Methyllycaconitine, α-bungarotoxin and (+)-tubocurarine block fast ATP-gated currents in rat dorsal root ganglion cells

Abstract

1. The effects of nicotinic acetylcholine receptor antagonists were studied on currents evoked by application of ATP to rat isolated dorsal root ganglion cells, and human embryonic kidney 293 cells expressing rat P2X 3 and P2X 2/3 receptors. 2. The rapidly desensitising (within 100 ms) current in dorsal root ganglion cells was inhibited by methyllycaconitine, α-bungarotoxin and (+)-tubocurarine (concentrations giving half-maximal inhibition were approximately 40, 60 and 800 nM, respectively), but not by hexamethonium (100 μM) or mecamylamine (100 μM). The sustained (> 250 ms) current in dorsal root ganglion cells was inhibited by (+)-tubocurarine (80% by 10 μM), but not by methyllycaconitine (200 nM), α-bungarotoxin (200 nM), mecamylamine (100 μM) or hexamethonium (100 μM). 3. Rapidly desensitising currents evoked by α,βmethylene-ATP in human embryonic kidney cells expressing P2X 3 receptors were inhibited by methyllycaconitine and α-bungarotoxin, at concentrations similar to those effective in dorsal root ganglion cells. 4. The results indicate that some nicotinic acetylcholine receptor antagonists are potent blockers of P2X receptors on neurons, particularly the homo-oligomeric P2X 3 receptor. This finding suggests that these drugs should be used with care to discriminate between P2X and neuronal acetylcholine receptor types.