Abstract
Renal and cardiac recipients undergoing aggressive immunosuppressive therapy with cyclosporin A have been reported to have unusually high incidences of Epstein–Barr virus (EBV) genome–positive lymphomas. T cells have been shown to be of critical importance in controlling the lymphoproliferative potential of the EB virus.
EBV–specific T cell clones were generated
In this study, we show that cyclosporin A does not interfere with antigen recognition, since the T cell cytotoxic potential is unchanged. However, cyclosporin A induces a dose–dependent reduction in membrane IL-2 receptor expression which consequently limits the proliferation of the antigen-activated cell. This may translate
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