Halothane inhibits the neurotoxin stimulated [14C]guanidinium influx through ‘silent’ sodium channels in rat glioma C6 cells

Abstract

We have investigated the effect of pharmacological agents on [¹⁴C]guanidinium ion influx through sodium channels in C₆ rat glioma and N18 mouse neuroblastoma cells. The sodium channels of the N18 cells can be activated by aconitme alone, indicating that they are voltage-dependent channels. In contrast, sodium channels in the C₆ cells require the synergistic action of aconitine and scorpion toxin for activation and are therefore characterized as so-called silent channels. The general anesthetic halothane used at clinical concentrations, specifically inhibited the ion flux through the silent sodium channel of C₆ rat glioma cells. The voltage-dependent channels of the N18 cells were insensitive to halothane at the concentrations tested.