Signaling Modulates Cytolytic T Lymphocyte Effector Functions

Cytolytic T cells use two mechanisms to kill virally infected cells, tumor cells, or other potentially autoreactive T cells in short-term in vitro assays. The perforin/granule exocytosis mechanism uses preformed cytolytic granules that are delivered to the target cell to induce apoptosis and eventual lysis. FasL/Fas (CD95 ligand/CD95)–mediated cytolysis requires de novo protein synthesis of FasL by the CTL and the presence of the death receptor Fas on the target cell to induce apoptosis. Using a CD8 1 CTL clone that kills via both the perforin/granule exocytosis and FasL/Fas mechanisms, and a clone that kills via the FasL/Fas mechanism only, we have examined the requirement of intraand extracellular Ca 2 1 in TCR-triggered cytolytic effector function. These two clones, a panel of Ca 2 1 antagonists, and agonists were used to determine that a large biphasic increase in intracellular calcium concentration, characterized by release of Ca 2 1 from intracellular stores followed by a sustained influx of extracellular Ca 2 1 , is required for perforin/granule exocytosis. Only the sustained influx of extracellular Ca 2 1 is required for FasL induction and killing. Thapsigargin, at low concentrations, induces this small but sustained increase in [Ca 2 1 ] i and selectively induces FasL/Fas-mediated cytolysis but not granule exocytosis. These results further define the role of Ca 2 1 in perforin and FasL/Fas killing and demonstrate that differential Ca 2 1 signaling can modulate T cell effector functions.