Schlösser B, Kudernatsch M B, Sutor B, ten Bruggencate G
Department of Physiology, University of Munich, Germany.
Neurosci Lett. 1995 May 19;191(1-2):126-30. doi: 10.1016/0304-3940(94)11552-3.
The actions of opioid receptor agonists on stimulus evoked dopamine overflow in rat neostriatal slices were investigated using fast cyclic voltammetry. Activation of delta and mu receptors reversibly depressed striatal dopamine efflux induced by intrastriatal stimulation. The inhibitory effect of DADLE (D-Ala2, D-Leu5-enkephalin, delta/mu agonist), DPDPE (D-Pen2,5-enkephalin, delta selective) and DALDA (D-Arg2, Lys4-dermorphin-(1,4)-amide, mu selective), respectively, were concentration dependent and could be blocked by application of receptor subtype selective antagonists. At a concentration of 1 microM, the kappa receptor agonist U-50488H inhibited dopamine overflow. This effect could be partially antagonized by kappa receptor selective antagonists. Prior application of virtually ineffective concentrations (< or = 0.1 microM) of the kappa agonist reduced the efficacy of 1 microM U-50488H suggesting a desensitization of the receptor. Since the stimulus induced dopamine overflow in striatal slices can be attributed solely to the release of dopamine from presynaptic terminals, these experiments demonstrate that delta, mu and kappa opioid receptors exert an inhibitory control on striatal dopamine release via a presynaptic mechanism.
利用快速循环伏安法研究了阿片受体激动剂对大鼠新纹状体切片中刺激诱发的多巴胺释放的作用。δ和μ受体的激活可逆性地抑制了纹状体内刺激诱发的纹状体多巴胺外流。DADLE(D-丙氨酸2,D-亮氨酸5-脑啡肽,δ/μ激动剂)、DPDPE(D-青霉胺2,5-脑啡肽,δ选择性激动剂)和DALDA(D-精氨酸2,赖氨酸4-皮啡肽-(1,4)-酰胺,μ选择性激动剂)的抑制作用分别呈浓度依赖性,且可被受体亚型选择性拮抗剂阻断。在1微摩尔浓度下,κ受体激动剂U-50488H抑制多巴胺外流。这种作用可被κ受体选择性拮抗剂部分拮抗。预先应用实际上无效浓度(≤0.1微摩尔)的κ激动剂可降低1微摩尔U-50488H的效力,提示受体脱敏。由于纹状体切片中刺激诱发的多巴胺外流可完全归因于突触前终末多巴胺的释放,这些实验表明δ、μ和κ阿片受体通过突触前机制对纹状体多巴胺释放发挥抑制性控制。
