion of superantigen‐reactive T cells is enhanced by cortisone

Abstract

The Tcell receptor (TcR) V_β‐specific expansion, deletion and induction of nonresponsiveness among murine T cells responding to superantigens in the periphery has been well characterized. Here we demonstrate that clonal deletion of staphylococcal enterotoxin (SE) B‐reactive V_β 8.2⁺ cells can be significantly increased when mice are injected with hydrocortisone (HC) following superantigen stimulation in vivo. The induced sensitivity to HC persists for at least 30 days after SEB injection, making it unlikely that proliferating cells were uniquely responsible for the enhanced deletion. Superantigen‐induced HC sensitivity was a general phenomenon and could also be observed among V_β 11⁺ cells after the injection of SEA. Experiments conducted on thymectomized mice indicated that HC‐sensitive, SEB‐responsive cells could not be accounted for by rapidly produced, immature lymphocytes recently exported from the thymus. Further, V_β 8.1⁺ peripheral lymphocytes from TcR transgenic mice expressing the Mls‐1^a superantigen were sensitive to HC. These results imply that the majority of cells remaining after superantigen‐induced clonal expansion and deletion in vivo have indeed reacted with the superantigen. Implications for differential superantigen recognition by Tcells expressing the same TcR V_β domain, perhaps due to a significant V_α contribution to the interaction in vivo, are discussed.