Your search keyword '"Naltrindole"' showing total 31 results

1. δ-Opioid receptors in the accumbens shell mediate the influence of both excitatory and inhibitory predictions on choice.

Author

Laurent, Vincent, Wong, Felix L, and Balleine, Bernard W

Abstract

Background and Purpose: Stimuli that predict rewarding events can control choice between future actions, and this control could be mediated by δ-opioid receptors in the nucleus accumbens shell (NAc-S). Stimuli predicting the absence of important events can also guide choice, although it remains unknown whether they do so via changes in an accumbal δ-opioid receptor-related process.Experimental Approach: δ-opioid receptor-eGFP mice were trained to perform two instrumental actions that delivered different food outcomes. Choice between the two actions was then tested in the presence of stimuli paired with either the delivery or the non-delivery of each of the two outcomes. Bilateral infusions of the δ-opioid receptor antagonist naltrindole into the NAc-S were used to determine the role of these receptors at the time of choice and δ-opioid receptor expression in the NAc-S used to assess functional activity.Key Results: A stimulus predicting a specific outcome biased choice performance towards the action previously earning that same outcome. In contrast, a stimulus signalling the absence of that outcome biased performance away from the action that delivered that outcome towards actions associated with the absence of that outcome. Both effects were associated with increased δ-opioid receptor expression on the membrane of cholinergic interneurons within the NAc-S. Furthermore, both effects were blocked by naltrindole infused into the NAc-S.Conclusions and Implications: These findings suggest that δ-opioid receptors in the NAc-S were involved in the effects of predictive learning on choice between actions, whether those predictions involve the presence or absence of specific rewarding events.Linked Articles: This article is part of a themed section on Opioids: New Pathways to Functional Selectivity. To view the other articles in this section visit http://dx.doi.org/10.1111/bph.2015.172.issue-2. [ABSTRACT FROM AUTHOR]

Published

2015

2. Augmentation of spinal morphine analgesia and inhibition of tolerance by low doses of mu- and delta-opioid receptor antagonists.

Author

Abul-Husn, N. S., Sutak, M., Milne, B., and Jhamandas, K.

Subjects

*ANALGESIA, *HORMONE antagonists, *DRUG receptors, *MORPHINE, *OPIOIDS, *DRUG tolerance, *DRUG dosage, *ANALGESICS, *ANIMAL experimentation, *CELL receptors, *COMPARATIVE studies, *DRUG interactions, *DOSE-effect relationship in pharmacology, *SPINAL injections, *RESEARCH methodology, *MEDICAL cooperation, *NALTREXONE, *NARCOTIC antagonists, *NARCOTICS, *PAIN, *PEPTIDES, *RATS, *RESEARCH, *SOMATOSTATIN, *EVALUATION research, *PAIN measurement, *PHARMACODYNAMICS

Abstract

Background and Purpose: Ultralow doses of naltrexone, a non-selective opioid antagonist, have previously been found to augment acute morphine analgesia and block the development of tolerance to this effect. Since morphine tolerance is dependent on the activity of micro and delta receptors, the present study investigated the effects of ultralow doses of antagonists selective for these receptor types on morphine analgesia and tolerance in tests of thermal and mechanical nociception.Experimental Approach: Effects of intrathecal administration of mu-receptor antagonists, CTOP (0.01 ng) or CTAP (0.001 ng), or a delta-receptor antagonist, naltrindole (0.01 ng), on spinal morphine analgesia and tolerance were evaluated using the tail-flick and paw-pressure tests in rats.Key Results: Both micro and delta antagonists augmented analgesia produced by a sub-maximal (5 microg) or maximal (15 microg) dose of morphine. Administration of the antagonists with morphine (15 microg) for 5 days inhibited the progressive decline of analgesia and prevented the loss of morphine potency. In animals exhibiting tolerance to morphine, administration of the antagonists with morphine produced a recovery of the analgesic response and restored morphine potency.Conclusions and Implications: Combining ultralow doses of micro- or delta-receptor antagonists with spinal morphine augmented the acute analgesic effects, inhibited the induction of chronic tolerance and reversed established tolerance. The remarkably similar effects of micro- and delta-opioid receptor antagonists on morphine analgesia and tolerance are interpreted in terms of blockade of the latent excitatory effects of the agonist that limit expression of its full activity. [ABSTRACT FROM AUTHOR]

Published

2007

3. Delta opioid receptor ligands modulate anxiety-like behaviors in the rat.

Author

Perrine, Shane A., Hoshaw, Brian A., and Unterwald, Ellen M.

Subjects

*OPIOID receptors, *ANXIETY, *RATS, *LOCOMOTION, *DIAZEPAM, *TRANQUILIZING drugs, *AMPHETAMINES, *ANIMALS, *BENZAMIDE, *CELL receptors, *DOSE-effect relationship in pharmacology, *HETEROCYCLIC compounds, *NALTREXONE, *PHARMACODYNAMICS

Abstract

The role of the delta opioid receptor in regulating anxiety-like behavior in male Sprague-Dawley rats was examined. Using an elevated plus maze, the effects of the selective delta opioid receptor antagonist naltrindole (1 or 5 mg kg(-1)) and agonist SNC80 (1, 5 or 20 mg kg(-1)) on anxiety-like behavior were measured. Anxiety was also measured following administration of diazepam (3 mg kg(-1)) and amphetamine (1 mg kg(-1)) and compared to the effects of SNC80. Locomotor activity following administration of naltrindole, SNC80, diazepam, and amphetamine was measured. Finally, the defensive burying paradigm was used to confirm the findings from the elevated plus maze. Results demonstrated that SNC80 produced dose-dependent anxiolytic effects similar to that of the classical antianxiety agent, diazepam. Administration of naltrindole caused anxiogenic behavior in rats further supporting the involvement of the delta opioid receptor system in regulating anxiety. Naltrindole also blocked the anxiolytic effects of SNC80. Amphetamine had no effect on anxiety-like behavior. SNC80 induced hyperactivity similar to amphetamine at the doses tested, while naltrindole and diazepam did not significantly affect locomotor activity. Although SNC80 can increase locomotor activity, control experiments reported herein indicate that hyperlocomotion is not sufficient to produce an anxiolytic response on the elevated plus maze. Together with the results from the defensive burying paradigm, this suggests that the effects of SNC80 on reducing anxiety are independent of its effects on locomotion. Collectively these data show that the delta opioid receptor system can regulate anxiety-like behavior in an anxiolytic (agonist) and anxiogenic (antagonist) manner. [ABSTRACT FROM AUTHOR]

Published

2006

4. PnPP-19, a spider toxin peptide, induces peripheral antinociception through opioid and cannabinoid receptors and inhibition of neutral endopeptidase

Author

M.E. de Lima, Daniela da Fonseca Pacheco, Igor D.G. Duarte, Ana Cristina Nogueira Freitas, Maurício F.M. Machado, and Adriana K. Carmona

Subjects

0301 basic medicine, Pharmacology, AM251, Cannabinoid receptor, Enkephalin, medicine.drug_class, medicine.medical_treatment, Anandamide, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Fatty acid amide hydrolase, Naltrindole, Opioid receptor, medicine, Cannabinoid, 030217 neurology & neurosurgery, medicine.drug

Abstract

Background and Purpose The synthetic peptide PnPP-19 has been studied as a new drug candidate to treat erectile dysfunction. However, PnTx2–6, the spider toxin from which the peptide was designed, induces hyperalgesia. Therefore, we intended to investigate the role of PnPP-19 in the nociceptive pathway. Experimental Approach Nociceptive thresholds were measured by paw pressure test. PnPP-19 was administered intraplantarly alone or with selective cannabinoid or opioid receptor antagonists. The hydrolysis of PnPP-19 by neutral endopeptidase (NEP) (EC 3.4.24.11), an enzyme that cleaves enkephalin, was monitored by HPLC and the cleavage sites were deduced by LC–MS. Inhibition by PnPP-19 and Leu-enkephalin of NEP enzyme activity was determined spectrofluorimetrically. Key Results PnPP-19 (5, 10 and 20 μg per paw) induced peripheral antinociception in rats. Specific antagonists of μ opioid receptors (clocinnamox), δ opioid receptors (naltrindole) and CB1 receptors (AM251) partly inhibited the antinociceptive effect of PnPP-19. Inhibition of fatty acid amide hydrolase by MAFP or of anandamide uptake by VDM11 enhanced PnPP-19-induced antinociception. NEP cleaved PnPP-19 only after a long incubation, and Ki values of 35.6 ± 1.4 and 14.6 ± 0.44 μmol·L−1 were determined for PnPP-19 and Leu-enkephalin respectively as inhibitors of NEP activity. Conclusions and Implications Antinociception induced by PnPP-19 appears to involve the inhibition of NEP and activation of CB1, μ and δ opioid receptors. Our data provide a greater understanding of the antinociceptive effects of PnPP-19. This peptide could be useful as a new antinociceptive drug candidate.

Published

2016

5. A novel mechanism for cytoprotection against hypoxic injury: δ-opioid receptor-mediated increase in Nrf2 translocation

Author

Ying Xia, Dongman Chao, Shan Cao, Honghao Zhou, and Gianfranco Balboni

Subjects

Pharmacology, Agonist, medicine.drug_class, Activator (genetics), Chromosomal translocation, Transfection, respiratory system, Biology, Cytoprotection, Molecular biology, Naltrindole, medicine, Viability assay, Receptor, medicine.drug

Abstract

Background and Purpose Hypoxia/reoxygenation induces synthesis of reactive oxygen species (ROS) which can attack macromolecules and cause brain injury. The transcription factor, nuclear factor (erythroid-derived 2)-like 2, (Nrf2), ia potent activator of genes with an antioxidant responsive element and Nrf2 can counteract oxidative injury by increasing expression of several antioxidative genes in response to ROS stress. Here, we show that activation of the δ-opioid receptor (DOR) increasedNrf2 protein expression and translocation, thereby leading to cytoprotection. Experimental Approach We used HEK293t cells exposed to 0.5% O2 for 16 h and then reoxygenated for 4 h as a model of hypoxia-reperfusion (H/R) injury. Real time PCR, Western blotting, siRNA and immunohistochemical techniques were used to follow Nrf2 expression and activity. Cell viability and damage (as LDH leakage) were also measured. Key Results H/R injury triggered Nrf2 translocation into the nucleus and up-regulated expression of several downstream genes, relevant to antioxidation, such as NAD(P)H:quinone oxidoreductase (NQO1). Incubation with the DOR agonist UFP-512 enhanced Nrf2 protein expression and translocation and up-regulated its downstream genes in normoxia and further increased Nrf2 expression and translocation after H/R, protecting the cells against loss of viability and damage. The effect of UFP-512 on Nrf2 nuclear translocation was blocked by the DOR antagonist, naltrindole. Also, DOR–mediated cytoprotection was strongly inhibited after transfection of HEK293t cells with Nrf2 siRNA. Conclusions and Implications The DOR agonist UFP-512 was cytoprotective against H/R injury and this effect was partly dependent on DOR-mediated increase in Nrf2 function.

Published

2015

6. δ-Opioid receptors up-regulate excitatory amino acid transporters in mouse astrocytes

Author

Jianfeng Liang, Harleen K. Sandhu, Gianfranco Balboni, Dong H. Kim, Yanbing Yu, Ying Xia, Li Zhang, and Dongman Chao

Subjects

Pharmacology, MAPK/ERK pathway, Agonist, medicine.drug_class, Biology, Receptor antagonist, Neuroprotection, Cell biology, Downregulation and upregulation, Naltrindole, medicine, Receptor, Protein kinase C, medicine.drug

Abstract

Background and Purpose Astrocytic excitatory amino acid transporters (EAATs) regulate extracellular glutamate concentrations and play a role in preventing neuroexcitotoxicity. As the δ-opioid receptor (DOP receptor) is neuroprotective against excitotoxic injury, we determined whether DOP receptor activation up-regulates EAAT expression and function. Experimental Approach We measured mRNA and protein expression of EAAT1, EAAT2 and EAAT3 in cultured mouse astrocytes exposed to a specific DOP receptor agonist (UFP-512) with or without a DOP receptor antagonist, DOP receptor siRNA or inhibitors of PKC, PKA, PI3K, p38, MAPK, MEK and ERK, and evaluated the function of EAATs by measuring glutamate uptake. Key Results Astrocytic DOP receptor mRNA and protein were suppressed by DOP receptor siRNA knockdown. DOP receptor activation increased mRNA and protein expression of EAAT1 and EAAT2, but not EAAT3, thereby enhancing glutamate uptake of astrocytes. DOP receptor-induced EAAT1 and EAAT2 expression was largely reversed by DOP receptor antagonist naltrindole or by DOP receptor siRNA knockdown, and suppressed by inhibitors of MEK, ERK and p38. DOP receptor-accelerated glutamate uptake was inhibited by EAAT blockers, DOP receptor siRNA knockdown or inhibitors of MEK, ERK or p38. In contrast, inhibitors of PKA, PKC or PI3K had no significant effect on DOP receptor-induced EAAT expression. Conclusions and Implications DOP receptor activation up-regulates astrocytic EAATs via MEK-ERK-p38 signalling, suggesting a critical role for DOP receptors in the regulation of astrocytic EAATs and protection against neuroexcitotoxicity. As decreased EAAT expression contributes to pathophysiology in many neurological diseases, including amyotrophic lateral sclerosis, our findings present a new platform for potential treatments of these diseases.

Published

2014

7. Sensitivity to μ-opioid receptor-mediated anti-nociception is determined by cross-regulation between μ- and δ-opioid receptors at supraspinal level

Author

Clara C Faura, María Rodríguez-Muñoz, J. Cremades, Juan J. Ballesta, and Javier Garzón

Subjects

Pharmacology, medicine.medical_specialty, medicine.drug_class, Chemistry, Stimulation, Receptor antagonist, Endocrinology, Opioid, Opioid receptor, Naltrindole, Internal medicine, medicine, Morphine, Potency, Receptor, medicine.drug

Abstract

BACKGROUND AND PURPOSE The perception of pain and its inhibition varies considerably between individuals, and this variability is still unexplained. The aim of the present study is to determine whether functional interactions between opioid receptors are involved in the inter-individual variability in the sensitivity to μ-opioid receptor agonists. EXPERIMENTAL APPROACH Anti-nociceptive tests, radioligand binding, stimulation of [35S]GTP–γ–S binding, inhibition of cAMP production and co-immunoprecipitation experiments were performed in two strains of rat (Sprague–Dawley bred at our university – SDU – and Wistar) that differ in their sensitivity to opioids. KEY RESULTS The increased anti-nociceptive potency of µ-opioid receptor agonists in SDU rats was reversed by the δ-opioid receptor antagonist, naltrindole. Inhibition of the binding of [3H] naltrindole by µ-opioid receptor agonists was different in brain membranes from SDU and Wistar rats. Differences were also evident in the effect of δ-opioid receptor ligands on the binding of [35S]GTP-γ–S stimulated by µ-opioid receptors agonists. No strain-related differences were detected in spinal cord membranes. The potency of morphine to inhibit cAMP production in brain membranes varied between the strains, in the presence of deltorphin II and naltrindole. Co-immunoprecipitation experiments demonstrated that δ-opioid receptors were associated with μ-opioid receptors to a higher extent in brain synaptosomal fractions from SDU than in those from Wistar rats. CONCLUSIONS AND IMPLICATIONS There was increased supraspinal cross-talk between μ and δ-opioid receptors in SDU, as compared with Wistar rats. This was related to an enhanced sensitivity to anti-nociception induced by µ-opioid receptor agonists.

Published

2012

8. Augmentation of spinal morphine analgesia and inhibition of tolerance by low doses of μ- and δ -opioid receptor antagonists

Author

Maaja Sutak, Noura S. Abul-Husn, Khem Jhamandas, and Brian Milne

Subjects

Pharmacology, Agonist, medicine.drug_class, business.industry, Analgesic, Opioid, Naltrindole, Opioid receptor, Drug tolerance, medicine, Morphine, business, Opioid antagonist, medicine.drug

Abstract

Background and purpose: Ultralow doses of naltrexone, a non-selective opioid antagonist, have previously been found to augment acute morphine analgesia and block the development of tolerance to this effect. Since morphine tolerance is dependent on the activity of μ and δ receptors, the present study investigated the effects of ultralow doses of antagonists selective for these receptor types on morphine analgesia and tolerance in tests of thermal and mechanical nociception. Experimental approach: Effects of intrathecal administration of μ-receptor antagonists, CTOP (0.01 ng) or CTAP (0.001 ng), or a δ-receptor antagonist, naltrindole (0.01 ng), on spinal morphine analgesia and tolerance were evaluated using the tail-flick and paw-pressure tests in rats. Key results: Both μ and δ antagonists augmented analgesia produced by a sub-maximal (5 μg) or maximal (15 μg) dose of morphine. Administration of the antagonists with morphine (15 μg) for 5 days inhibited the progressive decline of analgesia and prevented the loss of morphine potency. In animals exhibiting tolerance to morphine, administration of the antagonists with morphine produced a recovery of the analgesic response and restored morphine potency. Conclusions and implications: Combining ultralow doses of μ- or δ-receptor antagonists with spinal morphine augmented the acute analgesic effects, inhibited the induction of chronic tolerance and reversed established tolerance. The remarkably similar effects of μ- and δ-opioid receptor antagonists on morphine analgesia and tolerance are interpreted in terms of blockade of the latent excitatory effects of the agonist that limit expression of its full activity. British Journal of Pharmacology (2007) 151, 877–887; doi:10.1038/sj.bjp.0707277

Published

2007

9. Presynaptic opioid receptors on noradrenergic and serotonergic neurons in the human as compared to the rat neocortex

Author

Franziska Wedekind, Benjamin Berger, Thomas J. Feuerstein, Anna Katharina Rothmaier, Rolf Jackisch, and Josef Zentner

Subjects

Pharmacology, Agonist, medicine.medical_specialty, medicine.drug_class, (+)-Naloxone, Receptor antagonist, DAMGO, chemistry.chemical_compound, Nociceptin receptor, Endocrinology, chemistry, Naltrindole, Opioid receptor, Internal medicine, medicine, Norbinaltorphimine, medicine.drug

Abstract

1 Electrically evoked release of [3H]-noradrenaline ([3H]-NA) or [3H]-5-hydroxytryptamine ([3H]-5-HT) in slices of human and the rat neocortex was used to characterize presynaptic opioid receptors. 2 Release of [3H]-NA in rat neocortical slices was reduced only by the μ-receptor agonist DAMGO (pIC50: 7.27, CI95: [7.22, 7.32]; Imax: 77.6±1.6%; antagonized by naloxone: pA2: 8.88, CI95: [8.78, 8.98]). 3 Release of [3H]-NA in human neocortical slices was unaffected by DAMGO, but inhibited by the δ-receptor agonist DPDPE (Imax: 25.7±2.2%) and the κ-receptor agonist U-50,488H (19.7±2.7% inhibition at 1 μM). Both effects were antagonized by naltrindole (1 μM). 4 Release of [3H]-5-HT in rat neocortical slices, was inhibited by DAMGO (10 μM) and U-50,488H (1 and 10 μM) only in the presence of the 5-HT receptor antagonist methiotepin (1 μM). 5 Release of [3H]-5-HT in human neocortical slices was unaffected by DPDPE, but U-50,488H (Imax: 40.8±8.3%; antagonized by 0.1 μM norbinaltorphimine) and DAMGO (16.4±3.9% inhibition at 1 μM; antagonized by 0.1 μM naloxone) acted inhibitory. 6 Release of [3H]-5-HT in human neocortical slices was reduced by nociceptin/orphanin (0.1 and 1 μM). These effects were antagonized by the ORL1 antagonist J-113397 (1-[(3R,4R)-1-cyclo-octylmethyl-3-hydroxymethyl-4-piperidyl]-3-ethyl-1,3-dihydro-2H-benzimidazol-2-one; 0.1 μM). 7 This study provides evidence for significant species differences in opioid receptor-mediated modulation of NA and 5-HT-release in human vs rat neocortex. In rats, μ-opioid receptors modulate NA release, but 5-HT release is only weakly affected by μ- and κ-opioids. In contrast, NA release in human neocortex is modulated via δ-opioid receptors, but 5-HT release mainly via κ-opioid receptors. In addition also the ORL1 receptor seems to be involved in 5-HT release modulation. British Journal of Pharmacology (2006) 148, 795–806. doi:10.1038/sj.bjp.0706782

Published

2006

10. Agonist activity of naloxone benzoylhydrazone at recombinant and native opioid receptors

Author

D Concas, Pier Luigi Onali, and Maria C. Olianas

Subjects

Pharmacology, Agonist, medicine.medical_specialty, medicine.drug_class, GTPgammaS, Adenylyl cyclase, chemistry.chemical_compound, Nociceptin receptor, DAMGO, Endocrinology, chemistry, Opioid receptor, Naltrindole, Internal medicine, medicine, Receptor, medicine.drug

Abstract

1. In the present study, we examined the pharmacological activity of the putative kappa3-opioid receptor agonist naloxone benzoylhydrazone (NalBzoH) at recombinant human opioid receptors individually expressed in Chinese hamster ovary (CHO) cells and native opioid receptors present in rat striatum. 2. At the mu-opioid receptor (MOR), NalBzoH stimulated guanosine-5'-O-(3-[35S]thio)triphosphate ([35S]GTPgammaS) binding (pEC50=8.59) and inhibited cyclic AMP accumulation (pEC50=8.74) with maximal effects (Emax) corresponding to 55 and 65% of those obtained with the MOR agonist DAMGO, respectively. The MOR antagonist CTAP blocked the stimulatory effects of NalBzoH and DAMGO with similar potencies. 3. At the kappa-opioid receptor (KOR), NalBzoH stimulated [35S]GTPgammaS binding (pEC50=9.70) and inhibited cyclic AMP formation (pEC50=9.45) as effectively as the selective KOR agonist (-)-U-50,488. The NalBzoH effect was blocked by the KOR antagonist nor-binaltorphimine (nor-BNI) (pKi=10.30). 4. In CHO cells expressing the delta-opioid receptor (DOR), NalBzoH increased [35S]GTPgammaS binding (pEC50=8.49) and inhibited cyclic AMP formation (pEC50=8.61) almost as effectively as the DOR agonist DPDPE. Naltrindole (NTI), a selective DOR antagonist, completely blocked the response to NalBzoH (pKi of 10.40). 5. In CHO cells expressing the nociceptin/orphanin FQ (N/OFQ) receptor (NOP), NalBzoH failed to exert agonist effects and antagonized the agonist-induced receptor activation. 6. When compared to other opioid receptor ligands, NalBzoH showed an efficacy that was lower than that of morphine at MOR, but higher at KOR and DOR. 7. In rat striatum, NalBzoH enhanced [35S]GTPgammaS binding and inhibited adenylyl cyclase activity. These effects were antagonized by either CTAP, nor-BNI or NTI, each antagonist blocking a fraction of the NalBzoH response. 8. These data demonstrate that NalBzoH displays agonist activity at MOR, DOR and KOR expressed either in a heterologous cell system or in a native environment.

Published

2006

11. Characterisation of opioid receptors involved in modulating circular and longitudinal muscle contraction in the rat ileum

Author

Paul J. White, Ian M. Coupar, and Andrew Colin Gray

Subjects

Pharmacology, Agonist, medicine.medical_specialty, Enkephalin, medicine.drug_class, chemistry.chemical_compound, DAMGO, Endocrinology, chemistry, Competitive antagonist, Naltrindole, Opioid receptor, Internal medicine, medicine, DADLE, μ-opioid receptor, medicine.drug

Abstract

1. The aim of the present investigation was to characterise the opioid receptor subtypes present in the rat ileum using a method that detects drug action on the enteric nerves innervating the circular and longitudinal muscles. 2. Neurogenic contractions were reversibly inhibited by morphine (circular muscle pEC50, 6.43+/-0.17, Emax 81.7+/-5.0%; longitudinal muscle pEC50, 6.65+/-0.27, Emax 59.7+/-7.8%), the mu-opioid receptor-selective agonist, DAMGO ([D-Ala2,N-Me-Phe4,Gly5-ol]enkephalin acetate) (circular pEC50, 7.85+/-0.04, Emax 97.8+/-3.6%; longitudinal pEC50, 7.35+/-0.09, Emax 56.0+/-6.1%), the delta-selective agonist DADLE ([D-Ala2,D-Leu5]enkephalin acetate) (circular pEC50, 7.41+/-0.17, Emax, 93.3+/-8.4%; longitudinal pEC50, 6.31+/-0.07, Emax 66.5+/-5.2%) and the kappa-selective agonist U 50488H (trans-(+/-)-3,4-dichloro-N-methyl-N-[2-(1-pyrrolidinyl)cyclohexyl]benzeneacetamide methanesulphonate) (circular pEC50, 5.91+/-0.41, Emax, 83.5+/-26.8%; longitudinal pEC50, 5.60+/-0.08, Emax 74.3+/-7.2%). Agonist potencies were generally within expected ranges for activity at the subtype for which they are selective, except for U 50488H, which was less potent than expected. 3. The mu and delta receptor-selective antagonists, CTAP (H-D-Phe-Cys-Tyr-D-Trp-Arg-Thr-Pen-Thr-NH2) and naltrindole, caused progressive, parallel rightward shifts in the DAMGO and DADLE curves, respectively. Analysis indicated conformity to theoretical simple competitive antagonist behaviour. U 50488H effects were insensitive to the kappa-selective antagonist, n-BNI. A high concentration (1 microM) of naltrexone caused apparent potentiation of U 50488H effects. 4. CTAP pK(B) estimates were consistent with previously reported values for mu receptor antagonism (circular 7.84+/-0.17, longitudinal 7.64+/-0.35). However, the naltrindole pK(B) estimates indicated lower antagonist potency than expected (circular 8.22+/-0.23, longitudinal 8.53+/-0.35). 5. It is concluded that mu and possibly atypical delta receptors (but not kappa receptors) mediate inhibition of contraction in this model. Nonopioid actions of U 50488H are probably responsible for the inhibitory effects seen with this compound.

Published

2005

12. Pharmacological characterization of a 7-benzylidenenaltrexone-preferring opioid receptor in porcine ileal submucosa

Author

David R. Brown and DeWayne Townsend

Subjects

Pharmacology, medicine.medical_specialty, Enkephalin, medicine.drug_class, Chemistry, Narcotic antagonist, Antagonist, DAMGO, chemistry.chemical_compound, Endocrinology, Opioid receptor, Naltrindole, Internal medicine, medicine, Opioid peptide, Diprenorphine, medicine.drug

Abstract

In the intestine, opioids produce antidiarrhoeal and constipating actions that are mediated by enteric neurones. Through interactions with opioid receptors (ORs) on submucosal neurones, opioids suppress active ion transport evoked by transmural electrical stimulation (TES) in mucosa–submucosa sheets from the porcine ileum. In this study, we examined the pharmacological characteristics of the previously described OR, which is sensitive to the δ1-OR antagonist 7-benzylidenenaltrexone and modulates neurogenic transepithelial ion transport in this tissue preparation. Increases in short-circuit current (Isc, a measure of active anion transport) evoked by TES in ileal mucosa–submucosa sheets were inhibited by opioid agonists possessing high selectivity for either δ- or μ-ORs including [D-Pen2,5]enkephalin (DPDPE), [D-Ala2, Glu4]deltorphin II, and [D-Ala2, N-Me-Phe4, Gly5-ol]enkephalin (DAMGO). As determined by the Schild analysis, the actions of these agonists were competitively inhibited by 7-benzylidenenaltrexone. The nonequilibrium μ-OR antagonist β-funaltrexamine inhibited the actions of DAMGO only at a high concentration (1 μM) but did not alter DPDPE or deltorphin II action. At concentrations up to 10 μM, the nonequilibrium δ-OR antagonist naltrindole 5′-isothiocyanate did not alter the actions of δ- or μ-OR agonists. Radioligand binding analyses of neuronal homogenates from the ileal submucosa revealed that the nonselective OR ligand [3H]diprenorphine bound to two populations of specific binding sites. One of these sites possessed binding characteristics similar to the δ-OR. In summary, neurogenic ion transport in the porcine intestine is modulated by an OR which shares pharmacological characteristics of both μ- and δ-ORs and may represent a novel receptor entity. British Journal of Pharmacology (2003) 140, 691–700. doi:10.1038/sj.bjp.0705485

Published

2003

13. Involvement of μ - and κ -, but not δ -, opioid receptors in the peristaltic motor depression caused by endogenous and exogenous opioids in the guinea-pig intestine

Author

Ulrike Holzer-Petsche, Peter Holzer, Anaid Shahbazian, Helmut Schmidhammer, Eckhard Beubler, and Akos Heinemann

Subjects

Pharmacology, Agonist, medicine.medical_specialty, Cyprodime, medicine.drug_class, Receptor antagonist, DAMGO, chemistry.chemical_compound, Endocrinology, chemistry, Naltrindole, Opioid receptor, Internal medicine, medicine, Opioid peptide, Peristalsis, medicine.drug

Abstract

Opiates inhibit gastrointestinal propulsion, but it is not clear which opioid receptor types are involved in this action. For this reason, the effect of opioid receptor - selective agonists and antagonists on intestinal peristalsis was studied. Peristalsis in isolated segments of the guinea-pig small intestine was triggered by a rise of the intraluminal pressure and recorded via the intraluminal pressure changes associated with the peristaltic waves. Mu-opioid receptor agonists (DAMGO, morphine), kappa-opioid receptor agonists (ICI-204,448 and BRL-52,537) and a delta-opioid receptor agonist (SNC-80) inhibited peristalsis in a concentration-related manner as deduced from a rise of the peristaltic pressure threshold (PPT) and a diminution of peristaltic effectiveness. Experiments with the delta-opioid receptor antagonists naltrindole (30 nM) and HS-378 (1 microM), the kappa-opioid receptor antagonist nor-binaltorphimine (30 nM) and the mu-opioid receptor antagonist cyprodime (10 microM) revealed that the antiperistaltic effect of ICI-204,448 and BRL-52,537 was mediated by kappa-opioid receptors and that of morphine and DAMGO by mu-opioid receptors. In contrast, the peristaltic motor inhibition caused by SNC-80 was unrelated to delta-opioid receptor activation. Cyprodime and nor-binaltorphimine, but not naltrindole and HS-378, were per se able to stimulate intestinal peristalsis as deduced from a decrease in PPT. The results show that the neural circuits controlling peristalsis in the guinea-pig small intestine are inhibited by endogenous and exogenous opioids acting via mu- and kappa-, but not delta-, opioid receptors.

Published

2002

14. HS-599: a novel long acting opioid analgesic does not induce place-preference in rats

Author

G Improta, Roberta Lattanzi, Lucia Negri, Helmut Schmidhammer, Johannes Schütz, and Elisa Giannini

Subjects

Pharmacology, Agonist, medicine.medical_specialty, medicine.drug_class, business.industry, Deltorphin I, Dermorphin, Partial agonist, chemistry.chemical_compound, Endocrinology, chemistry, Naltrindole, Competitive antagonist, Internal medicine, medicine, Inverse agonist, business, medicine.drug, Buprenorphine

Abstract

When administered subcutaneously HS-599, a new didehydroderivative of buprenorphine (18,19-dehydrobuprenorphine), produced a long-lasting antinociceptive response in rats. Its potency exceeded twice that of buprenorphine. In the tail-flick test it acted as a full agonist but in the plantar test only as a partial agonist. Whereas the μ-opioid antagonists naloxone and naltrexone antagonized HS-599 antinociception the δ-opioid antagonist naltrindole and the κ-opioid antagonist nor-binaltorphimine did not. Unlike buprenorphine and morphine, HS-599 never induced conditioned place-preference in rats. In radioligand binding assays, compared with buprenorphine HS-599 had 3 fold higher μ-opioid receptor affinity but lower δ- and κ-opioid receptor affinity. In isolated guinea-pig ileum preparations, HS-599 only partially inhibited the electrically-stimulated contraction, acting as a partial opioid agonist. When tested against the μ-opioid receptor agonist dermorphin, it behaved as a non-equilibrium antagonist. Conversely, in mouse vas deferens (rich in δ-opioid receptors) and rabbit vas deferens preparations (rich in κ-opioid receptors) HS-599 acted as a pure equilibrium antagonist, shifting the log-concentration-response curves of the δ-opioid agonist deltorphin I and the κ-opioid agonist U-69593 to the right. In conclusion, HS-599 is a novel buprenorphine derivative with higher affinity, selectivity and potency than the parent compound, for μ-opioid receptors. It produces intense and long-lasting antinociception and does not induce place-preference in rats. British Journal of Pharmacology (2001) 134, 441–447; doi:10.1038/sj.bjp.0704280

Published

2001

15. Endogenous opioids suppress activation of nociceptors by sub-nanomolar nicotine

Author

Frederick Jia-Pei Miao, Jon D. Levine, and Neal L. Benowitz

Subjects

Pharmacology, medicine.medical_specialty, Chemistry, medicine.drug_class, (+)-Naloxone, Receptor antagonist, Extravasation, Nicotine, chemistry.chemical_compound, Nicotinic agonist, Endocrinology, Naltrindole, Internal medicine, medicine, Hexamethonium, medicine.drug, Endogenous opioid

Abstract

1. Nicotine can activate primary afferent nociceptors, one result of which is to increase neurogenic plasma extravasation. In this study we have demonstrated a novel proinflammatory effect of sub-nanomolar nicotine, mediated by peripheral action at sensory neurons. This action is normally masked by adrenal medulla-derived delta-opioid receptor agonists. 2. While neurogenic plasma extravasation in the knee joint of the rat was not increased by intra-articular perfusion of nicotine (10(-8) M), perfusion of nicotine, at concentrations as low as 10(-10) M, combined with naloxone to block opioid receptors (or naltrindole to block delta-opioid receptors) was able to enhance bradykinin-induced plasma extravasation. This pro-inflammatory effect of intra-articular nicotine was mimicked by subcutaneous nicotine which was abolished by intra-articularly-administered hexamethonium, a nicotinic receptor antagonist. 3. Following denervation of the adrenal medulla, intra-articular nicotine, alone at 10(-8) M, enhanced plasma extravasation, which was no longer enhanced by naloxone. 4. Destruction of primary afferents by neonatal treatment with capsaicin or blockade of sensory neurotransmitter by neurokinin-1 receptor antagonist RP-87,580 abolished the pro-inflammatory effect of nicotine. 5. The effect of nicotine we describe in promoting inflammation is exerted at extremely low concentrations and therefore could have relevance to smokers, patients receiving medicinal nicotine as therapy and even second-hand smokers. Since receptor mechanisms on peripheral terminals of nociceptors may also be present on central terminals, actions of the endogenous nicotinic agonist acetylcholine, at central terminals of primary afferents or at other sites in the central nervous system, may be similarly modulated by opioids.

Published

2001

16. Blockade of μ-opioid receptors reveals the hyperalgesic effect of orphanin FQ/nociceptin in the rat hot plate test

Author

Kabirullah Lutfy and Nigel T. Maidment

Subjects

Pharmacology, Opioidergic, medicine.medical_specialty, medicine.drug_class, Chemistry, (+)-Naloxone, Naltrexone, Nociceptin receptor, Endocrinology, Opioid, Opioid receptor, Naltrindole, Internal medicine, medicine, Opioid peptide, medicine.drug

Abstract

Orphanin FQ (OFQ, also known as nociceptin) has been proposed to oppose the antinociceptive effect of endogenous opioid peptides in the brain. We sought to determine whether, conversely, the endogenous opioid peptides counteract a pronociceptive action of OFQ. In testing this hypothesis, naloxone, a non-selective opioid receptor antagonist, was used to block the action of endogenous opioid peptides. We then examined whether OFQ would produce hyperalgesia in the absence of such an endogenous opioidergic tone. Neither naloxone (1 mg kg−1; s.c.) nor OFQ (up to 30 nmol; i.c.v.) alone induced any significant change in mean hot plate latency. However, OFQ dose-dependently produced hyperalgesia in rats pretreated with naloxone, implying that OFQ can indeed produce hyperalgesia once an endogenous opioidergic tone is inhibited. In subsequent studies, we used subtype selective opioid receptor antagonists to determine which class of opioid receptor is involved in this response. The effect of naloxone was reproduced using the selective μ-opioid receptor antagonist CTOP (D-Phe-Cyc-Tyr-D-Trp-Orn-Thr-Pen-Thr-NH2), but not by administration of the δ-opioid receptor antagonist, naltrindole (NTI) or the κ-opioid receptor antagonist nor-binaltorphimine (nor-BNI). These results suggest that endogenous opioid peptides acting at the μ-, but not κ- or δ-opioid receptor may be counteracting the hyperalgesic effect of OFQ in rats. British Journal of Pharmacology (2000) 131, 1684–1688; doi:10.1038/sj.bjp.0703746

Published

2000

17. Involvement of central opioid systems in human interferon-α induced immobility in the mouse forced swimming test

Author

Mitsuhiro Makino, Kiyoshi Takasuna, Chika Komiyama, Yutaka Kitano, and Masaaki Hirohashi

Subjects

Pharmacology, medicine.medical_specialty, medicine.drug_class, business.industry, Antagonist, Alpha interferon, Receptor antagonist, Endocrinology, Opioid, Naltrindole, Opioid receptor, Internal medicine, medicine, Receptor, business, medicine.drug, Behavioural despair test

Abstract

We investigated the mechanism by which human interferon-α (IFN-α) increases the immobility time in a forced swimming test, an animal model of depression. Central administration of IFN-α (0.05–50 IU per mouse, i.cist.) increased the immobility time in the forced swimming test in mice in a dose-dependent manner. Neither IFN-β nor -γ possessed any effect under the same experimental conditions. Pre-treatment with an opioid receptor antagonist, naloxone (1 mg kg−1, s.c.) inhibited the prolonged immobility time induced by IFN-α (60 KIU kg−1, i.v. or 50 IU per mouse. i.cist.). Peripheral administration of naloxone methiodide (1 mg kg−1, s.c.), which does not pass the blood–brain barrier, failed to block the effect of IFN-α, while intracisternal administration of naloxone methiodide (1 nmol per mouse) completely blocked. The effect of IFN-α was inhibited by a μ1-specific opioid receptor antagonist, naloxonazine (35 mg kg−1, s.c.) and a μ1/μ2 receptor antagonist, β-FNA (40 mg kg−1, s.c.). A selective δ-opioid receptor antagonist, naltrindole (3 mg kg−1, s.c.) and a κ-opioid receptor antagonist, nor-binaltorphimine (20 mg kg−1, s.c.), both failed to inhibit the increasing effect of IFN-α. These results suggest that the activator of the central opioid receptors of the μ1-subtype might be related to the prolonged immobility time of IFN-α, but δ and κ-opioid receptors most likely are not involved. British Journal of Pharmacology (2000) 130, 1269–1274; doi:10.1038/sj.bjp.0703432

Published

2000

18. Preweanling naltrindole administration differentially affects clonidine induced antinociception and plasma adrenaline levels in male and female neonatal rats

Author

Luis F. Alguacil, B. Fernández, Manuel Caamano, Antonio Aguilar, M Paz Viveros, Israel Alberti, and Eva Romero

Subjects

Pharmacology, Agonist, medicine.medical_specialty, Chemistry, medicine.drug_class, Analgesic, Naltrexone, Clonidine, Endocrinology, Nociception, Epinephrine, Naltrindole, Sympatholytic, Internal medicine, medicine, medicine.drug

Abstract

previously carried out in naive control neonatal rats. 4 In females, the functional blockade of the d-receptor by neonatal naltrindole treatment did not modify the sympatholytic eAect of clonidine but prevented clonidine induced antinociception. Conversely, in males naltrindole treatment allowed the appearance of clonidine antinociception and the sympatholytic eAect of clonidine. 5 The results indicate that the d-receptor is involved in the modulation of antinociceptive and sympatholytic responses to clonidine in neonatal rats and suggest the existence of sex diAerences in the interactions between d-opioid and a2-adrenergic receptors.

Published

1999

19. Constitutive activity of theδ-opioid receptor expressed in C6 glioma cells: identification of non-peptideδ-inverse agonists

Author

John R. Traynor, James H. Woods, Claire L. Neilan, and Huda Akil

Subjects

Pharmacology, Agonist, medicine.drug_class, Chemistry, (+)-Naloxone, Pertussis toxin, Naltriben, Opioid receptor, Naltrindole, medicine, Biophysics, Inverse agonist, Receptor, medicine.drug

Abstract

1. G-protein coupled receptors can exhibit constitutive activity resulting in the formation of active ternary complexes in the absence of an agonist. In this study we have investigated constitutive activity in C6 glioma cells expressing either the cloned delta-(OP1) receptor (C6delta), or the cloned mu-(OP3) opioid receptor (C6mu). 2. Constitutive activity was measured in the absence of Na+ ions to provide an increased signal. The degree of constitutive activity was defined as the level of [35S]-GTPgammaS binding that could be inhibited by pre-treatment with pertussis toxin (PTX). In C6delta cells the level of basal [35S]-GTPgammaS binding was reduced by 51.9+/-6.1 fmols mg-1 protein, whereas in C6mu; and C6 wild-type cells treatment with PTX reduced basal [35S]-GTPgammaS binding by only 10.0+/-3.5 and 8.6+/-3.1 fmols mg-1 protein respectively. 3. The delta-antagonists N, N-diallyl-Tyr-Aib-Aib-Phe-Leu-OH (ICI 174,864), 7-benzylidenenaltrexone (BNTX) and naltriben (NTB), in addition to clocinnamox (C-CAM), acted as delta-opioid receptor inverse agonists. Naloxone, buprenorphine, and naltrindole were neutral antagonists. Furthermore, naltrindole blocked the reduction in [35S]-GTPgammaS binding caused by the inverse agonists. The inverse agonists did not inhibit basal [35S]-GTPgammaS binding in C6mu; or C6 wild-type cell membranes. 4. Competition binding assays in C6delta cell membranes revealed a leftward shift in the displacement curve of [3H]-naltrindole by ICI 174,864 and C-CAM in the presence of NaCl and the GTP analogue, GppNHp. There was no change in the displacement curve for BNTX or NTB under these conditions. 5. These data confirm the presence of constitutive activity associated with the delta-opioid receptor and identify three novel, non-peptide, delta-opioid inverse agonists.

Published

1999

20. Spinal effect of a neuropeptide FF analogue on hyperalgesia and morphine-induced analgesia in mononeuropathic and diabetic rats

Author

Christine Courteix, Joseph Fialip, Marie-Ange Coudoré-Civiale, Anne-Marie Privat, Alain Eschalier, and Jean-Marie Zajac

Subjects

Pharmacology, business.industry, Naltrexone, Dose–response relationship, Nociception, Naltrindole, Neuropathic pain, Hyperalgesia, Morphine, Medicine, Neuropeptide FF, medicine.symptom, business, medicine.drug

Abstract

1DMe, a neuropeptide FF (NPFF) analogue, has been shown to produce antinociception and to enhance morphine analgesia in rats after intrathecal administration. To determine whether 1DMe could correct hyperalgesia and restore morphine efficacy in mononeuropathic (MN) and diabetic (D) rats we examined the spinal effect of 1DMe in MN and D rats without and after spinal blockade of mu- and delta-opioid receptors with CTOP and naltrindole, respectively. The influence of 1DMe on morphine-induced antinociception was assessed in the two models using isobolographic analysis. Whereas 1DMe intrathecally injected (0.1, 1, 7.5 microg rat(-1)) was ineffective in normal (N) rats, it suppressed mechanical hyperalgesia (decrease in paw pressure-induced vocalisation thresholds) in both MN and D rats. This effect was completely cancelled by CTOP (10 microg rat(-1)) and naltrindole (1 microg rat(-1)) suggesting that it requires the simultaneous availability of mu- and delta-opioid receptors. The combinations of morphine: 1DMe (80.6:19.4% and 99.8:0.2%, in MN and D rats, respectively) followed by isobolographic analysis, showed a superadditive interaction, relative to the antinociceptive effect of single doses, in D rats only. In N rats, the combination of morphine: 1DMe (0.5 mg kg(-1), i.v.: 1 microg rat(-1), i.t., ineffective doses) resulted in a weak short-lasting antinociceptive effect. These results show a different efficacy of 1DMe according to the pain model used, suggesting that the pro-opioid effects of the NPFF in neuropathic pain are only weak, which should contribute to hyperalgesia and to the impaired efficacy of morphine.

Published

1999

21. Nociceptin inhibits non-adrenergic non-cholinergic contraction in guinea-pig airway

Author

Domenico Spina, Clive P. Page, and S Shah

Subjects

Pharmacology, medicine.medical_specialty, Antagonist, Neuropeptide, Substance P, Peptide hormone, chemistry.chemical_compound, Nociceptin receptor, Endocrinology, chemistry, Capsaicin, Naltrindole, Internal medicine, medicine, Norbinaltorphimine, medicine.drug

Abstract

1. Electrical field stimulation (EFS) of guinea-pig isolated main bronchi induced a non-adrenergic non-cholinergic (NANC) contractile response. Nociceptin (0.01-1 microm) significantly inhibited the contractile response to EFS (P 0.05). 2. The mu-, delta- and kappa-opioid receptor antagonists, naloxone (0.3 microM), naltrindole (3 microM) and norbinaltorphimine (1 microm), respectively, did not significantly affect the inhibitory effect of nociceptin (0.03 microM; P>0.05). 3. The novel nociceptin antagonist, [Phe1psi(CH2-NH)Gly2]nociceptin(1-13)NH2 (0.03-1 microM); the sigma ligands, carbetapentane (30 microM), 3-phenylpiperidine (30-100 microM) and (+)-cyclazocine (10-100 microM) significantly reversed the inhibitory effect of nociceptin (0.03 microM, P 0.05). 4. EFS of guinea-pig bronchial preparations significantly increased SP-LI release above basal SP-LI (P

Published

1998

22. The involvement of the opioidergic system in the antinociceptive mechanism of action of antidepressant compounds

Author

Alex Gray, Robert David Edmund Sewell, and P.S.J. Spencer

Subjects

Pharmacology, Opioidergic, medicine.medical_specialty, medicine.drug_class, business.industry, (+)-Naloxone, Naltrexone, Endocrinology, Opioid, Naltrindole, Opioid receptor, Internal medicine, medicine, business, Opioid peptide, medicine.drug, Endogenous opioid

Abstract

Debate exists as to the nature of antidepressant-induced antinociception. It is unclear whether antidepressants are inherently antinociceptive, are able to potentiate opioid antinociception or both. We have used the acetic acid induced abdominal constriction assay in mice to investigate antidepressant-induced antinociception. All the antidepressants tested (s.c.) produced dose-dependent protection against acetic acid-induced abdominal constriction. Similarly, morphine and aspirin were also effective antinociceptive agents in this nociceptive assay. Opioid antagonists, naloxone (0.5 mg kg−1, s.c.) and naltrindole (1 mg kg−1, s.c.), shifted the dose-response relationships to the right for each of the antidepressant agents (dothiepin, amitriptyline, sibutramine, (+)-oxaprotiline and paroxetine). In this context the naloxone dose-ratios were 1.95, 3.90, 2.32, 4.50 and 2.65, with naltrindole dose-ratios of 4.36, 17.00, 4.28, 11.48 and 2.65 were obtained, respectively. Naloxone also shifted the morphine dose-response relationship to the right, by a factor of 2.62, whilst naltrindole had no effect upon morphine antinociception. Aspirin antinociception remained unaffected by both opioid antagonists. The enkephalin catabolism inhibitor acetorphan, by itself, produced no activity in this test at a dose of 10 mg kg−1 (s.c.). However, at higher doses, acetorphan produced a linear dose-response relationship against acetic acid-induced abdominal constriction. When acetorphan was administered before either the antidepressants or morphine, there was a clear potentiation of the antidepressant- or morphine-induced antinociception. However, acetorphan had no effect on aspirin antinociception. Since neither of the opioid antagonists were able to attenuate, nor was acetorphan able to potentiate, aspirin antinociception, we concluded that the mechanism of antidepressant-induced antinociception is different from that of the non-steroidal anti-inflammatory drugs. These data are consistent with the view that antidepressants may induce endogenous opioid peptide release, as shown by the acetorphan study. In this context, the ability of naltrindole to displace the antidepressant dose-response relationship to the right without affecting morphine antinociception, implicates the δ-opioid receptor and endogenous opioid peptides in antidepressant-induced antinociception.

Published

1998

23. κ1 - and κ2 -opioid receptors mediating presynaptic inhibition of dopamine and acetylcholine release in rat neostriatum

Author

Arie H. Mulder, François Hogenboom, and Anton N. M. Schoffelmeer

Subjects

Pharmacology, Agonist, medicine.medical_specialty, medicine.drug_class, Dynorphin, (+)-Naloxone, Receptor antagonist, κ-opioid receptor, DAMGO, chemistry.chemical_compound, Endocrinology, chemistry, Naltrindole, Opioid receptor, Internal medicine, medicine, medicine.drug

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.

Published

1997

24. l-Leucyl-l-arginine, naltrindole and d-arginine block antinociception elicited by l-arginine in mice with carrageenin-induced hyperalgesia

Author

Yumiko Nishimura, Atsufumi Kawabata, and Hiroshi Takagi

Subjects

Male, Indoles, Arginine, Injections, Subcutaneous, Narcotic Antagonists, (+)-Naloxone, Pharmacology, Carrageenan, Kyotorphin, Mice, chemistry.chemical_compound, Naltrindole, Randall–Selitto test, medicine, Animals, Pain Measurement, Opioidergic, Analgesics, business.industry, Antagonist, Brain, Stereoisomerism, Dipeptides, Naltrexone, Morphinans, chemistry, Hyperalgesia, Anesthesia, Endorphins, medicine.symptom, business, Research Article, medicine.drug

Abstract

1. Intraplantar injection of carrageenin into the mouse hind paw produced hyperalgesia when measured by the paw pressure test (Randall & Selitto method). 2. Subcutaneous administration of L-arginine (100-1,000 mg kg-1), a possible precursor of kyotorphin which is an endogenous analgesic neuropeptide, inhibited carrageenin-induced hyperalgesia in a dose-dependent manner. This effect was blocked by subcutaneous administration of naloxone, naltrindole, a selective delta-opioid receptor antagonist (enkephalin antagonist), and D-arginine. 3. Intracerebroventricular administration of L-leucyl-L-arginine inhibited the antinociceptive effect of systemically administered L-arginine in hyperalgesic mice. 4. Intracerebroventricular administration of L-arginine (3 and 30 micrograms per mouse) and kyotorphin (300 ng-3 micrograms per mouse) produced antinociception in hyperalgesic mice. The antinociceptive effects of L-arginine but not kyotorphin were blocked by intracerebroventricular administration of D-arginine. 5. These results suggest that L-arginine-induced antinociception is mediated by activation of 'kyotorphinergic' nerves followed by activation of the 'opioidergic' (possible 'enkephalinergic') nerves in the central nervous system.

Published

1992

25. Modulation of peristalsis in the guinea-pig isolated small intestine by exogenous and endogenous opioids

Author

Marcello Costa, Marcello Tonini, and Sally A. Waterman

Subjects

Male, Narcotics, Agonist, medicine.medical_specialty, Enkephalin, medicine.drug_class, Guinea Pigs, In Vitro Techniques, Dynorphins, chemistry.chemical_compound, Naltrindole, Internal medicine, Intestine, Small, medicine, Animals, Endogenous opioid, Peristalsis, Pharmacology, Analgesics, Enkephalins, Enkephalin, Ala(2)-MePhe(4)-Gly(5), DAMGO, Endocrinology, chemistry, Receptors, Opioid, Female, Endorphins, medicine.symptom, Enkephalin, D-Penicillamine (2,5), Norbinaltorphimine, Algorithms, Research Article, Muscle Contraction, Muscle contraction, medicine.drug

Abstract

1. A recording method was developed to measure physiological parameters of the preparatory and emptying phases of peristalsis in vitro. This method enabled measurement of: the compliance of the intestinal wall during the preparatory phase (a reflection of the resistance of the wall to distension); longitudinal muscle contraction during the preparatory phase; the threshold volume required to trigger the emptying phase; the maximal ejection pressure and the average power generated during the emptying phase, which reflects the rate at which the intestine performs work. Modulation of these parameters by exogenous and endogenous opioids acting at mu, kappa and delta opioid receptors was investigated. 2. The compliance of the intestinal wall during the preparatory phase was reduced by the mu opioid receptor agonist, [D-Ala2, N-methyl-Phe4, Gly5-ol] enkephalin (DAMGO) but not by the kappa agonist, dynorphin, or the delta agonist, [D-penicillamine2, D-penicillamine5] enkephalin (DPDPE). Reflex contraction of the longitudinal muscle during the preparatory phase was inhibited by DAMGO, dynorphin and DPDPE. The threshold volume required to trigger the emptying phase of peristalsis was increased by DAMGO, dynorphin and DPDPE. 3. The maximal ejection pressure generated during the emptying phase was reduced by dynorphin and DPDPE, but not by DAMGO. The average power generated by the intestine when emptying was not altered by any of the agonists. 4. Electrically stimulated contractions of longitudinal muscle in strips of longitudinal muscle-myenteric plexus were not inhibited by DPDPE. Similarly, DPDPE did not significantly inhibit electrically induced contraction of circular muscle in strips of circular muscle-myenteric plexus.5. Each of the agonist effects on peristaltic parameters was antagonized by the appropriate antagonist:D-Phe-Cys-Tyr-D-Trp-Orn-Thr-Pen-Thr-NH2 (CTOP) (mu), norbinaltorphimine (nor-BNI) (kappa), naltrindole(delta).6. It is concluded that mu and kappa agonists act primarily on excitatory circular and longitudinal muscle motor neurones. The delta agonist probably acts on enteric neurones presynaptic to excitatory circular and longitudinal muscle motor neurones.7. Antagonists for mu, delta and kappa receptors did not affect any parameters of peristalsis when the intestine emptied against a low resistance. However, when emptying against a high outflow resistance, the average power generated by the intestine was increased by the kappa antagonist, nor-BNI, but not by CTOP or naltrindole.8. It is concluded that endogenous opioids appear to have little role in peristalsis when the intestine is working against a low outflow resistance. However endogenous opioids, acting primarily at kappa receptors,provide a braking mechanism by inhibiting the emptying phase of peristalsis in conditions in which the intestine empties against a higher resistance.

Published

1992

26. Antagonism of swim-stress-induced antinociception by the δ-opioid receptor antagonist naltrindole in adult and young rats

Author

Sally R. Pinker and Ian Kitchen

Subjects

Male, Agonist, Aging, medicine.medical_specialty, Indoles, medicine.drug_class, Narcotic Antagonists, Physical Exertion, Pharmacology, Naltrexone, chemistry.chemical_compound, Naltrindole, Corticosterone, Opioid receptor, Receptors, Opioid, delta, Internal medicine, medicine, Animals, Antagonist, Nociceptors, Rats, Inbred Strains, Receptor antagonist, Rats, Endocrinology, Animals, Newborn, Morphinans, chemistry, Receptors, Opioid, Antagonism, Stress, Psychological, Research Article, medicine.drug

Abstract

1. The availability of the non-peptide delta-opioid receptor antagonist naltrindole has provided the possibility for in vivo studies on the function of delta-opioid receptors. We have studied the effects of naltrindole on swim-stress-induced antinociception in adult and neonatal rats. 2. Adult, 25 and 20 day old rats were stressed by warm water (20 degrees C) swimming for 3 min periods and antinociception was assessed by the tail immersion test (50 degrees C). 3. Naltrindole (0.5 and 1 mg kg-1) antagonized swim-stress-induced antinociception in adult and 25 day old rats but in 20 day old rats naltrindole (1 mg kg-1) was without effect. 4. Antinociception induced by the highly mu-opioid receptor selective agonist alfentanil was completely antagonized by naloxone (1 mg kg-1) but virtually unaffected by naltrindole (1 mg kg-1). 5. Neither naloxone nor naltrindole (1 mg kg-1) antagonized swim-stress-induced rises in plasma corticosterone in adult rats at the time of peak antinociception. 6. In conclusion, naltrindole shows in vivo antagonism of opioid-mediated responses. Swim-stress-induced antinociception is mediated through the delta-opioid receptor in 25 day old and adult rats and through the mu-opioid site in 20 day old animals.

Published

1990

27. Inhibition of tachykinin release from peripheral endings of sensory nerves by nociceptin, a novel opioid peptide

Author

Sandro Giuliani and Carlo Alberto Maggi

Subjects

Male, medicine.medical_specialty, Narcotic Antagonists, Neurokinin A, Guinea Pigs, Stimulation, (+)-Naloxone, In Vitro Techniques, chemistry.chemical_compound, Naltrindole, Internal medicine, Tachykinins, medicine, Animals, Kidney Pelvis, Neurons, Afferent, Peripheral Nerves, Opioid peptide, Pharmacology, Nerve Endings, Electric Stimulation, Nociceptin receptor, medicine.anatomical_structure, Endocrinology, Opioid, chemistry, Opioid Peptides, Receptors, Opioid, medicine.drug, Sensory nerve, Muscle Contraction, Research Article

Abstract

The novel heptadecapeptide opioid, nociceptin, produced a concentration-dependent (EC50 28 nM) suppression of the inotropic response of the guinea-pig isolated renal pelvis to electrical stimulation, a response mediated by release of tachykinins from sensory nerves. Nociceptin did not affect the response to neurokinin A, indicating a prejunctional site of action on tachykininergic nerves. The effect of nociceptin was unchanged in the presence of the mu, delta and kappa opioid receptor antagonists, naloxone, naltrindole and nor-binaltorphimine.

Published

1996

28. Antidepressant-like effects of CCKB antagonists in mice: antagonism by naltrindole

Author

M. Derrien, C. Durieux, and B.P. Roques

Subjects

Male, medicine.medical_specialty, Conditioning, Classical, Molecular Sequence Data, Pharmacology, Motor Activity, Cholecystokinin receptor, Naltrexone, Mice, Naltrindole, Internal medicine, medicine, Animals, Drug Interactions, Amino Acid Sequence, Receptor, Cholecystokinin, Benzodiazepinones, Behavior, Animal, Chemistry, Phenylurea Compounds, Antagonist, Antidepressive Agents, Peptide Fragments, Endocrinology, Mechanism of action, Opioid, Receptors, Cholecystokinin, medicine.symptom, hormones, hormone substitutes, and hormone antagonists, medicine.drug, Research Article

Abstract

1. The effects of selective CCKB agonists, BC 264 and BC 197 were investigated in the conditioned suppression of motility test in mice, an animal model used to select antidepressant drugs. The results showed that both CCKB agonists at doses of 3 and 30 micrograms kg-1, accentuated the suppression of motility in shocked mice and did not modify the behaviour of non-shocked mice. The effects of BC 264 were suppressed by L-365,260. 2. L-365,260 alone, at doses of 0.2 and 2 mg kg-1 decreased motor inhibition in shocked mice and had no effect in non-shocked mice. 3. The effects of L-365,260 observed in shocked mice were suppressed by naltrindole, a selective antagonist for delta-opioid receptors, suggesting the occurrence of physiological adverse interactions between CCK and opioid systems. 4. Together, these results suggest that CCKB antagonists could block centrally located CCKB receptors to produce antidepressant-like effects which could indirectly involve delta-opioid receptor stimulation.

Published

1994

29. L-arginine exerts a dual role in nociceptive processing in the brain: involvement of the kyotorphin-Met-enkephalin pathway and NO-cyclic GMP pathway

Author

Hiroshi Takagi, Atsufumi Kawabata, and Nahoko Umeda

Subjects

Met-enkephalin, Male, Enkephalin, Enkephalin, Methionine, Narcotic Antagonists, Mice, Inbred Strains, (+)-Naloxone, Pharmacology, Arginine, Nitric Oxide, Kyotorphin, chemistry.chemical_compound, Mice, Naltrindole, Neural Pathways, medicine, Animals, Endorphins, Cyclic GMP, Injections, Intraventricular, Pain Measurement, Analgesics, Naloxone, Brain, Nociceptors, Dibutyryl Cyclic GMP, Naltrexone, Methylene Blue, NG-Nitroarginine Methyl Ester, chemistry, Biochemistry, Spinal Cord, Tail flick test, medicine.drug, Research Article

Abstract

1. Intracerebroventricular (i.c.v.) administration of L-arginine (L-Arg), at 10-100 micrograms per mouse, produced antinociception in mice, as assessed by the tail flick test; this antinociception was reversed by pretreatment (s.c.) with naltrindole (NTI), a delta-selective opioid antagonist, and by co-administered L-leucyl-L-arginine (Leu-Arg), a kyotorphin (endogenous Met-enkephalin releaser) receptor antagonist. 2. L-NG-nitroarginine methyl ester (L-NAME), a NO synthase inhibitor, but not D-NG-nitroarginine methyl ester, given i.c.v. at 3-10 micrograms per mouse, exhibited antinociceptive activity that was resistant to naloxone (s.c.), NTI (s.c.) and Leu-Arg (i.c.v.). 3. The L-NAME (i.c.v.)-induced antinociception was not reversed by L-Arg (i.c.v.), which was antinociceptive by itself, but was abolished by combined injection of L-Arg plus Leu-Arg (i.c.v.) or by L-Arg (i.c.v.) after NTI (s.c.). 4. Methylene blue (MB), a soluble guanylate cyclase inhibitor, at 0.1-1 microgram per mouse, produced antinociception by i.c.v. administration. The antinociception induced by MB (i.c.v.) or L-NAME (i.c.v.) was reversed by co-administered dibutyryl cyclic GMP. 5. These findings suggest that L-Arg plays a dual role in nociceptive processing in the brain, being antinociceptive via the kyotorphin-Met-enkephalin pathway and nociceptive via the NO-cyclic GMP pathway.

Published

1993

30. Effects of the delta-opioid receptor antagonist naltrindole on antinociceptive responses to selective delta-agonists in post-weanling rats

Author

Ian Kitchen, T.J. Crook, and Raymond G. Hill

Subjects

Male, medicine.medical_specialty, Indoles, Enkephalin, medicine.drug_class, Deltorphin I, Narcotic Antagonists, Pharmacology, Naltrexone, chemistry.chemical_compound, Naltrindole, Opioid receptor, Internal medicine, Receptors, Opioid, delta, medicine, Animals, Rats, Wistar, Pain Measurement, Analgesics, Naloxone, Antagonist, Enkephalins, Receptor antagonist, Rats, Endocrinology, chemistry, Morphinans, Antagonism, Enkephalin, D-Penicillamine (2,5), Oligopeptides, medicine.drug, Enkephalin, Leucine, Research Article

Abstract

1. Antagonism, by the selective delta-opioid receptor antagonist naltrindole, of the antinociceptive effects of [D-Pen2, D-Pen5] enkephalin (DPDPE), [D-Ser2, Leu5, Thr6] enkephalin (DSLET) and D-Ala2 deltorphin I (DELT I) has been studied in 25 day old rats. 2. Antinociception was measured by the 50 degrees C tail immersion test following i.p. administration of agonists and/or antagonists. 3. Dose-related antinociception was observed with DPDPE, DSLET and DELT I and ED75 doses were computed (0.66 mg kg-1, 0.65 mg kg-1, 0.032 mg kg-1 respectively) and used for antagonism studies. 4. Naltrindole (0.01 mg kg-1) significantly attenuated the antinociceptive effects of DPDPE and DSLET with 0.1 mg kg-1 producing complete reversal of the effects of the ED75 dose. In contrast, naltrindole at 0.01 and 0.1 mg kg-1 did not alter antinociceptive responses to DELT I. Naltrindole at 1 mg kg-1 significantly attenuated DELT I antinociception. 5. Naloxone (1 mg kg-1) produced equivalent degrees of antagonism of the antinociceptive effects of DPDPE, DSLET and DELT I. ICI 174,864 (1 mg kg-1) also antagonized antinociception with a differential degree of attenuation (DSLET > DPDPE > DELT I). 6. Naltrindole (1 mg kg-1) had no effect on the antinociception induced by the selective mu-agonist alfentanil (60 micrograms kg-1). Naltrindole, naloxone or ICI 174,864 had no effect on nociceptive latencies. 7. The differential antagonism by naltrindole of the effects of three selective delta-agonists suggests delta-receptor heterogeneity.Further, the lower sensitivity of response to DELT I suggests that this agent may exert its antinociceptive effects at a different 6 receptor subtype from DPDPE or DSLET.

Published

1992

31. Manifestations of acute opiate withdrawal contracture in rabbit jejunum after mu-, kappa- and delta-receptor agonist exposure

Author

L.A. Morrone, L. Romanelli, and Pacifico Valeri

Subjects

Agonist, Atropine, Male, medicine.medical_specialty, Pyrrolidines, medicine.drug_class, Substance-Related Disorders, Receptors, Opioid, mu, (+)-Naloxone, Opioid, Hexamethonium Compounds, Tetrodotoxin, In Vitro Techniques, Hexamethonium, Hexamethonium compound, chemistry.chemical_compound, delta, Naltrindole, Internal medicine, Receptors, Opioid, delta, Receptors, medicine, 4-Dichloro-N-methyl-N-(2-(1-pyrrolidinyl)-cyclohexyl)-benzeneacetamide, pharmacology, Jejunum, drug effects, Male, Morphine, drug effects, Naloxone, pharmacology, Oligopeptides, delta, Receptors, kappa, Receptors, Animals, kappa, Morphine, Chemistry, Naloxone, Receptors, Opioid, kappa, 3,4-Dichloro-N-methyl-N-(2-(1-pyrrolidinyl)-cyclohexyl)-benzeneacetamide, (trans)-Isomer, Endocrinology, Jejunum, drug effects, Deltorphin, Receptors, Opioid, Rabbits, pharmacology, Norbinaltorphimine, Oligopeptides, medicine.drug, Muscle Contraction, Research Article

Abstract

1. Following a 5 min in vitro exposure to morphine (1.3 x 10(-7) M), U-50,488H (2.5 x 10(-8) M) and deltorphin (1.6 x 10(-8)-6.5 x 10(-9) M), the rabbit isolated jejunum exhibited a precipitated contracture after the addition of naloxone (2.75 x 10(-7) M). 2. The precipitated responses to U-50,488H and deltorphin but not to morphine were reproducible in the same tissue. 3. The precipitated contractures were blocked completely by tetrodotoxin (3 x 10(-7) M), partially by atropine (1.5 x 10(-7) M) and not affected by hexamethonium (1.4 x 10(-5) M). 4. Naloxone administration (2.75 x 10(-7) M) before the agonist prevented the development of the adaptive response to morphine and U-50,488H but not to deltorphin. 5. The selective antagonists norbinaltorphimine (2.7 x 10(-8)-2.7 x 10(-9) M) and naltrindole (1.1 x 10(-7) M) prevented the adaptive response development only to the respective agonists. 6. The opioid agonists partially inhibited the spontaneous activity of the tissue. This study has shown that independent activation of mu-, kappa- and delta-opioid receptors can induce dependence in this isolated tissue. Rabbit jejunum is a suitable tissue for studying the acute effects of opioids on the adaptative processes determined by their administration.

Published

1992