Enhancement of retinal acetylcholine release by DAMGO: possibly a direct opioid receptor‐mediated excitatory effect

Abstract

An eye‐cup preparation in anaesthetized rabbits was used to examine opioid modulation of acetylcholine (ACh) release from cholinergic neurones in the retina. The μ‐opioid receptor agonist, [D‐Ala2, MePhe4, Gly‐ol5]‐enkephalin (DAMGO), when applied locally to the retina at concentrations between 1–30 μm significantly increased the light‐evoked release of ACh. The effect of DAMGO was completely blocked by the selective μ‐receptor antagonist CTOP but the k‐receptor antagonist nor‐binaltorphimine (norBNI) did not affect the action of DAMGO on ACh release indicating that the opioid produced its effect by activation of μ‐receptors (the rabbit retina has negligible δ‐receptors). Blockade with bicuculline and strychnine of GABAergic and glycinergic inputs to the cholinergic neurones did not affect the action of DAMGO on ACh release. Also DAMGO did not reduce the potassium‐evoked release of either GABA or glycine from rat isolated retinas. Exposure of the rabbit retina to a combination of an A1‐adenosine receptor antagonist, 8‐cyclopentyl‐1,3 dipropylxanthine (DPCPX), and adenosine deaminase did not affect the enhancing action of DAMGO on the light‐evoked release of ACh. When the retina in the rabbit eye‐cup was exposed to kainate, the release of ACh was increased by approximately three times the resting release. In the presence of DAMGO the kainate‐evoked release of ACh was enhanced by 44%. These experiments show that activation of μ‐opioid receptors by DAMGO increases the release of ACh elicited by physiological stimulation (flickering light). Since we could find no evidence that DAMGO reduces inhibitory inputs to the cholinergic neurones, it seems that the enhancing action of DAMGO on the light‐evoked release of ACh involves a direct excitatory effect rather than disinhibition. This conclusion is supported by the enhancing action of DAMGO on the kainate‐evoked release of ACh because kainate is thought to act directly on the cholinergic neurones. 1994 British Pharmacological Society