| Abstract: | Intracellular recording techniques were used to investigate the effects of neuronal serotonin application, either by micropipet under pressure or by addition to the superfusing fluid, on membrane potential and conductance during experiments on spinal ganglia cells from adult rats. Serotonin action on spinal ganglia neurons induced depolarization with reduced conductance, hyperpolarization, and increased membrane conductance, as well as mixed response. Only one response pattern was examined. Depolarization response in spinal ganglia neurons sensitive to methysergide were potentiated by activating type 2 serotonin receptors (5HT2): e- and hyperpolarizing response insensitive to methysergide, propranolol, and cocaine action was produced via type 1 serotonin receptor (5HT1A). Neuronal response produced by serotonin (5HT2 mediation) did not depend on change in intraneuronal concentration of cAMP and the action of pertussis toxin. The second pattern of response was inhibited in the presence of pertussis toxin and modulated considerably by change in intraneuronal cAMP concentration and tryptazine action. Findings from research on ionic dependence showed that response mediated by 5HT2 resulted from blockade of M-current potassium channels and that brought about by 5HT1A is associated with disturbed function of cAMP-dependent potassium ionic channels.A. M. Gorkii Medical Institute, Donetsk. Translated from Neirofiziologiya, Vol. 21, No. 1, pp. 86–93, January–February, 1989. |
