Possible involvement of NMDA receptor‐mediated transmission in barbiturate physical dependence

Abstract

1 The competitive antagonists at the N-methyl-d-aspartate (NMDA) receptor, CGP39551 and CGP37849, protected against the barbiturate withdrawal syndrome in mice, as measured by ratings of convulsive behaviour on handling. 2 The effective doses of these compounds were lower than those required to prevent seizures due to NMDA in naive animals; these were in turn lower than those needed to prevent the convulsive effects of the α-aminobutyric acid (GABA) antagonist, bicuculline. 3 The NMDA-receptor antagonists did not alter the increase in the incidence of convulsions due to the GABA_A antagonist, bicuculline, that is seen during barbiturate withdrawal, although the latencies to these convulsions during barbital withdrawal were significantly increased after CGP39551. 4 Barbiturate withdrawal did not affect the convulsive actions of NMDA, whether measured by the incidence of convulsions or by intravenous infusion. 5 The B_max for [³H]-dizocilpine ([³H]-MK801) binding was significantly increased by chronic barbital treatment in cerebrocortical but not in hippocampal tissues, while the K_d remained unaltered in either case. 6 At 1 h and 24 h after administration of a single dose of barbitone, the B_max for [³H]-dizocilpine binding was unaltered in cerebrocortical tissue. Acute addition of barbitone in vitro did not alter [³H]-dizocilpine binding or the displacement of binding of thienylcyclohexylpyridine.