PENTOBARBITAL, DIAZEPAM, AND ETHANOL ABOLISH THE INTERPHASE DIMINUTION OF PAIN IN THE FORMALIN TEST - EVIDENCE FOR PAIN MODULATION BY GABA(A) RECEPTORS

There are two phases to the behavioral response to injection of formalin. After an initial vigourous response, a period of reduced pain occurs 10 to 15 n-tin after formalin, followed by reemergence of pain-related behaviors. These phases are believed to represent acute chemical stimulation of afferent neurons followed by injury-related inflammatory pain. Pentobarbital (10, 15, or 25 mg/kg), diazepam (0.5, 1.5, or 5.0 mg/kg), or ethanol (0.5, 1.0, or 1.5 g/kg) attenuated the diminution of pain between the two phases, so that pain was continuous throughout 60 min of testing, but had no effect on pain scores during the peaks of either phase. The effects of pentobarbital and diazepam were blocked by picrotoxin (2.5 mg/kg), which itself had no effect. Ro 15-1788 also blocked the effect of diazepam. Picrotoxin did not effectively antagonize the effect of ethanol. A high dose of picrotoxin (5.0 mg/kg) caused seizures in some rats and also eliminated the interphase depression of pain. The results suggest that the biphasic time course of formalin pain is produced by a central antinociceptive mechanism that is inhibited by GABA(A) receptors.