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Kappa1- and kappa2-opioid receptors mediating presynaptic inhibition of dopamine and acetylcholine release in rat neostriatum.κ1和κ2阿片受体介导大鼠新纹状体中多巴胺和乙酰胆碱释放的突触前抑制。
Br J Pharmacol. 1997 Oct;122(3):520-4. doi: 10.1038/sj.bjp.0701394.
2
Pharmacological profile of various kappa-agonists at kappa-, mu- and delta-opioid receptors mediating presynaptic inhibition of neurotransmitter release in the rat brain.多种κ-激动剂对大鼠脑中介导神经递质释放突触前抑制作用的κ-、μ-和δ-阿片受体的药理学特性
Br J Pharmacol. 1991 Feb;102(2):518-22. doi: 10.1111/j.1476-5381.1991.tb12203.x.
3
Opioid receptor ligands in the neonatal rat spinal cord: binding and in vitro depression of the nociceptive responses.新生大鼠脊髓中的阿片受体配体:结合与伤害性反应的体外抑制
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4
Role of kappa opioid receptors in modulating cholinergic twitches in the circular muscle of guinea-pig colon.κ阿片受体在调节豚鼠结肠环形肌胆碱能抽搐中的作用。
Br J Pharmacol. 1996 Nov;119(5):985-9. doi: 10.1111/j.1476-5381.1996.tb15768.x.
5
Opioid receptor-mediated inhibition of dopamine and acetylcholine release from slices of rat nucleus accumbens, olfactory tubercle and frontal cortex.阿片受体介导对大鼠伏隔核、嗅结节和额叶皮质切片中多巴胺和乙酰胆碱释放的抑制作用。
Eur J Pharmacol. 1990 Jun 8;181(3):267-78. doi: 10.1016/0014-2999(90)90088-n.
6
Mu-, delta- and kappa-opioid receptor-mediated inhibition of neurotransmitter release and adenylate cyclase activity in rat brain slices: studies with fentanyl isothiocyanate.μ、δ和κ阿片受体介导的大鼠脑片神经递质释放及腺苷酸环化酶活性抑制:异硫氰酸芬太尼的研究
Eur J Pharmacol. 1988 Sep 13;154(2):169-78. doi: 10.1016/0014-2999(88)90094-5.
7
Delta, mu and kappa opioid receptor agonists inhibit dopamine overflow in rat neostriatal slices.δ、μ和κ阿片受体激动剂抑制大鼠新纹状体切片中的多巴胺外溢。
Neurosci Lett. 1995 May 19;191(1-2):126-30. doi: 10.1016/0304-3940(94)11552-3.
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Receptor selectivity of Met-enkephalin-Arg6-Phe7, an endogenous opioid peptide, in cerebral cortex of human and rat.内源性阿片肽甲硫氨酸脑啡肽-精氨酸6-苯丙氨酸7在人和大鼠大脑皮层中的受体选择性
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Opioid receptor antagonists discriminate between presynaptic mu and delta receptors and the adenylate cyclase-coupled opioid receptor complex in the brain.阿片受体拮抗剂可区分大脑中突触前的μ受体和δ受体以及与腺苷酸环化酶偶联的阿片受体复合物。
J Pharmacol Exp Ther. 1992 Oct;263(1):20-4.
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Opioid receptor-mediated inhibition of 3H-dopamine and 14C-acetylcholine release from rat nucleus accumbens slices. A study on the possible involvement of K+ channels and adenylate cyclase.阿片受体介导对大鼠伏隔核切片中3H-多巴胺和14C-乙酰胆碱释放的抑制作用。关于钾离子通道和腺苷酸环化酶可能参与情况的研究。
Naunyn Schmiedebergs Arch Pharmacol. 1992 Jun;345(6):627-32. doi: 10.1007/BF00164575.

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Divergent properties and independent regulation of striatal dopamine and GABA co-transmission.纹状体多巴胺和 GABA 共传递的发散特性和独立调控。
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Opioids in cancer: The κ‑opioid receptor (Review).阿片类药物在癌症中的作用:κ 阿片受体(综述)。
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Chronic ethanol exposure increases inhibition of optically targeted phasic dopamine release in the nucleus accumbens core and medial shell ex vivo.慢性乙醇暴露增加了在体外用光靶向法靶向伏隔核核心和中间壳的相位多巴胺释放的抑制作用。
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Biased agonists of the kappa opioid receptor suppress pain and itch without causing sedation or dysphoria.κ阿片受体的偏向性激动剂可抑制疼痛和瘙痒,且不会引起镇静或烦躁不安。
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Neuroprotection by the kappa-opioid receptor agonist, BRL52537, is mediated via up-regulating phosphorylated signal transducer and activator of transcription-3 in cerebral ischemia/reperfusion injury in rats.κ 阿片受体激动剂 BRL52537 通过上调脑缺血/再灌注损伤大鼠中磷酸化信号转导子和转录激活子 3 实现神经保护作用。
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κ1和κ2阿片受体介导大鼠新纹状体中多巴胺和乙酰胆碱释放的突触前抑制。

Kappa1- and kappa2-opioid receptors mediating presynaptic inhibition of dopamine and acetylcholine release in rat neostriatum.

作者信息

Schoffelmeer A N, Hogenboom F, Mulder A H

机构信息

Research Institute Neurosciences Vrije Universiteit, Department of Pharmacology, Free University, Medical Faculty, Amsterdam, The Netherlands.

出版信息

Br J Pharmacol. 1997 Oct;122(3):520-4. doi: 10.1038/sj.bjp.0701394.

DOI:10.1038/sj.bjp.0701394
PMID:9351509
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1564953/
Abstract
  1. The effects of selective opioid receptor agonists and antagonists on N-methyl-D-aspartate (NMDA, 10 microM)-induced release of [3H]-dopamine and [14C]-acetylcholine (ACh) from superfused neostriatal slices were studied to investigate the possible occurrence of functional kappa-opioid receptor subtypes in rat brain. 2. The kappa receptor agonists (-)-ethylketocyclazocine ((-)-EKC), U69593 and the endogenous opioid peptide dynorphin A1-13 caused a naloxone-reversible inhibition of NMDA-induced [3H]-dopamine release, with pD2 values of about 9, 8.5 and 8.2, respectively, whereas both the mu agonist Tyr-D-Ala-Gly-(NMe)Phe-Gly-ol (DAMGO) and the delta agonist D-Pen2-D-Pen5-enkephalin (DPDPE) were ineffective in this respect. The inhibitory effect of submaximally effective concentrations of dynorphin A1-13, U69593 and (-)-EKC on NMDA-induced [3H]-dopamine release were not changed by the delta1/delta2-opioid receptor antagonist naltrindole (up to a concentration of 1 microM, but reversed by the kappa receptor antagonist nor-binaltorphimine (nor-BNI), with an IC50) as low as 0.02 nM, indicating the involvement of U69593-sensitive kappa1-opioid receptors. 3. NMDA-induced [14C]-ACh release was reduced in a naloxone-reversible manner by DPDPE (pD2 about 7.2), dynorphin A1-13 (pD2 6.7) and EKC (pD2 6.2), but not by U69593 and DAMGO. The inhibitory effect of a submaximally effective concentration of DPDPE, unlike those of dynorphin A1-13 and (-)-EKC, on NMDA-induced [14C]-ACh release was antagonized by naltrindole with an IC50 of 1 nM, indicating the involvement of delta-opioid receptors in the inhibitory effect of DPDPE. On the other hand, the inhibitory effects of dynorphin A1-13 and (-)-EKC on [14C]-ACh release were readily antagonized by nor-BNI with an IC50 of about 3 nM. A 100 fold higher concentration of nor-BNI also antagonized the inhibitory effect of DPDPE, indicating the involvement of U69593-insensitive kappa2-opioid receptors in the inhibitory effects of dynorphin A1-13 and (-)-EKC. 4. Although naloxone benzoylhydrazone (NalBzoH), displaying high affinity towards the putative kappa3-opioid receptor, antagonized the inhibitory effects of dynorphin A1-13 and (-)-EKC on [3H]-dopamine and [14C]-ACh release as well as that of U69593 on [3H]-dopamine release, it displayed a low apparent affinity (IC50 about 100 nM) in each case. 5. In conclusion, whereas activation of kappa1-opioid receptors causes presynaptic inhibition of NMDA-induced dopamine release, kappa2 receptor activation results in inhibition of ACh release in rat neostriatum. As such, this study is the first to provide unequivocal in vitro evidence for the existence of functionally distinct kappa-opioid receptor subtypes in the brain.
摘要
  1. 研究了选择性阿片受体激动剂和拮抗剂对N-甲基-D-天冬氨酸(NMDA,10微摩尔)诱导的从灌流的新纹状体切片中释放[3H]-多巴胺和[14C]-乙酰胆碱(ACh)的影响,以研究大鼠脑中可能存在的功能性κ-阿片受体亚型。2. κ受体激动剂(-)-乙基酮环唑辛((-)-EKC)、U69593和内源性阿片肽强啡肽A1-13引起纳洛酮可逆性抑制NMDA诱导的[3H]-多巴胺释放,其pD2值分别约为9、8.5和8.2,而μ激动剂酪氨酰-D-丙氨酰-甘氨酰-(N-甲基)苯丙氨酰-甘氨醇(DAMGO)和δ激动剂D-青霉胺2-D-青霉胺5-脑啡肽(DPDPE)在这方面无效。强啡肽A1-13、U69593和(-)-EKC的次最大有效浓度对NMDA诱导的[3H]-多巴胺释放的抑制作用不受δ1/δ2-阿片受体拮抗剂纳曲吲哚(浓度高达1微摩尔)的影响,但被κ受体拮抗剂去甲二氢吗啡酮(nor-BNI)逆转,其IC50低至0.02纳摩尔,表明涉及U69593敏感的κ1-阿片受体。3. DPDPE(pD2约7.2)、强啡肽A1-13(pD2 6.7)和EKC(pD2 6.2)以纳洛酮可逆的方式降低了NMDA诱导的[14C]-ACh释放,但U69593和DAMGO没有。与强啡肽A1-13和(-)-EKC不同,DPDPE的次最大有效浓度对NMDA诱导的[14C]-ACh释放的抑制作用被纳曲吲哚拮抗,IC50为1纳摩尔,表明δ-阿片受体参与了DPDPE的抑制作用。另一方面,强啡肽A1-13和(-)-EKC对[14C]-ACh释放的抑制作用很容易被nor-BNI拮抗,IC50约为3纳摩尔。比nor-BNI高100倍的浓度也拮抗了DPDPE的抑制作用,表明U69593不敏感的κ2-阿片受体参与了强啡肽A1-13和(-)-EKC的抑制作用。4. 尽管对假定的κ3-阿片受体具有高亲和力的纳洛酮苯甲酰腙(NalBzoH)拮抗了强啡肽A1-13和(-)-EKC对[3H]-多巴胺和[14C]-ACh释放的抑制作用以及U69593对[3H]-多巴胺释放的抑制作用,但在每种情况下它都表现出低表观亲和力(IC50约100纳摩尔)。5. 总之,κ1-阿片受体的激活导致NMDA诱导的多巴胺释放的突触前抑制,而κ2受体的激活导致大鼠新纹状体中ACh释放的抑制。因此,本研究首次提供了明确的体外证据,证明脑中存在功能不同的κ-阿片受体亚型。