LOW CONCENTRATIONS OF PROTEIN-KINASE C-ACTIVATING AGONISTS SUPPRESS CHOLECYSTOKININ-OPE-EVOKED CA2+ MOBILIZATION IN RAT PANCREATIC ACINI

The phenethyl ester analogues of cholecystokinin, OPE and JMV-180, are fully efficacious rat pancreatic secretagoguges which, unlike cholecy stokinin (CCK), do not elicit supramaximal inhibition of secretion, an d stimulate a sustained rise of cytosolic calcium ([Ca2+](i)) above ba sal levels. We have recently shown that low-level protein kinase C (PK C) activation by preincubation of acini with 1 nM 12-O-tetradecanoylph orbol-13-acetate (TPA) or minimally secreting concentrations of PKC-ac tivating receptor agonists (1 pM CCK-8, 0.1 mu M carbachol or 10 pM bo mbesin) cause supramaximal inhibition of OPE-stimulated enzyme secreti on. We now show that treatment of acini under these conditions also su ppresses the sustained rise of [Ca2+](i) stimulated by OPE to basal le vels in these cells, without changing the initial OPE-stimulated [Ca2](i) peak. The resultant pattern of calcium signalling is similar to t hat evoked by supramaximal concentrations of native CCK. This suggests that even low concentrations of PKC-activating agonists have the pote ntial to induce inhibitory effects on Ca2+ mobilization and that this kinase is important in generating the supramaximal inhibition observed in response to CCK.