1. The effect of opiates on neurotransmission between visualized hypogastric nerve boutons and postganglionic cell bodies has been examined using extracellular recording of nerve bouton impulses (NBIs) and excitatory postsynaptic currents (e.p.s.cs). 2. Morphine (10 to 40 microM) did not affect neurotransmission in the ganglia. Dynorphin-A (4 microM) and U50488H (1 microM) decreased quantal transmitter release and naloxone (10 microM) reversed these effects. 3. Morphine (10 microM), dynorphin-A (4 microM) and U50488H (1 microM) did not affect either the time course or consistency with which the NBI was recorded. 4. Dynorphin-A (1 to 4 microM) and U50488H (1 microM) decreased the average amplitude of e.p.s.cs by increasing the number of failures to release quanta from single or small groups of 2 to 4 boutons during continuous nerve stimulation at 0.1 Hz. 5. The decrease in quantal release induced by dynorphin-A and U50488H in 0.2 to 0.5 mM [Ca2+]zero was readily reversed by increasing the extracellular calcium ion concentration to 1 mM. 6. It was concluded that kappa-opioid receptors are located on the boutons of the hypogastric nerve and when activated by kappa-opioid receptor agonists reduce quantal release without affecting the NBI.