Your search keyword '"Receptors, Opioid agonists"' showing total 1,218 results

1. Advances in attenuating opioid-induced respiratory depression: A narrative review.

Author

Fan YZ, Duan YL, Chen CT, Wang Y, and Zhu AP

Subjects

Humans, Receptors, Opioid drug effects, Receptors, Opioid metabolism, Receptors, Opioid agonists, Narcotic Antagonists therapeutic use, Narcotic Antagonists pharmacology, Respiratory Insufficiency chemically induced, Respiratory Insufficiency drug therapy, Analgesics, Opioid adverse effects, Analgesics, Opioid therapeutic use

Abstract

Opioids exert analgesic effects by agonizing opioid receptors and activating signaling pathways coupled to receptors such as G-protein and/or β-arrestin. Concomitant respiratory depression (RD) is a common clinical problem, and improvement of RD is usually achieved with specific antagonists such as naloxone; however, naloxone antagonizes opioid analgesia and may produce more unknown adverse effects. In recent years, researchers have used various methods to isolate opioid receptor-mediated analgesia and RD, with the aim of preserving opioid analgesia while attenuating RD. At present, the focus is mainly on the development of new opioids with weak respiratory inhibition or the use of non-opioid drugs to stimulate breathing. This review reports recent advances in novel opioid agents, such as mixed opioid receptor agonists, peripheral selective opioid receptor agonists, opioid receptor splice variant agonists, biased opioid receptor agonists, and allosteric modulators of opioid receptors, as well as in non-opioid agents, such as AMPA receptor modulators, 5-hydroxytryptamine receptor agonists, phosphodiesterase-4 inhibitors, and nicotinic acetylcholine receptor agonists., Competing Interests: The authors have no conflicts of interest to disclose., (Copyright © 2024 the Author(s). Published by Wolters Kluwer Health, Inc.)

Published

2024

2. Buprenorphine: The Opioid that Cried 'Partial Agonist'.

Author

Bettinger JJ and Cleary J

Subjects

Humans, Drug Partial Agonism, Chronic Pain drug therapy, Animals, Receptors, Opioid agonists, Receptors, Opioid metabolism, Receptors, Opioid drug effects, Buprenorphine pharmacokinetics, Buprenorphine therapeutic use, Buprenorphine adverse effects, Analgesics, Opioid therapeutic use, Analgesics, Opioid adverse effects, Analgesics, Opioid pharmacokinetics

Abstract

Background: Although buprenorphine use has increased dramatically over the past decade, its unique pharmacologic and pharmacokinetic profile often leads to misconceptions about its overall utility and has created a drastic underrepresentation in patients with chronic non-can- cer pain. A common misnomer associated with buprenorphine is because of 'partial agonist' activity, it exhibits a plateauing of typical opioid-related side effects (including respiratory depression, constipation, euphoria, and hypogonadal axis suppression), but additionally it must exhibit a plateauing effect of overall analgesic potential. However, novel downstream molecular and cellular mechanisms offer new insights that help support the clinical potential that buprenorphine's analgesic actions may not have a ceiling, like its side effect profile. This interactive symposium will provide an enhanced review of the evolving research that helps unravel the complexity around buprenorphine's varying pharmacologic effects including actions on various opioid receptors, promiscuity to elicit varying actions on mu-opioid receptors coupled with different isoforms of G~ subunits, role in the intracellular recruitment of beta-arrestin, binding to different splice variants of mu-opioid receptors, and greater spinal versus supraspinal activity. The final half of this symposium will be designed to substantiate evidence with various human clinical trial data to further support buprenorphine's place on the analgesic ladder.

Published

2024

3. The nociceptin/orphanin FQ receptor partial agonist sunobinop promotes non-REM sleep in rodents and patients with insomnia.

Author

Whiteside GT, Kyle DJ, Kapil RP, Cipriano A, He E, Zhou M, Shet MS, Hummel M, Knappenberger T, Fukumura K, Matsuo Y, Uehira M, Hiroyama S, Takai N, Willsie SK, and Harris SC

Subjects

Animals, Humans, Receptors, Opioid agonists, Receptors, Opioid physiology, Opioid Peptides, Nociceptin Receptor, Rodentia, Sleep, Nociceptin, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

The potent and partial agonist sunobinop activates the nociceptin/orphanin-FQ peptide receptor and promotes non-REM sleep in rodents and patients with insomnia.

Published

2024

4. A dual nociceptin and mu opioid receptor agonist exhibited robust antinociceptive effect with decreased side effects.

Author

Hsu YT, Chen SR, Chang YC, Chang HF, Yeh TK, Chuang JY, Loh HH, Hsieh HP, Ueng SH, and Yeh SH

Subjects

Mice, Animals, Receptors, Opioid agonists, Nociceptin Receptor, Opioid Peptides pharmacology, Opioid Peptides therapeutic use, Analgesics, Opioid adverse effects, Pain chemically induced, Pain drug therapy, Analgesics adverse effects, Nociceptin, Receptors, Opioid, mu agonists, Drug-Related Side Effects and Adverse Reactions

Abstract

The compelling demand of a consummate analgesic medication without addiction is rising due to the clinical mistreatment. Additionally, the series of severe untoward effects usually deterred the utilization while coping with serious pain. As a possible turning point, we revealed that compound 14 is a dual agonist of mu opioid receptor (MOR) and nociceptin-orphanin FQ opioid peptide (NOP) receptor in this study. More importantly, compound 14 achieves pain relieving at very small doses, meanwhile, reduces several unwanted side effects such as constipation, reward, tolerance and withdrawal effects. Here, we evaluated the antinociception and side effects of this novel compound from wild type and humanized mice to further develop a safer prescription analgesic drug., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier Masson SAS. All rights reserved.)

Published

2023

5. Discovery and structure-activity relationships (SAR) of a novel class of 2-substituted N-piperidinyl indole-based nociceptin opioid receptor ligands.

Author

Meyer ME, Doshi A, Polgar WE, and Zaveri NT

Subjects

Ligands, Molecular Docking Simulation, Opioid Peptides, Nociceptin Receptor, Indoles pharmacology, Structure-Activity Relationship, Nociceptin, Analgesics, Opioid pharmacology, Receptors, Opioid agonists, Receptors, Opioid metabolism

Abstract

The development of SAR around substituted N-piperidinyl indole-based nociceptin opioid receptor (NOP) ligands led to the discovery of a novel series of 2-substituted N-piperidinyl indoles that provide both selective NOP full agonists and bifunctional NOP full agonists-μ opioid (MOP) receptor partial agonists. 2-substituted N-piperidinyl indoles have improved potency at the NOP receptor and are NOP full agonists, compared to our previously reported 3-substituted N-piperidinyl indoles that are selective NOP partial agonists. SAR in this series of 2-substituted N-piperidinyl indoles shows that 2-substitution versus 3-substitution on the indole moiety affects their intrinsic activity and opioid receptor selectivity. Molecular docking of these 2-substituted N-piperidinyl indoles in an active-state NOP homology model and MOP receptor structures provides a rationale for the differences observed in the binding, functional profiles and selectivity of 2-substituted versus 3-substituted N-piperidinyl indoles., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

6. Nociceptin Receptor-Related Agonists as Safe and Non-addictive Analgesics.

Author

Ding H, Kiguchi N, Dobbins M, Romero-Sandoval EA, Kishioka S, and Ko MC

Subjects

Animals, Humans, Nociceptin Receptor, Receptors, Opioid agonists, Pain drug therapy, Receptors, Opioid, mu agonists, Analgesics, Opioid adverse effects, Analgesics adverse effects, Drug-Related Side Effects and Adverse Reactions, Respiratory Insufficiency chemically induced, Respiratory Insufficiency drug therapy

Abstract

As clinical use of currently available opioid analgesics is often impeded by dose-limiting adverse effects, such as abuse liability and respiratory depression, new approaches have been pursued to develop safe, effective, and non-addictive pain medications. After the identification of the nociceptin/orphanin FQ (N/OFQ) peptide (NOP) receptor more than 25 years ago, NOP receptor-related agonists have emerged as a promising target for developing novel and effective opioids that modulate the analgesic and addictive properties of mu-opioid peptide (MOP) receptor agonists. In this review, we highlight the effects of the NOP receptor-related agonists compared with those of MOP receptor agonists in experimental rodent and more translational non-human primate (NHP) models and the development status of key NOP receptor-related agonists as potential safe and non-addictive analgesics. Several lines of evidence demonstrated that peptidic and non-peptidic NOP receptor agonists produce potent analgesic effects by intrathecal delivery in NHPs. Moreover, mixed NOP/MOP receptor partial agonists (e.g., BU08028, BU10038, and AT-121) display potent analgesic effects when administered intrathecally or systemically, without eliciting adverse effects, such as respiratory depression, itch behavior, and signs of abuse liability. More importantly, cebranopadol, a mixed NOP/opioid receptor agonist with full efficacy at NOP and MOP receptors, produces robust analgesic efficacy with reduced adverse effects, conferring promising outcomes in clinical studies. A balanced coactivation of NOP and MOP receptors is a strategy that warrants further exploration and refinement for the development of novel analgesics with a safer and effective profile., (© 2023. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2023

7. C(21)-fluorinated thevinol scaffold for opioid ligands. 21,21,21-Trifluoro-6-O-nororvinols: Design, synthesis and analgesic activity.

Author

Sandulenko IV, Belozertseva IV, Zvartau EE, Zelentsova MV, Ambartsumyan AA, Smol'yakov AF, and Moiseev SK

Subjects

Mice, Animals, Receptors, Opioid agonists, Narcotic Antagonists pharmacology, Structure-Activity Relationship, Ligands, Receptors, Opioid, mu agonists, Analgesics, Opioid pharmacology, Analgesics pharmacology

Abstract

Thevinols and their 3-O-demethylated relatives, orvinols, are derivatives of the Diels-Alder adduct of natural alkaloid thebaine with methyl vinyl ketone. Taken together, thevinols and orvinols constitute an important family of opioid receptor (OR) ligands playing an important role in both the OR mediated antinociception and OR antagonism. Herein, we disclose for the first time the OR activity of orvinols fluorinated within the pharmocophore associated with C(20) and its surrounding along with a dependence of the activity profile on the substituent at N(17). Starting from thevinone and 18,19-dihydrothevinone, a family of C(21)-fluorinated orvinols bearing methyl, cyclopropylmethyl (CPM), and allyl substituent at N(17) was synthesized. The fluorinated compounds were evaluated for OR activity. The orvinols bearing three fluorine atoms at C(21) were found to retain the properties of OR ligands and their activity profile depends on the substituent at N(17). Pilot in vivo experiments in a model of acute pain (tail-flick test in mice) revealed that 6-O-desmethyl-21,21,21-trifluoro-20-methylorvinol at doses 1.0-10.0 mg/kg (s.c.) exhibits analgesic activity at the level of morphine for a duration of 30-180 min. Its N(17)-CPM counterpart demonstrated the partial opioid agonist properties. The N(17)-allyl substituted derivative showed no analgesic activity. In vivo evaluation of an analgesic activity indicates that 21,21,21-trifluoro-20-methylorvinols represent a novel family of OR ligands related to buprenorphine, diprenorphine, etc. These compounds are promising for the structure-activity relationship studies among the thevinol/orvinol series as well as for a search for new OR ligands with potentially valuable pharmacological profiles., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier Masson SAS. All rights reserved.)

Published

2023

8. Synergistic interaction between DAMGO-NH 2 and NOP01 in peripherally acting antinociception in two mouse models of formalin pain.

Author

Li N, Xiao J, Niu J, Zhang M, Shi Y, Yu B, Zhang Q, Chen D, Zhang N, and Fang Q

Subjects

Animals, Mice, Analgesics pharmacology, Analgesics therapeutic use, Dose-Response Relationship, Drug, Enkephalin, Ala(2)-MePhe(4)-Gly(5)- pharmacology, Enkephalin, Ala(2)-MePhe(4)-Gly(5)- therapeutic use, Ligands, Nociceptin Receptor, Peptides therapeutic use, Receptors, Opioid, mu agonists, Drug Interactions, Analgesics, Opioid pharmacology, Analgesics, Opioid therapeutic use, Pain drug therapy, Receptors, Opioid agonists

Abstract

The most commonly used opioid analgesics are limited by their severe side-effects in the clinical treatment of pain. Preliminary reports indicate that the combination of classical opioids and N/OFQ receptor (NOP) ligands may be an effective strategy to reduce unwanted side-effects and improve antinociception. But the interaction of these two receptor ligands in pain regulation at the peripheral level remains unclear. In this study, the antinociception of a designed amide analogue of the mu opioid receptor (MOP) peptide agonist DAMGO, DAMGO-NH 2 , and its antinociceptive interaction with the peripherally limited NOP peptide agonist NOP01 was investigated in two mouse models of formalin pain. Our results showed that DAMGO-NH 2 acted as a MOP agonist in in vitro functional assays. Moreover, local subcutaneous or intraplantar injection of DAMGO-NH 2 exerted dose-related antinociception in both phases of the formalin orofacial and intraplantar pain, which could be mediated by the classical opioid receptor. Peripheral but not central pretreatment with the peripherally restricted opioid antagonist naloxone methiodide inhibited local DAMGO-NH 2 -induced antinociception, supporting the involvement of the peripheral opioid receptor in local DAMGO-NH 2 -induced antinociception. Furthermore, co-administration of the inactive doses of DAMGO-NH 2 and NOP01 produced effective antinociception. More importantly, isobolographic analysis indicates that the combination of DAMGO-NH 2 and NOP01 elicited supra-additive antinociception in these two models of formalin pain. In addition, the combination of DAMGO-NH 2 and NOP01 did not change motor function of mice in rotarod test. In conclusion, these data suggest that peripheral DAMGO-NH 2 and particularly its combination therapy with NOP01 may be effective for pain management., Competing Interests: Declarations of Competing Interest None., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

9. OCP002, a Mixed Agonist of Opioid and Cannabinoid Receptors, Produces Potent Antinociception With Minimized Side Effects.

Author

Xu B, Zhang Q, Chen D, Zhang M, Zhang R, Zhao W, Qiu Y, Xu K, Xiao J, Niu J, Shi Y, Li N, and Fang Q

Subjects

Animals, Mice, Analgesics, Opioid, Dose-Response Relationship, Drug, Receptors, Cannabinoid, Analgesics pharmacology, Cannabinoids, Receptors, Opioid agonists, Visceral Pain chemically induced, Visceral Pain drug therapy, Cannabinoid Receptor Agonists pharmacology

Abstract

Background: Increasing attention has been attracted to the development of bifunctional compounds to minimize the side effects of opioid analgesics. Pharmacological studies have verified the functional interaction between opioid and cannabinoid systems in pain management, suggesting that coactivation of the opioid and cannabinoid receptors may provide synergistic analgesia with fewer adverse reactions. Herein, we developed and characterized a novel bifunctional compound containing the pharmacophores of the mu-opioid receptor agonist DALDA and the cannabinoid peptide VD-Hpα-NH2, named OCP002., Methods: The opioid and cannabinoid agonistic activities of OCP002 were investigated in calcium mobilization and western blotting assays, respectively. Moreover, the central and peripheral antinociceptive effects of OCP002 were evaluated in mouse preclinical models of tail-flick test, carrageenan-induced inflammatory pain, and acetic acid-induced visceral pain, respectively. Furthermore, the potential opioid and cannabinoid side effects of OCP002 were systematically investigated in mice after intracerebroventricular (ICV) and subcutaneous (SC) administrations., Results: OCP002 functioned as a mixed agonist toward mu-opioid, kappa-opioid, and cannabinoid CB1 receptors in vitro. ICV and SC injections of OCP002 produced dose-dependent antinociception in mouse models of nociceptive (the median effective dose [ED50] values with 95% confidence interval [CI] are 0.14 [0.12-0.15] nmol and 0.32 [0.29-0.35] μmol/kg for ICV and SC injections, respectively), inflammatory (mechanical stimulation: ED50 values [95% CI] are 0.76 [0.64-0.90] nmol and 1.23 [1.10-1.38] μmol/kg for ICV and SC injections, respectively; thermal stimulation: ED50 values [95% CI] are 0.13 [0.10-0.17] nmol and 0.23 [0.08-0.40] μmol/kg for ICV and SC injections, respectively), and visceral pain (ED50 values [95% CI] are 0.0069 [0.0050-0.0092] nmol and 1.47 [1.13-1.86] μmol/kg for ICV and SC injections, respectively) via opioid and cannabinoid receptors. Encouragingly, OCP002 cannot cross the blood-brain barrier and exerted nontolerance-forming analgesia over 6-day treatment at both supraspinal and peripheral levels. Consistent with these behavioral results, repeated OCP002 administration did not elicit microglial hypertrophy and proliferation, the typical features of opioid-induced tolerance, in the spinal cord. Furthermore, at the effective analgesic doses, SC OCP002 exhibited minimized opioid and cannabinoid side effects on motor performance, body temperature, gastric motility, physical and psychological dependence, as well as sedation in mice., Conclusions: This study demonstrates that OCP002 produces potent and nontolerance-forming antinociception in mice with reduced opioid- and cannabinoid-related side effects, which strengthen the candidacy of bifunctional drugs targeting opioid/cannabinoid receptors for translational-medical development to replace or assist the traditional opioid analgesics., Competing Interests: The authors declare no conflicts of interest., (Copyright © 2022 International Anesthesia Research Society.)

Published

2023

10. Endometriosis and Opioid Receptors: Are Opioids a Possible/Promising Treatment for Endometriosis?

Author

Guan Q, Velho RV, Sehouli J, and Mechsner S

Subjects

Female, Humans, Analgesics, Opioid adverse effects, Pain drug therapy, Analgesics therapeutic use, Receptors, Opioid, mu agonists, Receptors, Opioid agonists, Endometriosis drug therapy

Abstract

Endometriosis (EM), defined as the presence of endometrial-like tissue with surrounding smooth muscle cells outside the uterus, is a disregarded gynecological disease reported to affect 6-10% of women of reproductive age, with 30-50% of them suffering from chronic pelvic pain and infertility. Since the exact pathogenic mechanisms of EM are still unclear, no curative therapy is available. As pain is an important factor in EM, optimal analgesia should be sought, which to date has been treated primarily with non-steroidal anti-inflammatory drugs (NSAIDs), metamizole or, in extreme cases, opioids. Here, we review the pain therapy options, the mechanisms of pain development in EM, the endogenous opioid system and pain, as well as the opioid receptors and EM-associated pain. We also explore the drug abuse and addiction to opioids and the possible use of NOP receptors in terms of analgesia and improved tolerability as a target for EM-associated pain treatment. Emerging evidence has shown a promising functional profile of bifunctional NOP/MOP partial agonists as safe and nonaddictive analgesics. However, until now, the role of NOP receptors in EM has not been investigated. This review offers a thought which still needs further investigation but may provide potential options for relieving EM-associated pain., Competing Interests: The authors declare no conflicts of interest.

Published

2023

11. Benzo[b]thiophene-2-carboxamides as novel opioid receptor agonists with potent analgesic effect and reduced constipation.

Author

Kuppusamy R, Hsu YT, Ke YY, Chang PW, Chang YC, Chang HF, Wang PC, Lin YH, Huang YC, Yeh TK, Chuang JY, Loh HH, Shih C, Chen CT, Yeh SH, and Ueng SH

Subjects

Humans, Receptors, Opioid, mu agonists, Receptors, Opioid agonists, Opioid Peptides, Morphine pharmacology, Analgesics pharmacology, Analgesics therapeutic use, Analgesics chemistry, Constipation chemically induced, Constipation drug therapy, Thiophenes pharmacology, Thiophenes therapeutic use, Analgesics, Opioid adverse effects

Abstract

Currently, there is a significant unmet need for novel analgesics with fewer side effects. In this study, we carried out structural modification of a hit compound previously identified in an artificial-intelligence (AI) virtual screening and discovered the potent analgesic, benzo[b]thiophene-2-carboxamide analog (compound 25) with new structural scaffold. We investigated the signaling pathways of opioid receptors mediated by compound 25, and found this racemic compound activated mu-opioid receptor through the cyclic adenosine monophosphate (cAMP) and β-arrestin-2-mediated pathways with strong potency and efficacy, and accompanying nociceptin-orphanin FQ opioid peptide and delta-opioid receptors through the cAMP pathway with weak potencies. Compound 25 elicited potent antinociception in thermal-stimulated pain (ED 50 value of 127.1 ± 34.65 μg/kg) and inflammatory-induced allodynia models with less gastrointestinal transit inhibition and antinociceptive tolerance than morphine. Overall, this study revealed a novel analgesic with reduced risks of side effects., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier Masson SAS. All rights reserved.)

Published

2022

12. Synthesis, Biological Activity and Molecular Docking of Chimeric Peptides Targeting Opioid and NOP Receptors.

Author

Wtorek K, Ghidini A, Gentilucci L, Adamska-Bartłomiejczyk A, Piekielna-Ciesielska J, Ruzza C, Sturaro C, Calò G, Pieretti S, Kluczyk A, McDonald J, Lambert DG, and Janecka A

Subjects

Animals, Mice, Receptors, Opioid, kappa, Narcotic Antagonists pharmacology, Receptors, Opioid, mu agonists, Molecular Docking Simulation, Ligands, Dose-Response Relationship, Drug, Naloxone, Analgesics pharmacology, Peptides pharmacology, Chimera, Peptides, Cyclic, Analgesics, Opioid therapeutic use, Receptors, Opioid agonists

Abstract

Recently, mixed opioid/NOP agonists came to the spotlight for their favorable functional profiles and promising outcomes in clinical trials as novel analgesics. This study reports on two novel chimeric peptides incorporating the fragment Tyr-c[D-Lys-Phe-Phe]Asp-NH 2 ( RP-170 ), a cyclic peptide with high affinity for µ and κ opioid receptors (or MOP and KOP, respectively), conjugated with the peptide Ac-RYYRIK-NH 2 , a known ligand of the nociceptin/orphanin FQ receptor (NOP), yielding RP-170-RYYRIK-NH 2 ( KW-495 ) and RP-170-Gly 3 -RYYRIK-NH 2 ( KW-496 ). In vitro, the chimeric KW-496 gained affinity for KOP, hence becoming a dual KOP/MOP agonist, while KW-495 behaved as a mixed MOP/NOP agonist with low nM affinity. Hence, KW-495 was selected for further in vivo experiments. Intrathecal administration of this peptide in mice elicited antinociceptive effects in the hot-plate test; this action was sensitive to both the universal opioid receptor antagonist naloxone and the selective NOP antagonist SB-612111. The rotarod test revealed that KW-495 administration did not alter the mice motor coordination performance. Computational studies have been conducted on the two chimeras to investigate the structural determinants at the basis of the experimental activities, including any role of the Gly 3 spacer.

Published

2022

13. OREX-1038: a potential new treatment for pain with low abuse liability and limited adverse effects.

Author

Gerak LR, Maguire DR, Cami-Kobeci G, Olson KM, Traynor JR, Husbands SM, France CP, Acevedo L, Belli B, and Flynn P

Subjects

Animals, Isoquinolines, Naltrexone analogs & derivatives, Phenylpropionates, Rats, Receptors, Opioid agonists, Receptors, Opioid, mu agonists, Analgesics, Opioid adverse effects, Pain drug therapy

Abstract

Drugs targeting mu opioid receptors are the mainstay of clinical practice for treating moderate-to-severe pain. While they can offer excellent analgesia, their use can be limited by adverse effects, including constipation, respiratory depression, tolerance, and abuse liability. Multifunctional ligands acting at mu opioid and nociceptin/orphanin FQ peptide receptors might provide antinociception with substantially improved adverse-effect profiles. This study explored one of these ligands, OREX-1038 (BU10038), in several assays in rodents and nonhuman primates. Binding and functional studies confirmed OREX-1038 to be a low-efficacy agonist at mu opioid and nociceptin/orphanin FQ peptide receptors and an antagonist at delta and kappa opioid receptors with selectivity for opioid receptors over other proteins. OREX-1038 had long-acting antinociceptive effects in postsurgical and complete Freund's adjuvant (CFA)-induced thermal hyperalgesia assays in rats and a warm water tail-withdrawal assay in monkeys. OREX-1038 was active for at least 24 h in each antinociception assay, and its effects in monkeys did not diminish over 22 days of daily administration. This activity was coupled with limited effects on physiological signs (arterial pressure, heart rate, and body temperature) and no evidence of withdrawal after administration of naltrexone or discontinuation of treatment in monkeys receiving OREX-1038 daily. Over a range of doses, OREX-1038 was only transiently self-administered, which diminished rapidly to nonsignificant levels; overall, both OREX-1038 and buprenorphine maintained less responding than remifentanil. These results support the concept of dual mu and nociceptin/orphanin FQ peptide receptor partial agonists having improved pharmacological profiles compared with opioids currently used to treat pain., (Copyright © 2022 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2022

14. Cannabinoid 1 and mu-Opioid Receptor Agonists Synergistically Inhibit Abdominal Pain and Lack Side Effects in Mice.

Author

Yu Y, Tsang QK, Jaramillo-Polanco J, Lomax AE, Vanner SJ, and Reed DE

Subjects

Analgesics pharmacology, Analgesics therapeutic use, Analgesics, Opioid pharmacology, Analgesics, Opioid therapeutic use, Animals, Female, Male, Mice, Mice, Inbred C57BL, Receptor, Cannabinoid, CB1, Abdominal Pain drug therapy, Cannabinoid Receptor Agonists pharmacology, Cannabinoid Receptor Agonists therapeutic use, Cannabinoids pharmacology, Cannabinoids therapeutic use, Receptors, Opioid agonists

Abstract

While effective in treating abdominal pain, opioids have significant side effects. Recent legalization of cannabis will likely promote use of cannabinoids as an adjunct or alternative to opioids, despite a lack of evidence. We aimed to investigate whether cannabinoids inhibit mouse colonic nociception, alone or in combination with opioids at low doses. Experiments were performed on C57BL/6 male and female mice. Visceral nociception was evaluated by measuring visceromotor responses (VMR), afferent nerve mechanosensitivity in flat-sheet colon preparations, and excitability of isolated DRG neurons. Blood oxygen saturation, locomotion, and defecation were measured to evaluate side effects. An agonist of cannabinoid 1 receptor (CB1R), arachidonyl-2'-chloroethylamide (ACEA), dose-dependently decreased VMR. ACEA and HU-210 (another CB1R agonist) also attenuated colonic afferent nerve mechanosensitivity. Additionally, HU-210 concentration-dependently decreased DRG neuron excitability, which was reversed by the CB1R antagonist AM-251. Conversely, cannabinoid 2 receptor (CB2R) agonists did not attenuate VMR, afferent nerve mechanosensitivity, or DRG neuron excitability. Combination of subanalgesic doses of CB1R and µ-opioid receptor agonists decreased VMR; importantly, this analgesic effect was preserved after 6 d of twice daily treatment. This combination also attenuated afferent nerve mechanosensitivity and DRG neuron excitability, which was inhibited by neuronal nitric oxide synthase and guanylate cyclase inhibitors. This combination avoided side effects (decreased oxygen saturation and colonic transit) caused by analgesic dose of morphine. Activation of CB1R, but not CB2R, decreased colonic nociception both alone and in synergy with µ-opioid receptor. Thus, CB1R agonists may enable opioid dose reduction and avoid opioid-related side effects. SIGNIFICANCE STATEMENT One of the most cited needs for patients with abdominal pain are safe and effective treatment options. The effectiveness of opioids in the management of abdominal pain is undermined by severe adverse side effects. Therefore, strategies to replace opioids or reduce the doses of opioids to suppress abdominal pain is needed. This study in mice demonstrates that cannabinoid 1 receptor (CB1R) agonists inhibit visceral sensation. Furthermore, a combination of subanalgesic doses of µ-opioid receptor agonist and CB1R agonist markedly reduce abdominal pain without causing the side effects of high-dose opioids. Thus, CB1R agonists, alone or in combination with low-dose opioids, may be a novel and safe treatment strategy for abdominal pain., (Copyright © 2022 the authors.)

Published

2022

15. PPL-138 (BU10038): A bifunctional NOP/mu partial agonist that reduces cocaine self-administration in rats.

Author

Cippitelli A, Martinez M, Zribi G, Cami-Kobeci G, Husbands SM, and Toll L

Subjects

Animals, Dose-Response Relationship, Drug, Female, Isoquinolines, Male, Naltrexone analogs & derivatives, Opioid Peptides, Phenylpropionates, Rats, Receptors, Opioid agonists, Receptors, Opioid, mu agonists, Self Administration, Nociceptin, Cocaine pharmacology

Abstract

The search for new and effective treatments for cocaine use disorder (CUD) is a priority. We determined whether PPL-138 (BU10038), a compound with partial agonist activity at both nociceptin opioid peptide (NOP) and mu-opioid receptors, reduces cocaine consumption, reinstatement, and whether the compound itself produces reinforcing effects in rats. Using an intermittent access (IntA) cocaine self-administration procedure, we found that PPL-138 (0.1 and 0.3 mg/kg) effectively decreased the total number of cocaine infusions and burst-like cocaine intake in both male and female rats. Responses for food in an IntA model of food self-administration were not altered for either sex, although locomotor activity was increased in female but not male rats. Blockade of NOP receptors with the selective antagonist J-113397 (5 mg/kg) did not prevent the PPL-138-induced suppression of cocaine self-administration, whereas blockade of mu-opioid receptors by naltrexone (1 mg/kg) reversed such effect. Consistently, treatment with morphine (1, 3, and 10 mg/kg) dose-dependently reduced IntA cocaine self-administration measures. PPL-138 also reduced reinstatement of cocaine seeking at all doses examined. Although an initial treatment with PPL-138 (2.5, 10, and 40 μg/kg/infusion) appeared rewarding, the compound did not maintain self-administration behavior. Animals treated with PPL-138 showed initial suppression of cocaine self-administration, which was eliminated following repeated daily dosing. However, suppression of cocaine self-administration was retained when subsequent PPL-138 treatments were administered 48 h apart. These findings demonstrate that the approach of combining partial NOP/mu-opioid activation successfully reduces cocaine use, but properties of PPL-138 seem to depend on the timing of drug administration., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

16. Endogenous opiates and behavior: 2020.

Author

Bodnar RJ

Subjects

Analgesics, Opioid pharmacology, Animals, Female, Learning physiology, Pain drug therapy, Pregnancy, Opioid Peptides pharmacology, Receptors, Opioid agonists

Abstract

This paper is the forty-third consecutive installment of the annual anthological review of research concerning the endogenous opioid system, summarizing articles published during 2020 that studied the behavioral effects of molecular, pharmacological and genetic manipulation of opioid peptides and receptors as well as effects of opioid/opiate agonists and antagonists. The review is subdivided into the following specific topics: molecular-biochemical effects and neurochemical localization studies of endogenous opioids and their receptors (1), the roles of these opioid peptides and receptors in pain and analgesia in animals (2) and humans (3), opioid-sensitive and opioid-insensitive effects of nonopioid analgesics (4), opioid peptide and receptor involvement in tolerance and dependence (5), stress and social status (6), learning and memory (7), eating and drinking (8), drug abuse and alcohol (9), sexual activity and hormones, pregnancy, development and endocrinology (10), mental illness and mood (11), seizures and neurologic disorders (12), electrical-related activity and neurophysiology (13), general activity and locomotion (14), gastrointestinal, renal and hepatic functions (15), cardiovascular responses (16), respiration and thermoregulation (17), and immunological responses (18)., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

17. NOP01, a NOP receptor agonist, produced potent and peripherally restricted antinociception in a formalin-induced mouse orofacial pain model.

Author

Xiao J, Niu J, Xu B, Zhang R, Zhang M, Zhang N, Xu K, Zhang Q, Chen D, Shi Y, Fang Q, and Li N

Subjects

Analgesics pharmacology, Animals, Disease Models, Animal, Facial Pain chemically induced, Formaldehyde, Mice, Pain Measurement, Nociceptin Receptor, Analgesics therapeutic use, Facial Pain drug therapy, Nociception drug effects, Receptors, Opioid agonists

Abstract

Orofacial pain is one of the most common medical challenges. A preliminary report indicates that the NOP receptor may act as a therapeutic target in orofacial pain. Previous studies have shown that [(pF)Phe 4 , Aib 7 , Aib 11 , Arg 14 , Lys 15 ]N/OFQ-NH 2 (NOP01) functions as a potent NOP receptor peptide agonist. This work aims to investigate the antinociception of NOP01 and its possible action mechanisms in a formalin-induced mouse orofacial pain model at different levels. Our results demonstrated that local, intraperitoneal (i.p.) or intrathecal (i.t.) injection of NOP01 produced dose-related antinociception in both phases of the formalin pain, which could be inhibited by the NOP receptor antagonist but not the classical opioid receptor antagonist. Furthermore, the antinociception induced by systemic NOP01 was blocked by local but not spinal pretreatment with the NOP receptor antagonist, suggesting the involvement of the peripheral NOP receptor in NOP01-induced systemic antinociception. Moreover, local injection of NOP01 markedly suppressed the expression of c-Fos protein induced by formalin in ipsilateral trigeminal ganglion (TG) neurons. In conclusion, this work suggests that NOP01 exerts significant antinociception on orofacial pain at both peripheral and spinal levels via the NOP receptor. Notably, NOP01 cannot readily penetrate the blood-brain barrier. Thus, NOP01 may behave as a potential compound for developing peripherally restricted analgesics., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

18. Opioid receptors modulate parallel fiber-Purkinje cell synaptic transmission in mouse cerebellum.

Author

Bai J, Ye T, Wei YB, Yang Y, Yang HM, and Lan Y

Subjects

Animals, Excitatory Postsynaptic Potentials, Glutamic Acid metabolism, Male, Mice, Purkinje Cells drug effects, Purkinje Cells physiology, Receptors, Opioid agonists, Purkinje Cells metabolism, Receptors, Opioid metabolism, Synaptic Transmission

Abstract

Opioid receptors play important roles in, among others, learning and memory, emotional responses, addiction, and pain. In recent years, the cerebellum has received increasing attention for its role in non-motor functions. The Purkinje cell (PC) is the only efferent neuron in the cerebellar cortex, and receives glutamatergic synaptic inputs from the parallel fibers (PF) formed by the axons of granule cells. Studies have shown that opioid receptors are expressed during the development of cerebellar cells. However, the distribution of opioid receptors, their subtypes in cerebellar PF-PC synapses, and their effects on synaptic transmission remain unclear. To examine these questions, we used whole-cell patch clamp recordings and pharmacological methods to determine the effects of activating three different opioid receptor subtypes on synaptic transmission at PF-PC synapses. In the presence of picrotoxin, mouse cerebellar slices were perfused with agonists or blockers of different opioid receptor subtypes, and the changes in excitatory postsynaptic currents (EPSCs) were examined. Both agonists of µ-opioid receptors (MOR) and δ-opioid receptors (DOR) significantly reduced the amplitude and area under the curve of PF-PC EPSCs in a concentration-dependent manner, accompanied by an increase in the paired-pulsed ratio (PPR). These effects could be blocked by respective receptor antagonists. In contrast, no significant changes were found after the application of κ-opioid receptor (KOR) agonists. In conclusion, MOR and DOR are present at the axon terminals of PF in the mouse cerebellar cortex, whereas no or negligible amounts of KOR are found. Activation of MOR and DOR regulates PF-PC synaptic transmission via inhibition of glutamate (Glu) release in cerebellar cortex in mice. We also found that endogenous opioid peptides are present in PF-PC synapses of mouse cerebellum, which also can inhibit the release of Glu., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2022

19. Effects of delta-opioid receptor agonist pretreatment on the cardiotoxicity of bupivacaine in rats.

Author

Wang C, Sun S, Jiao J, Yu X, and Huang S

Subjects

Animals, Disease Models, Animal, Dose-Response Relationship, Drug, Rats, Rats, Sprague-Dawley, Anesthetics, Local adverse effects, Benzamides pharmacology, Bupivacaine adverse effects, Cardiotoxicity prevention & control, Piperazines pharmacology, Receptors, Opioid agonists

Abstract

Background: Delta-opioid receptor is widely expressed in human and rodent hearts, and has been proved to protect cardiomyocytes against ischemia/reperfusion and heart failure. The antagonist of delta-opioid receptor could block the rescue effect of lipid emulsion against local anesthetic cardiotoxicity. However, no evidence is available for the direct effect of delta-opioid-receptor agonists on the cardiotoxicity of local anesthetics., Methods: Anesthetized Sprague Dawley rats were divided into five groups. Group NS received 2 ml·kg -1 ·min -1 normal saline, group LE received 2 ml·kg -1 ·min -1 30% lipid emulsion and group BW received 0.1, 1.0, or 5.0 mg/kg BW373U86, a delta-opioid-receptor agonist, for 5 min. Then 0.5% bupivacaine was infused intravenously at a rate of 3.0 mg·kg -1 ·min -1 until asystole. The time of arrhythmia, 50% mean arterial pressure-, 50% heart rate-reduction and asystole were recorded, and the dose of bupivacaine at each time point was calculated., Results: All three different doses of BW373U86 did not affect the arrhythmia, 50% mean arterial pressure-reduction, 50% heart rate-reduction and asystole dose of bupivacaine compared with group NS. 30% LE significantly increased the bupivacaine threshold of 50% mean arterial pressure-reduction (17.9 [15.4-20.7] versus 7.2 [5.9-8.7], p = 0.018), 50% heart rate-reduction (18.7 ± 4.2 versus 8.8 ± 1.7, p < 0.001) and asystole (26.5 [21.0-29.1] versus 11.3 [10.7-13.4], p = 0.008) compared with group NS. There was no difference between group LE and group NS in the arrhythmia dose of bupivacaine (9.9 [8.9-11.7] versus 5.6 [4.5-7.0], p = 0.060)., Conclusions: Our data show that BW373U86 does not affect the cardiotoxicity of bupivacaine compared with NS control in rats. 30% LE pretreatment protects the myocardium against bupivacaine-induced cardiotoxicity., (© 2022. The Author(s).)

Published

2022

20. Designer Benzodiazepines' Activity on Opioid Receptors: A Docking Study.

Author

Catalani V, Botha M, Corkery JM, Guirguis A, Vento A, and Schifano F

Subjects

Humans, Analgesics, Ligands, Receptors, Opioid, delta agonists, Receptors, Opioid, delta drug effects, Receptors, Opioid, delta metabolism, Receptors, Opioid, kappa agonists, Receptors, Opioid, kappa drug effects, Receptors, Opioid, kappa metabolism, Receptors, Opioid, mu agonists, Receptors, Opioid, mu drug effects, Receptors, Opioid, mu metabolism, Analgesics, Opioid adverse effects, Analgesics, Opioid chemistry, Analgesics, Opioid pharmacology, Anti-Anxiety Agents, Benzodiazepines adverse effects, Benzodiazepines chemistry, Benzodiazepines pharmacology, Receptors, Opioid agonists, Receptors, Opioid drug effects, Receptors, Opioid metabolism, Designer Drugs adverse effects, Designer Drugs chemistry, Designer Drugs pharmacology

Abstract

Background: Previous studies have reported that benzodiazepines (BZDs) seem to enhance euphoric and reinforcing properties of opioids in opioid users so that a direct effect on opioid receptors has been postulated, together with a possible synergistic induction of severe side effects due to co use of BDZs and opioids. This is particularly worrisome given the appearance on the market of designer benzodiazepines (DBZDs), whose activity/toxicity profiles are scarcely known., Objectives: This study aimed to evaluate, through computational studies, the binding affinity (or lack thereof) of 101 DBZDs identified online on the kappa, mu, and delta opioid receptors (K, M, DOR); and to assess whether their mechanism of action could include activation of the latter., Methods: MOE® was used for the computational studies. Pharmacophore mapping based on strong opioids agonist binders' 3D chemical features was used to filter the DBZDs. Resultant DBZDs were docked into the crystallised 3D active conformation of KOR (PDB6B73), DOR (PDB6PT3) and MOR (PDB5C1M). Co-crystallised ligands and four strong agonists were used as reference compounds. A score (S, Kcal/mol) representative of the predicted binding affinity, and a description of ligand interactions were obtained from MOE®., Results: The docking results, filtered for S < -8.0 and the interaction with the Asp residue, identified five DBZDs as putative binders of the three ORs : ciclotizolam, fluloprazolam, JQ1, Ro 48-6791, and Ro 48-8684., Conclusion: It may be inferred that at least some DBZDs may have the potential to activate opioid receptors. This could mediate/increase their anxiolytic, analgesic, and addiction potentials, as well as worsen the side effects associated with opioid co-use., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2022

21. Central Nervous System Distribution of an Opioid Agonist Combination with Synergistic Activity.

Author

Griffith JI, Kim M, Bruce DJ, Peterson CD, Kitto KF, Mohammad AS, Rathi S, Fairbanks CA, Wilcox GL, and Elmquist WF

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, ATP Binding Cassette Transporter, Subfamily G, Member 2 genetics, Animals, Drug Combinations, Drug Synergism, Female, Genotype, Loperamide administration & dosage, Male, Mice, Mice, Inbred ICR, Morpholines administration & dosage, Tissue Distribution, Central Nervous System metabolism, Loperamide pharmacokinetics, Morpholines pharmacokinetics, Receptors, Opioid agonists

Abstract

Novel combinations of specific opioid agonists like loperamide and oxymorphindole targeting the µ - and δ -opioid receptors, respectively, have shown increased potency with minimized opioid-associated risks. However, whether their interaction is pharmacokinetic or pharmacodynamic in nature has not been determined. This study quantitatively determined whether these drugs have a pharmacokinetic interaction that alters systemic disposition or central nervous system (CNS) distribution. We performed intravenous and oral in vivo pharmacokinetic assessments of both drugs after discrete dosing and administration in combination to determine whether the combination had any effect on systemic pharmacokinetic parameters or CNS exposure. Drugs were administered at 5 or 10 mg/kg i.v. or 30 mg/kg orally to institute for cancer research (ICR) mice and 5 mg/kg i.v. to Friend leukemia virus strain B mice of the following genotypes: wild-type, breast cancer resistance protein ( Bcrp -/- ) (Bcrp knockout), Mdr1a/b -/- [P-glycoprotein (P-gp) knockout], and Bcrp -/- Mdr1a/b -/- (triple knockout). In the combination, clearance of oxymorphindole (OMI) was reduced by approximately half, and the plasma area under the concentration-time curve (AUC) increased. Consequently, brain and spinal cord AUCs for OMI in the combination also increased proportionately. Both loperamide and OMI are P-gp substrates, but administration of the two drugs in combination does not alter efflux transport at the CNS barriers. Because OMI alone shows appreciable brain penetration but little therapeutic efficacy on its own, and because loperamide's CNS distribution is unchanged in the combination, the mechanism of action for the increased potency of the combination is most likely pharmacodynamic and most likely occurs at receptors in the peripheral nervous system. This combination has favorable characteristics for future development. SIGNIFICANCE STATEMENT: Opioids have yet to be replaced as the most effective treatments for moderate-to-severe pain and chronic pain, but their side effects are dangerous. Combinations of opioids with peripheral activity, such as loperamide and oxymorphindole, would be valuable in that they are effective at much lower doses and have reduced risks for dangerous side effects because the µ -opioid receptor agonist is largely excluded from the CNS., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2022

22. Cardiovascular and renal effects of novel nonpeptide nociceptin opioid peptide receptor agonists.

Author

Denys IB, Gao J, Sutphen JC, Zaveri NT, and Kapusta DR

Subjects

Animals, Hyperphagia, Hypertension drug therapy, Hypertension metabolism, Ligands, Rats, Rats, Sprague-Dawley, Nociceptin Receptor, Analgesics, Opioid pharmacology, Receptors, Opioid agonists

Abstract

Background and Purpose: Partial agonists of the nociceptin opioid peptide (NOP) receptor have potential therapeutic use as antihypertensive and water diuretics (aquaretics). To date, peptide NOP receptor ligands have failed to progress in clinical trials due to poor pharmacokinetics and adverse effects. Nonpeptide, small-molecule NOP receptor ligands may be more suitable as therapeutic agents. This study investigated the cardiovascular and renal responses produced by the novel nonpeptide NOP agonists AT-403, AT-090, AT-127, and AT-039., Experimental Approach: Changes in mean arterial pressure (MAP), heart rate (HR), renal excretory function and occurrence of sedation and hyperphagia were determined before and after i.v. bolus injection or infusion of the NOP agonists in conscious Sprague-Dawley rats. Additional studies involving (i) measurement of renal sympathetic nerve activity (RSNA) and (ii) renal denervation were conducted to investigate the role of the renal nerves in the cardiorenal responses to AT-039., Key Results: Bolus i.v. injection of AT-403, AT-090, AT-127 and AT-039 produced significant decreases in MAP and HR and a sodium-sparing diuresis. AT-403, AT-090, and AT-127, but not AT-039, induced sedation and hyperphagia at all doses tested. Infusion i.v. of AT-039 produced hypotension and aquaresis without adverse central nervous system effects or change in HR, responses that were also observed in renal denervated rats., Conclusions and Implications: Nonpeptide NOP agonists decrease blood pressure and produce aquaresis in conscious rodents. Due to lack of sedation and hyperphagia, AT-039 represents a novel NOP agonist that may be useful for treatment of hypertension and/or volume overload/hyponatraemic states., (© 2021 The British Pharmacological Society.)

Published

2022

23. Involvement of the nociceptin opioid peptide receptor in morphine-induced antinociception, tolerance and physical dependence in female mice.

Author

Hao XQ, Wang ZY, Chen JM, Wu N, and Li J

Subjects

Animals, Dose-Response Relationship, Drug, Female, Mice, Opioid Peptides pharmacology, Prospective Studies, Receptors, Opioid agonists, Nociceptin, Analgesics, Opioid pharmacology, Morphine pharmacology

Abstract

Nociceptin opioid peptide (NOP) receptor modulates pain transmission and is considered a prospective target for pain management. Under acute pain conditions in rodents, however, no definitive conclusions about effects of systemically intervening NOP receptors on nociception, classical opioid-induced antinociception, tolerance and physical dependence have been drawn. Given that opioid analgesia has sex differences, and females experience greater pain and consume more opioids, clarifying these issues in females will help develop novel analgesics. To clarify the role of NOP receptors on the pharmacological profiles of µ-opioid receptor agonists, in this study, a selective agonist (SCH221510) and antagonist (SB612111) of the NOP receptor were subcutaneously administered in female mice in multiple animal models. In hot-plate test, neither SCH221510 (3 and 10 mg/kg, sc) nor SB612111 (10 mg/kg, sc) produced significant antinociception. SCH221510 (3 mg/kg, sc) attenuated but SB612111 (10 mg/kg, sc) enhanced morphine-induced antinociception, with rightward and leftward shift of morphine dose-response curves, respectively. SCH221510 (3 mg/kg, sc) combined with morphine (10 mg/kg, sc) accelerated the development of morphine antinociceptive tolerance. Conversely, SB612111 (10 mg/kg, sc) delayed morphine tolerance development. Neither SCH221510 (3 mg/kg, sc) nor SB612111 (10 mg/kg, sc) statistically significantly altered the development of morphine-induced physical dependence. Therefore, systemic activation of NOP receptors attenuated morphine antinociception to acute thermal stimuli, facilitated morphine-induced antinociceptive tolerance but did not robustly alter physical dependence in female mice. Systemic blockade of NOP receptors produced opposite actions. These findings demonstrate that N/OFQ-NOP receptor system plays diverse roles in modulating pharmacological profiles of µ-opioid receptor agonists., (© 2021. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2021

24. Characterization of the Synergistic Effect between Ligands of Opioid and Free Fatty Acid Receptors in the Mouse Model of Colitis.

Author

Binienda A, Makaro A, Talar M, Krajewska JB, Tarasiuk A, Bartoszek A, Fabisiak A, Mosińska P, Niewinna K, Dziedziczak K, Świerczyński M, Kordek R, Salaga M, and Fichna J

Subjects

Aniline Compounds administration & dosage, Animals, Butyrates administration & dosage, Colitis immunology, Disease Models, Animal, Drug Synergism, Enkephalin, Ala(2)-MePhe(4)-Gly(5)- administration & dosage, Enkephalin, D-Penicillamine (2,5)- administration & dosage, Inflammation drug therapy, Inflammation metabolism, Ligands, Male, Mice, Mice, Inbred BALB C, Naloxone administration & dosage, Narcotic Antagonists administration & dosage, Peroxidase metabolism, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled antagonists & inhibitors, Receptors, Opioid agonists, Receptors, Opioid, delta agonists, Receptors, Opioid, delta metabolism, Receptors, Opioid, mu agonists, Receptors, Opioid, mu metabolism, Sulfonamides administration & dosage, Thiophenes administration & dosage, Xanthenes administration & dosage, Colitis drug therapy, Colitis metabolism, Receptors, G-Protein-Coupled metabolism, Receptors, Opioid metabolism

Abstract

Background: Recent studies suggest that lipids, including free fatty acids (FFAs), are necessary for proper μ opioid receptor (MOR) binding and that activation of opioid receptors (ORs) improves intestinal inflammation. The objective of the study was to investigate a possible interaction between the ORs and FFA receptors (FFARs) ligands in the colitis., Methods: The potential synergistic effect of ORs and FFARs ligands was evaluated using mouse model of acute colitis induced by dextran sulfate sodium (DSS, 4%). Compounds were injected intraperitoneally (i.p.) once or twice daily at the doses of 0.01 or 0.02 mg/kg body weight (BW) (DAMGO-an MOR agonist), 0.3 mg/kg BW (DPDPE-a δ OR (DOR) agonist) and 1 mg/kg BW (naloxone-a non-selective OR antagonist, GLPG 0974-a FFAR2 antagonist, GSK 137647-a FFAR4 agonist and AH 7614-a FFAR4 antagonist) for 4 days., Results: Myeloperoxidase (MPO) activity was significantly decreased after DAMGO (0.02 mg/kg BW) and GSK 137647 (1 mg/kg BW) administration and co-administration as compared to DSS group., Conclusions: Treatment with ligands of ORs and FFARs may affect the immune cells in the inflammation; however, no significant influence on the severity of colitis and no synergistic effect were observed.

Published

2021

25. Glutamate Buffering Capacity and Blood-Brain Barrier Protection of Opioid Receptor Agonists Biphalin and Nociceptin.

Author

Nozohouri S, Zhang Y, Albekairi TH, Vaidya B, and Abbruscato TJ

Subjects

Analgesics pharmacology, Animals, Animals, Newborn, Capillary Permeability drug effects, Capillary Permeability physiology, Coculture Techniques, Dose-Response Relationship, Drug, Mice, Neuroprotective Agents pharmacology, Receptors, Opioid agonists, Receptors, Opioid metabolism, Nociceptin, Analgesics, Opioid pharmacology, Blood-Brain Barrier drug effects, Blood-Brain Barrier metabolism, Enkephalins pharmacology, Glutamic Acid metabolism, Opioid Peptides pharmacology

Abstract

Opioids play crucial roles in the regulation of many important brain functions including pain, memory, and neurogenesis. Activation of opioid receptors is reported to have neuroprotective effects after ischemic reperfusion injury. The objective of this study was to understand the role of biphalin and nociceptin, opioid receptor agonists, on blood-brain barrier (BBB) integrity during ischemic stroke. In this study, we aimed to measure the effect of biphalin and nociceptin on astrocytic glutamate uptake and on expression of excitatory amino acid transporter to study the indirect role of astrocytes on opioid receptor-mediated BBB protection during in vitro stroke conditions. We used mouse brain endothelial cells (bEnd.3) and primary astrocytes as an in vitro BBB model. Restrictive BBB properties were evaluated by measuring [ 14 C] sucrose paracellular permeability and the redistribution of the tight junction proteins. The protective effect of biphalin and nociceptin on BBB integrity was assessed after exposing cells to oxygen glucose deprivation (OGD) and glutamate. It was observed that combined stress (2 mM glutamate and 2 hours of OGD) significantly reduced glutamate uptake by astrocytes; however, biphalin and nociceptin treatment increased glutamate uptake in primary astrocytes. This suggests a role of increased astrocytic buffering capacity in opioid-meditated protection of the BBB during ischemic stroke. It was also found that the combined stress significantly increased [ 14 C] sucrose paracellular permeability in an in vitro BBB model. Biphalin and nociceptin treatment attenuated the effect of the combined stress, which was reversed by the opioid receptor antagonists, suggesting the role of opioid receptors in biphalin and nociception's BBB modulatory activity. SIGNIFICANT STATEMENT: There is an unmet need for discovering new efficacious therapeutic agents to offset the deleterious effects of ischemic stroke. Given the confirmed roles of opioid receptors in the regulation of central nervous system functions, opioid receptor agonists have been studied as potential neuroprotective options in ischemic conditions. This study adds to the knowledge about the cerebrovascular protective effects of opioid receptor agonists and provides insight about the mechanism of action of these agents., (Copyright ©2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2021

26. Shedding Light on the Pharmacological Interactions between μ-Opioid Analgesics and Angiotensin Receptor Modulators: A New Option for Treating Chronic Pain.

Author

Király K, Karádi DÁ, Zádor F, Mohammadzadeh A, Galambos AR, Balogh M, Riba P, Tábi T, Zádori ZS, Szökő É, Fürst S, and Al-Khrasani M

Subjects

Analgesics pharmacology, Analgesics, Opioid pharmacology, Animals, Humans, Neuralgia drug therapy, Nociception drug effects, Pain Management methods, Proto-Oncogene Mas, Receptors, Angiotensin metabolism, Receptors, Opioid agonists, Receptors, Opioid, mu agonists, Receptors, Opioid, mu metabolism, Chronic Pain drug therapy, Receptors, Angiotensin drug effects, Receptors, Opioid, mu drug effects

Abstract

The current protocols for neuropathic pain management include µ-opioid receptor (MOR) analgesics alongside other drugs; however, there is debate on the effectiveness of opioids. Nevertheless, dose escalation is required to maintain their analgesia, which, in turn, contributes to a further increase in opioid side effects. Finding novel approaches to effectively control chronic pain, particularly neuropathic pain, is a great challenge clinically. Literature data related to pain transmission reveal that angiotensin and its receptors (the AT1R, AT2R, and MAS receptors) could affect the nociception both in the periphery and CNS. The MOR and angiotensin receptors or drugs interacting with these receptors have been independently investigated in relation to analgesia. However, the interaction between the MOR and angiotensin receptors has not been excessively studied in chronic pain, particularly neuropathy. This review aims to shed light on existing literature information in relation to the analgesic action of AT1R and AT2R or MASR ligands in neuropathic pain conditions. Finally, based on literature data, we can hypothesize that combining MOR agonists with AT1R or AT2R antagonists might improve analgesia.

Published

2021

27. Optimization binding studies of opioid receptors, saturation and competition, using [ 3 H]-DAMGO.

Author

Khoramjouy M, Ahmadi F, Faizi M, and Shahhosseini S

Subjects

Animals, Codeine, Gene Expression Regulation drug effects, Male, Protein Binding, Rats, Rats, Sprague-Dawley, Receptors, Opioid metabolism, Analgesics, Opioid pharmacology, Enkephalin, Ala(2)-MePhe(4)-Gly(5)- pharmacology, Receptors, Opioid agonists, Tritium

Abstract

Background: Opioid analgesics are prescribed for the moderate to severe pain in the clinic. New analogs of µ-opioid receptors are introduced because they may have less adverse effects and better efficacy. However, these new analogs have to be screened for their receptor affinity before entering clinical trial phases. A common method to do such screening is using radioligand-binding-assay, which is a fast and precise screening technique if the assays are done at an optimum condition. One of the main challenges in this type of screening is to separate free/unbound radioligands from bound radioligands. In this study, we applied a centrifugation method instead of a filtration method to separate free radioligands from bound radioligands, and also optimized the conditions for radioligand receptor binding studies of µ-opioid receptors, saturation, and the competition., Methods: We used the midbrain and brainstem of naltrexone-treated rats as a source of µ-opioid receptors, and [ 3 H]-DAMGO as the radioligand. Naloxone was also used to determine non-specific binding. A given amount of membrane protein was incubated with an increasing amount of radioligand at 37 °C to saturate the receptors at equilibrium and the amount of radioligand saturated in the receptors were used in competition studies., Results: 160 µg membrane protein saturated with 20 nM [ 3 H]-DAMGO at 37 °C for 35 min with K d (15.06 nM, 95% CI 8.117-22.00) and B max (0.4750 pmol/mg, 95% CI 0.3839-0.5660)., Conclusion: Applying the centrifugation method instead of the filtration to separate free from bound radioligand produced repeatable and reliable results. The optimum conditions for radioligand binding were used in competition studies which resulted in the expected outcomes., (© 2021. Maj Institute of Pharmacology Polish Academy of Sciences.)

Published

2021

28. Functional Profile of Systemic and Intrathecal Cebranopadol in Nonhuman Primates.

Author

Ding H, Trapella C, Kiguchi N, Hsu FC, Caló G, and Ko MC

Subjects

Analgesics, Opioid administration & dosage, Animals, Dose-Response Relationship, Drug, Female, Fentanyl administration & dosage, Injections, Spinal, Macaca mulatta, Male, Opioid Peptides administration & dosage, Receptors, Opioid physiology, Receptors, Opioid, mu agonists, Receptors, Opioid, mu physiology, Nociceptin Receptor, Nociceptin, Indoles administration & dosage, Pain Measurement drug effects, Pain Measurement methods, Receptors, Opioid agonists, Spiro Compounds administration & dosage

Abstract

Background: Cebranopadol, a mixed nociceptin/opioid receptor full agonist, can effectively relieve pain in rodents and humans. However, it is unclear to what degree different opioid receptor subtypes contribute to its antinociception and whether cebranopadol lacks acute opioid-associated side effects in primates. The authors hypothesized that coactivation of nociceptin receptors and μ receptors produces analgesia with reduced side effects in nonhuman primates., Methods: The antinociceptive, reinforcing, respiratory-depressant, and pruritic effects of cebranopadol in adult rhesus monkeys (n = 22) were compared with μ receptor agonists fentanyl and morphine using assays, including acute thermal nociception, IV drug self-administration, telemetric measurement of respiratory function, and itch-scratching responses., Results: Subcutaneous cebranopadol (ED50, 2.9 [95% CI, 1.8 to 4.6] μg/kg) potently produced antinociception compared to fentanyl (15.8 [14.6 to 17.1] μg/kg). Pretreatment with antagonists selective for nociceptin and μ receptors, but not δ and κ receptor antagonists, caused rightward shifts of the antinociceptive dose-response curve of cebranopadol with dose ratios of 2 and 9, respectively. Cebranopadol produced reinforcing effects comparable to fentanyl, but with decreased reinforcing strength, i.e., cebranopadol (mean ± SD, 7 ± 3 injections) versus fentanyl (12 ± 3 injections) determined by a progressive-ratio schedule of reinforcement. Unlike fentanyl (8 ± 2 breaths/min), systemic cebranopadol at higher doses did not decrease the respiratory rate (17 ± 2 breaths/min). Intrathecal cebranopadol (1 μg) exerted full antinociception with minimal scratching responses (231 ± 137 scratches) in contrast to intrathecal morphine (30 μg; 3,009 ± 1,474 scratches)., Conclusions: In nonhuman primates, the μ receptor mainly contributed to cebranopadol-induced antinociception. Similar to nociceptin/μ receptor partial agonists, cebranopadol displayed reduced side effects, such as a lack of respiratory depression and pruritus. Although cebranopadol showed reduced reinforcing strength, its detectable reinforcing effects and strength warrant caution, which is critical for the development and clinical use of cebranopadol., (Copyright © 2021, the American Society of Anesthesiologists. All Rights Reserved.)

Published

2021

29. The Buprenorphine Analogue BU10119 Attenuates Drug-Primed and Stress-Induced Cocaine Reinstatement in Mice.

Author

Hillhouse TM, Olson KM, Hallahan JE, Rysztak LG, Sears BF, Meurice C, Ostovar M, Koppenhaver PO, West JL, Jutkiewicz EM, Husbands SM, and Traynor JR

Subjects

Animals, Mice, Male, Stress, Psychological drug therapy, Stress, Psychological metabolism, Cocaine-Related Disorders drug therapy, Mice, Inbred C57BL, Receptors, Opioid, mu agonists, Receptors, Opioid, mu metabolism, Drug-Seeking Behavior drug effects, Humans, Receptors, Opioid metabolism, Receptors, Opioid agonists, Narcotic Antagonists pharmacology, Receptors, Opioid, kappa agonists, Receptors, Opioid, kappa metabolism, Buprenorphine pharmacology, Buprenorphine analogs & derivatives, Cocaine pharmacology

Abstract

There are no Food and Drug Administration-approved medications for cocaine use disorder, including relapse. The μ -opioid receptor (MOPr) partial agonist buprenorphine alone or in combination with naltrexone has been shown to reduce cocaine-positive urine tests and cocaine seeking in rodents. However, there are concerns over the abuse liability of buprenorphine. Buprenorphine's partial agonist and antagonist activity at the nociception receptor (NOPr) and κ -opioid receptor (KOPr), respectively, may contribute to its ability to inhibit cocaine seeking. Thus, we hypothesized that a buprenorphine derivative that exhibits antagonist activity at MOPr and KOPr with enhanced agonist activity at the NOPr could provide a more effective treatment. Here we compare the pharmacology of buprenorphine and two analogs, BU10119 and BU12004, in assays for antinociception and for cocaine- and stress-primed reinstatement in the conditioned place preference paradigm. In vitro and in vivo assays showed that BU10119 acts as an antagonist at MOPr, KOPr, and δ -opioid receptor (DOPr) and a partial agonist at NOPr, whereas BU12004 showed MOPr partial agonist activity and DOPr, KOPr, and NOPr antagonism. BU10119 and buprenorphine but not BU12004 lessened cocaine-primed reinstatement. In contrast, BU10119, BU12004, and buprenorphine blocked stress-primed reinstatement. The selective NOPr agonist SCH221510 but not naloxone decreased cocaine-primed reinstatement. Together, these findings are consistent with the concept that NOPr agonism contributes to the ability of BU10119 and buprenorphine to attenuate reinstatement of cocaine-conditioned place preference in mice. The findings support the development of buprenorphine analogs lacking MOPr agonism with increased NOPr agonism for relapse prevention to cocaine addiction. SIGNIFICANCE STATEMENT: There are no Food and Drug Administration-approved medications for cocaine use disorder. Buprenorphine has shown promise as a treatment for cocaine relapse prevention; however, there are concerns over the abuse liability of buprenorphine. Here we show a buprenorphine analogue, BU10119, which lacks μ -opioid receptor agonism and inhibits cocaine-primed and stress-primed reinstatement in a conditioned place-preference paradigm. The results suggest the development of BU10119 for the management of relapse to cocaine seeking., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2021

30. Novel treatments for chronic pain: moving beyond opioids.

Author

O'Brien JB and Roman DL

Subjects

Adenylyl Cyclase Inhibitors therapeutic use, Adenylyl Cyclases physiology, Analgesics, Non-Narcotic therapeutic use, Analgesics, Opioid adverse effects, Analgesics, Opioid classification, Analgesics, Opioid therapeutic use, Animals, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Anticonvulsants therapeutic use, Antidepressive Agents therapeutic use, Chronic Pain etiology, Chronic Pain physiopathology, Drug Discovery, Humans, Opioid Epidemic, Opioid-Related Disorders, Receptors, Opioid agonists, Translational Research, Biomedical, Chronic Pain drug therapy

Abstract

It is essential that safe and effective treatment options be available to patients suffering from chronic pain. The emergence of an opioid epidemic has shaped public opinions and created stigmas surrounding the use of opioids for the management of pain. This reality, coupled with high risk of adverse effects from chronic opioid use, has led chronic pain patients and their healthcare providers to utilize nonopioid treatment approaches. In this review, we will explore a number of cellular reorganizations that are associated with the development and progression of chronic pain. We will also discuss the safety and efficacy of opioid and nonopioid treatment options for chronic pain. Finally, we will review the evidence for adenylyl cyclase type 1 (AC1) as a novel target for the treatment of chronic pain., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

31. Influence of G protein-biased agonists of μ-opioid receptor on addiction-related behaviors.

Author

Kudla L and Przewlocki R

Subjects

Animals, Humans, Signal Transduction drug effects, Analgesics, Opioid pharmacology, GTP-Binding Proteins metabolism, Receptors, Opioid agonists, Receptors, Opioid metabolism, Substance-Related Disorders metabolism

Abstract

Opioid analgesics remain a gold standard for the treatment of moderate to severe pain. However, their clinical utility is seriously limited by a range of adverse effects. Among them, their high-addictive potential appears as very important, especially in the context of the opioid epidemic. Therefore, the development of safer opioid analgesics with low abuse potential appears as a challenging problem for opioid research. Among the last few decades, different approaches to the discovery of novel opioid drugs have been assessed. One of the most promising is the development of G protein-biased opioid agonists, which can activate only selected intracellular signaling pathways. To date, discoveries of several biased agonists acting via μ-opioid receptor were reported. According to the experimental data, such ligands may be devoid of at least some of the opioid side effects, such as respiratory depression or constipation. Nevertheless, most data regarding the addictive properties of biased μ-opioid receptor agonists are inconsistent. A global problem connected with opioid abuse also requires the search for effective pharmacotherapy for opioid addiction, which is another potential application of biased compounds. This review discusses the state-of-the-art on addictive properties of G protein-biased μ-opioid receptor agonists as well as we analyze whether these compounds can diminish any symptoms of opioid addiction. Finally, we provide a critical view on recent data connected with biased signaling and its implications to in vivo manifestations of addiction., (© 2021. The Author(s).)

Published

2021

32. Clinical Pharmacology, Toxicity, and Abuse Potential of Opioids.

Author

Vearrier D and Grundmann O

Subjects

Analgesics, Opioid pharmacology, Analgesics, Opioid toxicity, Dose-Response Relationship, Drug, Drug Overdose epidemiology, Half-Life, Humans, Illicit Drugs pharmacology, Illicit Drugs toxicity, Narcotics pharmacokinetics, Narcotics toxicity, Prescription Drug Misuse adverse effects, Receptors, Opioid agonists, Narcotic-Related Disorders physiopathology, Narcotics pharmacology

Abstract

Opioids were the most common drug class resulting in overdose deaths in the United States in 2019. Widespread clinical use of prescription opioids for moderate to severe pain contributed to the ongoing opioid epidemic with the subsequent emergence of fentanyl-laced heroin. More potent analogues of fentanyl and structurally diverse opioid receptor agonists such as AH-7921 and MT-45 are fueling an increasingly diverse illicit opioid supply. Overdose from synthetic opioids with high binding affinities may not respond to a typical naloxone dose, thereby rendering autoinjectors less effective, requiring higher antagonist doses or resulting in a confusing clinical picture for health care providers. Nonscheduled opioid drugs such as loperamide and dextromethorphan are associated with dependence and risk of overdose as easier access makes them attractive to opioid users. Despite a common opioid-mediated pathway, several opioids present with unique pharmacodynamic properties leading to acute toxicity and dependence development. Pharmacokinetic considerations involve half-life of the parent opioid and its metabolites as well as resulting toxicity, as is established for tramadol, codeine, and oxycodone. Pharmacokinetic considerations, toxicities, and treatment approaches for notable opioids are reviewed., (© 2021, The American College of Clinical Pharmacology.)

Published

2021

33. Endogenous opiates and behavior: 2019.

Author

Bodnar RJ

Subjects

Analgesics, Opioid pharmacology, Animals, Cancer Pain drug therapy, Cancer Pain genetics, Chronic Pain drug therapy, Ethanol pharmacology, Female, Humans, Memory drug effects, Memory physiology, Pain, Postoperative drug therapy, Pregnancy, Receptors, Opioid agonists, Sexual Behavior physiology, Social Status, Substance-Related Disorders genetics, Opioid Peptides pharmacology, Opioid Peptides physiology, Receptors, Opioid physiology, Stress, Psychological physiopathology, Substance-Related Disorders etiology

Abstract

This paper is the forty-second consecutive installment of the annual anthological review of research concerning the endogenous opioid system, summarizing articles published during 2019 that studied the behavioral effects of molecular, pharmacological and genetic manipulation of opioid peptides and receptors as well as effects of opioid/opiate agonists and antagonists. The review is subdivided into the following specific topics: molecular-biochemical effects and neurochemical localization studies of endogenous opioids and their receptors (1), the roles of these opioid peptides and receptors in pain and analgesia in animals (2) and humans (3), opioid-sensitive and opioid-insensitive effects of nonopioid analgesics (4), opioid peptide and receptor involvement in tolerance and dependence (5), stress and social status (6), learning and memory (7), eating and drinking (8), drug abuse and alcohol (9), sexual activity and hormones, pregnancy, development and endocrinology (10), mental illness and mood (11), seizures and neurologic disorders (12), electrical-related activity and neurophysiology (13), general activity and locomotion (14), gastrointestinal, renal and hepatic functions (15), cardiovascular responses (16), respiration and thermoregulation (17), and immunological responses (18)., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

34. Regulation of Opioid Receptors by Their Endogenous Opioid Peptides.

Author

Gupta A, Gullapalli S, Pan H, Ramos-Ortolaza DL, Hayward MD, Low MJ, Pintar JE, Devi LA, and Gomes I

Subjects

Analgesics, Opioid pharmacology, Animals, Brain drug effects, Enkephalin, Ala(2)-MePhe(4)-Gly(5)- metabolism, Enkephalin, Ala(2)-MePhe(4)-Gly(5)- pharmacology, Female, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Opioid Peptides pharmacology, Analgesics, Opioid metabolism, Brain metabolism, Opioid Peptides metabolism, Receptors, Opioid agonists, Receptors, Opioid metabolism

Abstract

Activation of μ, δ, and κ opioid receptors by endogenous opioid peptides leads to the regulation of many emotional and physiological responses. The three major endogenous opioid peptides, β-endorphin, enkephalins, and dynorphins result from the processing of three main precursors: proopiomelanocortin, proenkephalin, and prodynorphin. Using a knockout approach, we sought to determine whether the absence of endogenous opioid peptides would affect the expression or activity of opioid receptors in mice lacking either proenkephalin, β-endorphin, or both. Since gene knockout can lead to changes in the levels of peptides generated from related precursors by compensatory mechanisms, we directly measured the levels of Leu-enkephalin and dynorphin-derived peptides in the brain of animals lacking proenkephalin, β-endorphin, or both. We find that whereas the levels of dynorphin-derived peptides were relatively unaltered, the levels of Leu-enkephalin were substantially decreased compared to wild-type mice suggesting that preproenkephalin is the major source of Leu-enkephalin. This data also suggests that the lack of β-endorphin and/or proenkephalin does not lead to a compensatory change in prodynorphin processing. Next, we examined the effect of loss of the endogenous peptides on the regulation of opioid receptor levels and activity in specific regions of the brain. We also compared the receptor levels and activity in males and females and show that the lack of β-endorphin and/or proenkephalin leads to differential modulation of the three opioid receptors in a region- and gender-specific manner. These results suggest that endogenous opioid peptides are important modulators of the expression and activity of opioid receptors in the brain.

Published

2021

35. Opioid Receptor Regulation of Neuronal Voltage-Gated Calcium Channels.

Author

Weiss N and Zamponi GW

Subjects

Analgesics, Opioid pharmacology, Animals, Calcium Channel Agonists pharmacology, Calcium Channel Blockers pharmacology, Calcium Signaling drug effects, Humans, Neurons drug effects, Receptors, Opioid agonists, Calcium Channels physiology, Calcium Signaling physiology, Neurons physiology, Receptors, Opioid physiology

Abstract

Neuronal voltage-gated calcium channels play a pivotal role in the conversion of electrical signals into calcium entry into nerve endings that is required for the release of neurotransmitters. They are under the control of a number of cellular signaling pathways that serve to fine tune synaptic activities, including G-protein coupled receptors (GPCRs) and the opioid system. Besides modulating channel activity via activation of second messengers, GPCRs also physically associate with calcium channels to regulate their function and expression at the plasma membrane. In this mini review, we discuss the mechanisms by which calcium channels are regulated by classical opioid and nociceptin receptors. We highlight the importance of this regulation in the control of neuronal functions and their implication in the development of disease conditions. Finally, we present recent literature concerning the use of novel μ-opioid receptor/nociceptin receptor modulators and discuss their use as potential drug candidates for the treatment of pain.

Published

2021

36. Interactive Mechanisms of Supraspinal Sites of Opioid Analgesic Action: A Festschrift to Dr. Gavril W. Pasternak.

Author

Rossi GC and Bodnar RJ

Subjects

Analgesics, Opioid pharmacology, Analgesics, Opioid therapeutic use, Animals, Brain drug effects, Humans, Morphine metabolism, Morphine pharmacology, Morphine therapeutic use, Narcotic Antagonists metabolism, Narcotic Antagonists pharmacology, Receptors, Opioid agonists, Spinal Cord drug effects, Spinal Cord metabolism, Analgesia methods, Analgesics, Opioid metabolism, Brain metabolism, Pain drug therapy, Pain metabolism, Receptors, Opioid metabolism

Abstract

Almost a half century of research has elaborated the discoveries of the central mechanisms governing the analgesic responses of opiates, including their receptors, endogenous peptides, genes and their putative spinal and supraspinal sites of action. One of the central tenets of "gate-control theories of pain" was the activation of descending supraspinal sites by opiate drugs and opioid peptides thereby controlling further noxious input. This review in the Special Issue dedicated to the research of Dr. Gavril Pasternak indicates his contributions to the understanding of supraspinal mediation of opioid analgesic action within the context of the large body of work over this period. This review will examine (a) the relevant supraspinal sites mediating opioid analgesia, (b) the opioid receptor subtypes and opioid peptides involved, (c) supraspinal site analgesic interactions and their underlying neurophysiology, (d) molecular (particularly AS) tools identifying opioid receptor actions, and (e) relevant physiological variables affecting site-specific opioid analgesia. This review will build on classic initial studies, specify the contributions that Gavril Pasternak and his colleagues did in this specific area, and follow through with studies up to the present.

Published

2021

37. Differential In Vitro Pharmacological Profiles of Structurally Diverse Nociceptin Receptor Agonists in Activating G Protein and Beta-Arrestin Signaling at the Human Nociceptin Opioid Receptor.

Author

Lu JJ, Polgar WE, Mann A, Dasgupta P, Schulz S, and Zaveri NT

Subjects

Animals, Cell Line, Gene Expression Regulation drug effects, Humans, Ligands, Molecular Structure, Phosphorylation, Signal Transduction drug effects, Small Molecule Libraries chemistry, Nociceptin Receptor, GTP-Binding Proteins metabolism, Receptors, Opioid agonists, Small Molecule Libraries pharmacology, beta-Arrestins metabolism

Abstract

Agonists at the nociceptin opioid peptide receptor (NOP) are under investigation as therapeutics for nonaddicting analgesia, opioid use disorder, Parkinson's disease, and other indications. NOP full and partial agonists have both been of interest, particularly since NOP partial agonists show a reduced propensity for behavioral disruption than NOP full agonists. Here, we investigated the in vitro pharmacological properties of chemically diverse NOP receptor agonists in assays measuring functional activation of the NOP receptor such as guanosine 5'-O-[gamma-thio]triphosphate (GTP γ S) binding, cAMP inhibition, G protein-coupled inwardly rectifying potassium (GIRK) channel activation, phosphorylation, β-arrestin recruitment and receptor internalization. When normalized to the efficacy of the natural agonist nociceptin/orphanin FQ (N/OFQ), we found that different functional assays that measure intrinsic activity produce inconsistent levels of agonist efficacy, particularly for ligands that were partial agonists. Agonist efficacy obtained in the GTP γ S assay tended to be lower than that in the cAMP and GIRK assays. These structurally diverse NOP agonists also showed differential receptor phosphorylation profiles at the phosphosites we examined and induced varying levels of receptor internalization. Interestingly, although the rank order for β-arrestin recruitment by these NOP agonists was consistent with their ability to induce receptor internalization, their phosphorylation signatures at the time point we investigated were not indicative of the levels of β-arrestin recruitment or internalization induced by these agonists. It is possible that other phosphorylation sites, yet to be identified, drive the recruitment of NOP receptor ensembles and subsequent receptor trafficking by some nonpeptide NOP agonists. These findings potentially help understand NOP agonist pharmacology in the context of ligand-activated receptor trafficking. SIGNIFICANCE STATEMENT: Chemically diverse agonist ligands at the nociceptin opioid receptor G protein-coupled receptor showed differential efficacy for activating downstream events after receptor binding, in a suite of functional assays measuring guanosine 5'-O-[gamma-thio]triphosphate binding, cAMP inhibition, G protein-coupled inwardly rectifying protein channel activation, β-arrestin recruitment, receptor internalization and receptor phosphorylation. These analyses provide a context for understanding nociceptin opioid peptide receptor (NOP) agonist pharmacology driven by ligand-induced differential NOP receptor signaling., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2021

38. Novel Mixed NOP/Opioid Receptor Peptide Agonists.

Author

Pacifico S, Albanese V, Illuminati D, Marzola E, Fabbri M, Ferrari F, Holanda VAD, Sturaro C, Malfacini D, Ruzza C, Trapella C, Preti D, Lo Cascio E, Arcovito A, Della Longa S, Marangoni M, Fattori D, Nassini R, Calò G, and Guerrini R

Subjects

Animals, Binding Sites, Cough chemically induced, Cough drug therapy, Disease Models, Animal, Guinea Pigs, Humans, Hydrophobic and Hydrophilic Interactions, Male, Molecular Dynamics Simulation, Peptides metabolism, Peptides therapeutic use, Receptors, Opioid metabolism, Receptors, Opioid, mu genetics, Receptors, Opioid, mu metabolism, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Structure-Activity Relationship, Nociceptin Receptor, Peptides chemistry, Receptors, Opioid agonists, Receptors, Opioid, mu agonists

Abstract

The nociceptin/orphanin FQ (N/OFQ)/N/OFQ receptor (NOP) system controls different biological functions including pain and cough reflex. Mixed NOP/opioid receptor agonists elicit similar effects to strong opioids but with reduced side effects. In this work, 31 peptides with the general sequence [Tyr/Dmt 1 ,Xaa 5 ]N/OFQ(1-13)-NH 2 were synthesized and pharmacologically characterized for their action at human recombinant NOP/opioid receptors. The best results in terms of NOP versus mu opioid receptor potency were obtained by substituting both Tyr 1 and Thr 5 at the N-terminal portion of N/OFQ(1-13)-NH 2 with the noncanonical amino acid Dmt. [Dmt 1,5 ]N/OFQ(1-13)-NH 2 has been identified as the most potent dual NOP/mu receptor peptide agonist so far described. Experimental data have been complemented by in silico studies to shed light on the molecular mechanisms by which the peptide binds the active form of the mu receptor. Finally, the compound exerted antitussive effects in an in vivo model of cough.

Published

2021

39. Novel Approaches, Drug Candidates, and Targets in Pain Drug Discovery.

Author

Obeng S, Hiranita T, León F, McMahon LR, and McCurdy CR

Subjects

Adrenergic Agonists therapeutic use, Analgesics pharmacology, Analgesics therapeutic use, Animals, Epoxide Hydrolases antagonists & inhibitors, Epoxide Hydrolases metabolism, Humans, Pain drug therapy, Receptors, Opioid agonists, Receptors, Opioid metabolism, Signal Transduction drug effects, Voltage-Gated Sodium Channels chemistry, Voltage-Gated Sodium Channels metabolism, Analgesics chemistry, Drug Discovery, Receptors, Opioid chemistry

Abstract

Because of the problems associated with opioids, drug discovery efforts have been employed to develop opioids with reduced side effects using approaches such as biased opioid agonism, multifunctional opioids, and allosteric modulation of opioid receptors. Receptor targets such as adrenergic, cannabinoid, P2X3 and P2X7, NMDA, serotonin, and sigma, as well as ion channels like the voltage-gated sodium channels Nav1.7 and Nav1.8 have been targeted to develop novel analgesics. Several enzymes, such as soluble epoxide hydrolase, sepiapterin reductase, and MAGL/FAAH, have also been targeted to develop novel analgesics. In this review, old and recent targets involved in pain signaling and compounds acting at these targets are summarized. In addition, strategies employed to reduce side effects, increase potency, and efficacy of opioids are also elaborated. This review should aid in propelling drug discovery efforts to discover novel analgesics.

Published

2021

40. Structure-Based SAR in the Design of Selective or Bifunctional Nociceptin (NOP) Receptor Agonists.

Author

Meyer ME, Doshi A, Yasuda D, and Zaveri NT

Subjects

Binding Sites, Ligands, Molecular Docking Simulation, Molecular Structure, Receptors, Opioid metabolism, Receptors, Opioid ultrastructure, Receptors, Opioid, mu metabolism, Receptors, Opioid, mu ultrastructure, Sequence Homology, Amino Acid, Structure-Activity Relationship, Nociceptin Receptor, Drug Design, Receptors, Opioid agonists, Receptors, Opioid, mu agonists

Abstract

The nociceptin opioid receptor (NOP), the fourth member of the opioid receptor family, and its endogenous peptide ligand, nociceptin or orphanin FQ (N/OFQ), play a vital role in several central nervous system pathways regulating pain, reward, feeding, anxiety, motor control and learning/memory. Both selective NOP agonists as well as bifunctional agonists at the NOP and mu opioid receptor (MOP) have potential therapeutic applications in CNS disorders related to these processes. Using Surflex-Dock protocols, we conducted a computational structure-activity study of four scaffold classes of NOP ligands with varying NOP-MOP selectivity. By docking these compounds into the orthosteric binding sites within an active-state NOP homology model, and an active-state MOP crystal structure, the goal of this study was to use a structure-based drug design approach to modulate NOP affinity and NOP vs. MOP selectivity. We first docked four parent compounds (no side chain) to determine their binding interactions within the NOP and MOP binding pockets. Various polar sidechains were added to the heterocyclic A-pharmacophore to modulate NOP ligand affinity. The substitutions mainly contained a 1-2 carbon chain with a polar substituent such as an amine, alcohol, sulfamide, or guanidine. The SAR analysis is focused on the impact of structural changes in the sidechain, such as chain length, hydrogen bonding capability, and basic vs neutral functional groups on binding affinity and selectivity at both NOP and MOP receptors. This study highlights structural modifications that can be leveraged to rationally design both selective NOP and bifunctional NOP-MOP agonists with different ratios of functional efficacy.

Published

2021

41. Recent Advances in Peripheral Opioid Receptor Therapeutics.

Author

Seth R, Kuppalli SS, Nadav D, Chen G, and Gulati A

Subjects

Analgesics adverse effects, Analgesics therapeutic use, Analgesics, Opioid adverse effects, Analgesics, Opioid therapeutic use, Chronic Pain drug therapy, Humans, Receptors, Opioid agonists, Receptors, Opioid therapeutic use

Abstract

Purpose of Review: Although opioids are excellent analgesics, they are associated with severe short- and long-term side effects that are especially concerning for the treatment of chronic pain. Peripherally acting opioid receptor agonists promise to mitigate the more serious centrally mediated side effects of opioids, and the goal of this paper is to identify and elaborate on recent advances in these peripheral opioid receptor therapeutics., Recent Findings: Peripheral opioid receptor agonists are effective analgesics that at the same time circumvent the problem of centrally mediated opioid side effects by (1) preferentially targeting peripheral opioid receptors that are often the source of the pain and (2) their markedly diminished permeability or activity across the blood-brain barrier. Recent novel bottom-up approaches have been notable for the design of therapeutics that are either active only at inflamed tissue, as in the case of fentanyl-derived pH-sensitive opioid ligands, or too bulky or hydrophilic to cross the blood-brain barrier, as in the case of morphine covalently bound to hyperbranched polyglycerols. Recent innovations in peripheral opioid receptor therapeutics of pH-sensitive opioid ligands and limiting opioid permeability across the blood-brain barrier have had promising results in animal models. While this is grounds for optimism that some of these therapeutics will be efficacious in human subjects at a future date, each drug must undergo individualized testing for specific chronic pain syndromes to establish not only the nuances of each drug's therapeutic effect but also a comprehensive safety profile.

Published

2021

42. Label-free cell phenotypic study of opioid receptors and discovery of novel mu opioid ligands from natural products.

Author

Hou T, Xu F, Peng X, Zhou H, Zhang X, Qiu M, Wang J, Liu Y, and Liang X

Subjects

Biological Products chemistry, Biosensing Techniques methods, Drug Discovery methods, Drug Evaluation, Preclinical methods, HEK293 Cells, Humans, Ligands, Receptors, Opioid agonists, Receptors, Opioid genetics, Structure-Activity Relationship, Biological Products pharmacology, Narcotic Antagonists pharmacology, Receptors, Opioid metabolism, Receptors, Opioid, mu agonists, Receptors, Opioid, mu antagonists & inhibitors

Abstract

Ethnopharmacological Relevance: Mu opioid receptor (MOR) is mainly a drug target for analgesia. Opioid-like agonists such as morphine have been clinically used for analgesia but have potential adverse effects. MOR antagonists have been demonstrated to alleviate these side effects. Plants (Carthamus tinctorius L, Cynanchum otophyllum C. K. Schneid., Coffea arabica L., Prinsepia utilis Royle and Lepidium meyenii Walp.) and Ganoderma fungi (Ganoderma hainanense J. D. Zhao, Ganoderma capense (Lloyd) Teng, Ganoderma cochlear (Blume et Nees) Bres., Ganoderma resinaceum Boud and Ganoderma applanatum (Pers.) Pat.) are traditional medicines with beneficial effects on immunoregulation, analgesia and the nervous system, but whether MORs are engaged in their effects remains unknown., Aim of the Study: This work aimed to identify MOR ligands among compounds isolated from the above-mentioned 10 species, and to investigate selectivity against four opioid receptor subtypes. By analyzing the structure-activity relationship and off-target effects, we could provide a new direction for the future development of MOR drugs., Materials and Methods: Four opioid receptor subtype models, including MOR, delta (DOR), kappa (KOR) and nop (NOR), were established with a label-free phenotypic dynamic mass redistribution assay to systematically profile the pharmacological properties of known ligands. Then, 82 natural compounds derived from the 10 species were screened against MOR to identify new ligands. The selectivity of the new ligands was characterized against the four subtypes, and off-target effects were also investigated on eight G protein-coupled receptors (GPCRs)., Results: The pharmacological properties of known ligands on transfected HEK293T-MOR, HEK293-DOR, HEK293-KOR and HEK293-NOR cell lines were characterized. Seven compounds purified from Ganoderma cochlear (Blume et Nees) Bres. and Carthamus tinctorius L were MOR antagonists with micromolar potency. Among them, compound 35 showed the strongest antagonistic activity on MOR with an IC 50 value of 10.0 ± 3.0 μM. To a certain extent, these seven new antagonists, exhibited antagonistic activity on the other opioid receptor subtypes, and they had almost no effect on other GPCRs, including CB1, CB2, M2 and beta2AR. Additionally, a compound from Lepidium meyenii Walp. displayed MOR agonistic activity., Conclusions: The established screening models opened new avenues for the discovery and evaluation of opioid receptor ligand selectivity. Together, the novel MOR antagonists and agonists will enrich the inventory of MOR ligands and benefit related therapies., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

43. Effect of opioid receptors of the cuneiform nucleus on cardiovascular responses in normotensive and hypotensive hemorrhagic rats.

Author

Mohebbati R, KhajaviRad A, Hosseini M, and Shafei MN

Subjects

Analgesics, Opioid administration & dosage, Animals, Blood Pressure drug effects, Heart Rate drug effects, Hemorrhage chemically induced, Hypotension chemically induced, Male, Microinjections methods, Midbrain Reticular Formation drug effects, Morphine administration & dosage, Naloxone administration & dosage, Narcotic Antagonists administration & dosage, Rats, Rats, Wistar, Receptors, Opioid agonists, Blood Pressure physiology, Heart Rate physiology, Hemorrhage physiopathology, Hypotension physiopathology, Midbrain Reticular Formation physiology, Receptors, Opioid physiology

Abstract

The presence of opioid receptors in the cuneiform nucleus (CnF), which is a mesencephalic area, and their involvement in the central cardiovascular responses have been shown. Therefore, this study is designed to examine the possible role of mu- (μ) and delta- (δ) opioid receptors in the CnF in the cardiovascular responses in normotensive and hemorrhagic hypotensive rats. Following anesthesia and the recording of the blood pressure, the agonist and antagonist of μ- (morphine and naloxone) and δ- (D-Pen 2, 5]-Enkephalin hydrate (DPDPE) and naltridole) receptors were microinjected into the CnF. In the hemorrhagic groups, the drugs were microinjected into the nucleus 2 min after withdrawing 15 % of the total blood volume (TBV). Time-course changes (Δ) in the mean arterial pressure (MAP), systolic blood pressure (SBP), and heart rate (HR) were obtained and compared with the control and hemorrhage groups. Microinjecting morphine in both normotensive and hemorrhagic rats significantly decreased ΔSBP, ΔMAP, and ΔHR; also, naloxone significantly increased all these parameters. The cardiovascular effects of DPDPE and naltridole were not significant in the normotensive rats; however, DPDPE attenuated only the tachycardia induced by the hypotensive hemorrhage. The findings of this study revealed that the opioid receptors in the CnF had an inhibitory effect on the cardiovascular parameters in both normotensive and hypotensive hemorrhagic conditions and these effects were mostly mediated by μ-opioid receptors., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

44. Intraoperative opioids are associated with improved recurrence-free survival in triple-negative breast cancer.

Author

Montagna G, Gupta HV, Hannum M, Tan KS, Lee J, Scarpa JR, Plitas G, Irie T, McCormick PJ, Fischer GW, Morrow M, and Mincer JS

Subjects

Analgesics, Opioid adverse effects, Databases, Factual, Dose-Response Relationship, Drug, Drug Administration Schedule, Female, Humans, Middle Aged, Neoplasm Recurrence, Local mortality, Receptors, Opioid genetics, Retrospective Studies, Time Factors, Treatment Outcome, Triple Negative Breast Neoplasms genetics, Triple Negative Breast Neoplasms mortality, Tumor Microenvironment, Analgesics, Opioid administration & dosage, Intraoperative Care adverse effects, Intraoperative Care mortality, Mastectomy adverse effects, Mastectomy mortality, Neoplasm Recurrence, Local prevention & control, Receptors, Opioid agonists, Triple Negative Breast Neoplasms surgery

Abstract

Background: Opioid-induced immunomodulation may be of particular importance in triple-negative breast cancer (TNBC) where an immune response is associated with improved outcome and response to immunotherapy. We evaluated the association between intraoperative opioids and oncological outcomes and explored patterns of opioid receptor expression in TNBC., Methods: Consecutive patients with stage I-III primary TNBC were identified from a prospectively maintained database. Opioid receptor expression patterns in the tumour microenvironment were analysed using publicly available bulk and single-cell RNA-seq data., Results: A total of 1143 TNBC cases were retrospectively analysed. In multivariable analysis, higher intraoperative opioid dose was associated with favourable recurrence-free survival, hazard ratio 0.93 (95% confidence interval 0.88-0.99) per 10 oral morphine milligram equivalents increase (P=0.028), but was not significantly associated with overall survival, hazard ratio 0.96 (95% confidence interval 0.89-1.02) per 10 morphine milligram equivalents increase (P=0.2). Bulk RNA-seq analysis of opioid receptors showed that OPRM1 was nearly non-expressed. Compared with normal breast tissue OGFR, OPRK1, and OPRD1 were upregulated, while TLR4 was downregulated. At a single-cell level, OPRM1 and OPRD1 were not detectable; OPRK1 was expressed mainly on tumour cells, whereas OGFR and TLR4 were more highly expressed on immune cells., Conclusions: We found a protective effect of intraoperative opioids on recurrence-free survival in TNBC. Opioid receptor expression was consistent with a net protective effect of opioid agonism, with protumour receptors either not expressed or downregulated, and antitumour receptors upregulated. In this era of personalised medicine, efforts to differentiate the effects of opioids across breast cancer subtypes (and ultimately individual patients) should continue., (Copyright © 2020 British Journal of Anaesthesia. Published by Elsevier Ltd. All rights reserved.)

Published

2021

45. Potential of Nociceptin/Orphanin FQ Peptide Analogs for Drug Development.

Author

Wtorek K and Janecka A

Subjects

Amino Acid Sequence, Humans, Ligands, Narcotic Antagonists chemistry, Narcotic Antagonists metabolism, Opioid Peptides metabolism, Receptors, Opioid agonists, Receptors, Opioid chemistry, Structure-Activity Relationship, Nociceptin Receptor, Nociceptin, Drug Discovery, Opioid Peptides chemistry, Receptors, Opioid metabolism

Abstract

Nociceptin receptor (NOP) belongs to the family of opioid receptors but was discovered and characterized much later than the so called classical opioid receptors, μ, δ and κ (or MOP, DOP and KOP, resp.). Nociceptin/orphanin FQ (N/OFQ) is the endogenous ligand of this receptor and it controls numerous important functions in the central nervous system and in the periphery, so its analogs may be developed as innovative drugs for the treatment of a variety of conditions and pathological states. Availability of potent and selective ligands with high affinity to NOP receptor is essential to fully understand the role of NOP-N/OFQ system in the body, which in turn may lead to designing novel therapeutics. Here, we have focused on reviewing the structure of potent peptide-based agonists, antagonists, biased analogs and bivalent ligands that target NOP receptor., (© 2020 Wiley-VHCA AG, Zurich, Switzerland.)

Published

2021

46. The kappa-opioid receptor agonist, nalfurafine, blocks acquisition of oxycodone self-administration and oxycodone's conditioned rewarding effects in male rats.

Author

Zamarripa CA, Patel TR, Williams BC, Pareek T, Schrock HM, Prisinzano TE, and Freeman KB

Subjects

Analgesics, Opioid pharmacology, Animals, Conditioning, Classical drug effects, Dose-Response Relationship, Drug, Male, Morphinans metabolism, Opioid-Related Disorders prevention & control, Oxycodone adverse effects, Oxycodone pharmacology, Rats, Rats, Sprague-Dawley, Receptors, Opioid agonists, Receptors, Opioid metabolism, Receptors, Opioid, kappa metabolism, Reinforcement, Psychology, Reward, Self Administration, Spiro Compounds metabolism, Substance-Related Disorders drug therapy, Substance-Related Disorders prevention & control, Morphinans pharmacology, Opioid-Related Disorders drug therapy, Receptors, Opioid, kappa agonists, Spiro Compounds pharmacology

Abstract

Mu-opioid receptor (MOR) agonists are highly efficacious for the treatment of pain but have significant abuse liability. Recently, we reported that nalfurafine, when combined with oxycodone at a certain ratio, reduced the reinforcing effects of oxycodone in rats while producing additive antinociceptive effects. Questions remain, however, including if the combination will function as a reinforcer in drug-naïve rats, and if the combination produces aversive effects that could explain nalfurafine's ability to reduce oxycodone self-administration? In the present study, we investigated nalfurafine's ability to reduce acquisition of oxycodone self-administration when the two were self-administered as a mixture in drug-naïve rats and nalfurafine's ability to attenuate a conditioned place preference (CPP) induced by oxycodone. In the self-administration study, male Sprague-Dawley rats self-administered intravenous injections of oxycodone (0.056 mg/kg/injection), an oxycodone/nalfurafine combination (0.056/0.0032 mg/kg/injection), or saline under fixed-ratio schedules of reinforcement for 20 days to compare rates of acquisition of drug taking. In the CPP assay, male Sprague-Dawley rats received subcutaneous injections of either saline, oxycodone (3.2 mg/kg), nalfurafine (0.18 mg/kg), or an oxycodone/nalfurafine combination at the same ratio used in the self-administration study (3.2 mg/kg/0.18 mg/kg). All subjects self-administering oxycodone alone met acquisition criteria. However, only 13% of subjects self-administering oxycodone/nalfurafine met criteria, and no subjects acquired self-administration of saline. Oxycodone, but not nalfurafine alone or the oxycodone/nalfurafine combination, produced rewarding effects in rats in the CPP test. These findings suggest that the combination of oxycodone and nalfurafine will be less habit forming in opioid-naïve patients than oxycodone alone.

Published

2020

47. The Role of Opioids and Their Receptors in Urological Malignancy: A Review.

Author

Lec PM, Lenis AT, Golla V, Brisbane W, Shuch B, Garraway IP, Reiter RE, and Chamie K

Subjects

Analgesics, Opioid administration & dosage, Cancer Pain etiology, Cell Movement drug effects, Cell Proliferation drug effects, Disease-Free Survival, Humans, Kidney drug effects, Kidney pathology, Male, Neoplasm Invasiveness pathology, Pain Management adverse effects, Pain Management methods, Perioperative Period, Prostate drug effects, Prostate pathology, Receptors, Opioid agonists, Urinary Bladder drug effects, Urinary Bladder pathology, Urologic Neoplasms complications, Urologic Neoplasms mortality, Urologic Neoplasms therapy, Analgesics, Opioid adverse effects, Cancer Pain drug therapy, Carcinogenesis drug effects, Receptors, Opioid metabolism, Urologic Neoplasms pathology

Abstract

Purpose: We reviewed the literature surrounding the role of opioids and their receptors in urological malignancy. Recent studies have suggested clinically significant effects of agonism or antagonism of opioid receptors on cancer related outcomes and tumorigenesis. The focus of these efforts has centered on nonurological malignancies. However, a compelling body of evidence is growing in the fields of prostate, bladder and kidney cancer., Materials and Methods: A systematic review of English language articles published through 2020 was conducted with key phrases related to kidney, bladder or prostate cancer, and opioids or narcotics. A total of 837 unique records were identified, of which 49 were selected for full text review and 33 were included in the qualitative analysis. Eight records were identified via citation review and 1 study was recently presented at a national meeting., Results: Retrospective reviews suggest poorer disease specific and recurrence-free survival with increased perioperative opioid administration in patients undergoing prostate or bladder cancer surgery. However, the data are controversial. Kappa opioid receptors are implicated in both proliferation and inhibition of prostate cancer cell growth across in vitro studies, with a proposed interaction with the androgen cascade. Similarly opioid growth factor receptor is highly expressed in prostate cancer cells and repressed by androgens. Prostate cancer tissue stains more intensely for the mu opioid receptor, and patients with higher expression have poorer oncologic outcomes. Opioid agonism in vitro induces urothelial cell carcinoma proliferation, migration and invasion, with possible additional influence from interactions with the bradykinin b2 receptor. Agonism of the mu, kappa and delta opioid receptors induces renal cell carcinoma tumorigenesis, possibly via upregulation of survivin. Meanwhile, opioid growth factor receptor agonism has the opposite effect in renal cell carcinoma., Conclusions: Evidence surrounding the role of opioids and their receptors in urological malignancy is provocative and should serve as an impetus for further investigation.

Published

2020

48. Potent and selective NOP receptor activation reduces cocaine self-administration in rats by lowering hedonic set point.

Author

Cippitelli A, Barnes M, Zaveri NT, and Toll L

Subjects

Animals, Buprenorphine, Cycloheptanes metabolism, Indoles metabolism, Male, Piperidines metabolism, Rats, Rats, Sprague-Dawley, Reinforcement Schedule, Self Administration, Nociceptin Receptor, Cocaine administration & dosage, Cocaine-Related Disorders metabolism, Receptors, Opioid agonists

Abstract

Developing new medications for the treatment of cocaine dependence continues to be a research priority. Compelling evidence indicates that mixed opioid receptor agonists, particularly bifunctional compounds that target nociceptin/orphanin FQ peptide (NOP) and mu opioid receptors, may be useful for the treatment of cocaine addiction. Here, we verify that potent and selective pharmacological activation of NOP receptors is sufficient to reduce relevant facets of cocaine addiction in animal models. Accordingly, we determined whether systemic injections of the small molecule AT-312 (0, 1, 3 mg/kg) could reduce operant cocaine self-administration, motivation for cocaine, and vulnerability to cocaine relapse in rats. Results indicate that a potent and selective NOP receptor agonist was equally efficacious in reducing the number of cocaine infusions in short (1-hour), as well as long (6-hour) access sessions. When tested on an economic-demand reinforcement schedule, AT-312 reduced Q 0 , the parameter that describes the amount of drug consumed at zero price, while leaving the parameter α, a measure of motivation for drug consumption, unaltered. Furthermore, AT-312 successfully reduced conditioned reinstatement of cocaine seeking. In contrast, the NOP receptor agonist did not modify food self-administration. Blockade of the NOP receptor with the antagonist SB-612111 prevented the effect of AT-312 in decreasing cocaine-reinforced responding under a 2-hour fixed ratio 1 schedule, suggesting a NOP receptor-mediated mechanism. This work demonstrates that potent and selective activation of NOP receptors is sufficient to decrease cocaine taking and seeking behaviors in rats., (© 2019 Society for the Study of Addiction.)

Published

2020

49. Biased Agonism at Nociceptin/Orphanin FQ Receptors: A Structure Activity Study on N/OFQ(1-13)-NH 2 .

Author

Pacifico S, Ferrari F, Albanese V, Marzola E, Neto JA, Ruzza C, Calò G, Preti D, and Guerrini R

Subjects

Animals, GTP-Binding Proteins chemistry, Peptide Fragments chemistry, Receptors, Opioid chemistry, Structure-Activity Relationship, Nociceptin Receptor, Nociceptin, Opioid Peptides pharmacology, Peptide Fragments agonists, Receptors, Opioid agonists

Abstract

Nociceptin/orphanin FQ (N/OFQ) controls different biological functions via selective stimulation of the N/OFQ peptide (NOP) receptor. The pleiotropic actions of N/OFQ may limit the development of NOP ligands as innovative drugs in different therapeutic areas. The pharmacological concept of functional selectivity (aka biased agonism) might be useful for amplifying beneficial actions and/or counteracting side effects. Thus, molecules with large bias factors toward G protein or β arrestin are required for investigating the translational value of NOP biased modulation. Herein, the biased behavior of a heterogeneous library of NOP-targeting peptide derivatives was evaluated in vitro with the aim to provide possible insights into the structural determinants that govern the selective activation of G protein versus β-arrestin. Our results demonstrate that lipidation of N/OFQ(1-13)-NH 2 is a useful strategy for obtaining G protein biased agonists for the NOP receptor.

Published

2020

50. Endogenous Opiates and Behavior: 2018.

Author

Bodnar RJ

Subjects

Animals, Humans, Mental Disorders metabolism, Narcotic Antagonists pharmacology, Opioid Peptides agonists, Opioid Peptides antagonists & inhibitors, Opioid Peptides pharmacology, Pain metabolism, Analgesics, Opioid pharmacology, Behavior drug effects, Learning physiology, Mental Disorders drug therapy, Opioid Peptides metabolism, Pain drug therapy, Receptors, Opioid agonists

Abstract

This paper is the forty-first consecutive installment of the annual anthological review of research concerning the endogenous opioid system, summarizing articles published during 2018 that studied the behavioral effects of molecular, pharmacological and genetic manipulation of opioid peptides and receptors as well as effects of opioid/opiate agonists and antagonists. The review is subdivided into the following specific topics: molecular-biochemical effects and neurochemical localization studies of endogenous opioids and their receptors (2), the roles of these opioid peptides and receptors in pain and analgesia in animals (3) and humans (4), opioid-sensitive and opioid-insensitive effects of nonopioid analgesics (5), opioid peptide and receptor involvement in tolerance and dependence (6), stress and social status (7), learning and memory (8), eating and drinking (9), drug abuse and alcohol (10), sexual activity and hormones, pregnancy, development and endocrinology (11), mental illness and mood (12), seizures and neurologic disorders (13), electrical-related activity and neurophysiology (14), general activity and locomotion (15), gastrointestinal, renal and hepatic functions (16), cardiovascular responses (17), respiration and thermoregulation (18), and immunological responses (19)., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020