μ激动剂德莫啡肽与δ激动剂[D-Ala2，Glu4]强啡肽在脊髓上镇痛和δ阿片受体结合中的相互作用。

Interaction between the mu-agonist dermorphin and the delta-agonist [D-Ala2, Glu4]deltorphin in supraspinal antinociception and delta-opioid receptor binding.

作者信息

Negri L, Improta G, Lattanzi R, Potenza R L, Luchetti F, Melchiorri P

机构信息

Institute of Medical Pharmacology, University La Sapienza, Roma, Italy.

出版信息

Br J Pharmacol. 1995 Dec;116(7):2931-8. doi: 10.1111/j.1476-5381.1995.tb15947.x.

DOI:10.1111/j.1476-5381.1995.tb15947.x

PMID:8680727

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1909203/

Abstract

In rats, the interaction between the mu-opioid agonist dermorphin and the delta-opioid agonist [D-Ala2, Glu4]deltorphin was studied in binding experiments to delta-opioid receptors and in the antinociceptive test to radiant heat. 2. When injected i.c.v., doses of [D-Ala2, Glu4]deltorphin higher than 20 nmol produced antinociception in the rat tail-flick test to radiant heat. Lower doses were inactive. None of the doses tested elicited the maximum achievable response. This partial antinociception was accomplished with an in vivo occupancy of more than 97% of brain delta-opioid receptors and of 17% of mu-opioid receptors. Naloxone (0.1 mg kg-1, s.c.), and naloxonazine (10 mg kg-1, i.v., 24 h before), but not the selective delta-opioid antagonist naltrindole, antagonized the antinociception. 3. In vitro competitive inhibition studies in rat brain membranes showed that [D-Ala2, Glu4]deltorphin displaced [3H]-naltrindole from two delta-binding sites of high and low affinity. The addition of 100 microM Gpp[NH]p produced a three fold increase in the [D-Ala2, Glu4]deltorphin Ki value for both binding sites. The addition of 10 nM dermorphin increased the Ki value of the delta-agonist for the high affinity site five times. When Gpp[NH]p was added to the incubation medium together with 10 nM dermorphin, the high affinity Ki of the delta-agonist increased 15 times. 4. Co-administration into the rat brain ventricles of subanalgesic doses of dermorphin and [D-Ala2, Glu4]deltorphin resulted in synergistic antinociceptive responses. 5. Pretreatment with naloxone or with the non-equilibrium mu-antagonists naloxonazine and beta-funaltrexamine completely abolished the antinociceptive response of the mu-delta agonist combinations. 6. Pretreatment with the delta-opioid antagonists naltrindole and DALCE reduced the antinociceptive response of the dermorphin-[D-Ala2, Glu4]deltorphin combinations to a value near that observed after the mu-agonist alone. At the dosage used, naltrindole occupied more than 98% of brain delta-opioid receptors without affecting mu-opioid-receptors. 7. These data suggest that in the rat tail-flick test to radiant heat, mu- and delta-opioid agonists co-operate positively in evoking an antinociceptive response. Although interactions between different opioid pathways cannot be excluded, in vitro binding results indicate that this co-operative antinociception is probably mediated by co-activation of the delta-opioid receptors at the cellular level by the mu- and delta-agonist.

摘要

在大鼠中，通过δ-阿片受体结合实验以及对辐射热的抗伤害感受试验，研究了μ-阿片激动剂德莫啡肽与δ-阿片激动剂[D-Ala2，Glu4]德尔托啡肽之间的相互作用。2. 脑室内注射时，高于20 nmol的[D-Ala2，Glu4]德尔托啡肽剂量在大鼠辐射热甩尾试验中产生抗伤害感受作用。较低剂量无活性。所测试的剂量均未引发最大可实现反应。这种部分抗伤害感受作用是在体内占据超过97%的脑δ-阿片受体和17%的μ-阿片受体的情况下实现的。纳洛酮（0.1 mg/kg，皮下注射）和纳洛酮嗪（10 mg/kg，静脉注射，提前给药24小时）可拮抗这种抗伤害感受作用，但选择性δ-阿片拮抗剂纳曲吲哚则不能。3. 大鼠脑膜的体外竞争性抑制研究表明，[D-Ala2，Glu4]德尔托啡肽从高亲和力和低亲和力的两个δ-结合位点取代了[3H]-纳曲吲哚。加入100 μM Gpp[NH]p使[D-Ala2，Glu4]德尔托啡肽对两个结合位点的Ki值增加了三倍。加入10 nM德莫啡肽使δ-激动剂对高亲和力位点的Ki值增加了五倍。当Gpp[NH]p与10 nM德莫啡肽一起加入孵育培养基时，δ-激动剂的高亲和力Ki值增加了15倍。4. 将亚镇痛剂量的德莫啡肽和[D-Ala2，Glu4]德尔托啡肽共同注入大鼠脑室可产生协同抗伤害感受反应。5. 用纳洛酮或非平衡μ-拮抗剂纳洛酮嗪和β-氟奈曲胺预处理可完全消除μ-δ激动剂组合的抗伤害感受反应。6. 用δ-阿片拮抗剂纳曲吲哚和DALCE预处理可将德莫啡肽-[D-Ala2，Glu4]德尔托啡肽组合的抗伤害感受反应降低至接近单独使用μ-激动剂后观察到的值。在所使用的剂量下，纳曲吲哚占据超过98%的脑δ-阿片受体而不影响μ-阿片受体。7. 这些数据表明，在大鼠辐射热甩尾试验中，μ-和δ-阿片激动剂在引发抗伤害感受反应方面积极协同作用。尽管不能排除不同阿片途径之间的相互作用，但体外结合结果表明，这种协同抗伤害感受作用可能是由μ-和δ-激动剂在细胞水平上共同激活δ-阿片受体介导的。