Effects of soman, an irreversible cholinesterase (ChE) inhibitor, on [ 3H]norepinephrine (NE) release evoked by N-methyl- d-aspartate (NMDA) were studied in rat brain cortical slices. Soman inhibited NMDA-stimulated [ 3H]NE release in a concentration-dependent manner. This effect was neither reversed by atropine, an antagonist of the muscarinic receptor, nor by d-tubocurarine, an antagonist of the nicotinic receptor. Incubation of the slices with NMDA antagonists, AP5, MK-801, ketamine or magnesium, resulted in inhibitory effects on NMDA-stimulated [ 3H]NE release. Soman significantly shifted the inhibition curves downward and significant interactions between these chemicals and soman were observed. Glycine potentiated the release of [ 3H]NE stimulated by NMDA, and soman did not alter this effect of glycine. Soman also inhibited the release of [ 3H]NE evoked by K + in a concentration-dependent manner. NMDA-stimulated [ 3H]NE release was inhibited by tetrodotoxin (TTX), an antagonist of voltage-dependent sodium channels, and a significant interaction between soman and TTX was observed. The [ 3H]NE release induced by NMDA was dependent on extracellular calcium concentrations and was inhibited by nifedipine, a selective blocker of the L-type voltage-dependent calcium channels (VDCC), or cadmium, a non-specific blocker of VDCC. However, no significant interaction between the effects of soman and calcium, nifedipine, or cadmium was observed. Taken together, the results suggested that: (1) soman has a direct action at non-cholinergic sites; (2) soman may interfere with some of the regulatory sites of the NMDA receptor–ion channel complex; and (3) the voltage-dependent sodium channel, but not VDCC, may be a site of action for soman.