A Novel G Protein-Biased Agonist at the δ Opioid Receptor with Analgesic Efficacy in Models of Chronic Pain.

Alexandra E Conibear,Eamonn Kelly,Bengt Von Mentzer,Valeria Tekus,Rob Hill,Junaid Asghar,Chris Bailey,Zsuzsanna Helyes,Josephine Palandri,Eva Borbely,David Kendall,Ingemar Starke,Graeme Henderson

doi:10.1124/jpet.119.258640

Abstract

Agonists at the δ opioid receptor are known to be potent antihyperalgesics in chronic pain models and effective in models of anxiety and depression. However, some δ opioid agonists have proconvulsant properties while tolerance to the therapeutic effects can develop. Previous evidence indicates that different agonists acting at the δ opioid receptor differentially engage signaling and regulatory pathways with significant effects on behavioral outcomes. As such, interest is now growing in the development of biased agonists as a potential means to target specific signaling pathways and potentially improve the therapeutic profile of δ opioid agonists. Here, we report on PN6047 (3-[[4-(dimethylcarbamoyl)phenyl]-[1-(thiazol-5-ylmethyl)-4-piperidylidene]methyl]benzamide), a novel G protein–biased and selective δ opioid agonist. In cell-based assays, PN6047 fully engages G protein signaling but is a partial agonist in both the arrestin recruitment and internalization assays. PN6047 is effective in rodent models of chronic pain but shows no detectable analgesic tolerance following prolonged treatment. In addition, PN6047 exhibited antidepressant-like activity in the forced swim test, and importantly, the drug had no effect on chemically induced seizures. PN6047 did not exhibit reward-like properties in the conditioned place preference test or induce respiratory depression. Thus, δ opioid ligands with limited arrestin signaling such as PN6047 may be therapeutically beneficial in the treatment of chronic pain states.SIGNIFICANCE STATEMENTPN6047 (3-[[4-(dimethylcarbamoyl)phenyl]-[1-(thiazol-5-ylmethyl)-4-piperidylidene]methyl]benzamide) is a selective, G protein–biased δ opioid agonist with efficacy in preclinical models of chronic pain. No analgesic tolerance was observed after prolonged treatment, and PN6047 does not display proconvulsant activity or other opioid-mediated adverse effects. Our data suggest that δ opioid ligands with limited arrestin signaling will be beneficial in the treatment of chronic pain.

Highlights

Treatment of chronic pain remains a significant medical challenge; in terms of analgesics, m opioid ligands such as morphine are routinely, albeit inappropriately, prescribed at present
In comparison with m receptor agonists, d receptor agonists are associated with a milder adverse effect profile with no respiratory depression (Gallantine and Meert, 2005), little or no gastrointestinal dysfunction (Gallantine and Meert, 2005; Feng et al, 2006), ABBREVIATIONS: BRET, bioluminescence resonance energy transfer; CPP, conditioned place preference; DADLE, [D-Ala2, D-Leu5]-enkephalin; DAMGO, [D-Ala2, N-MePhe4, Gly-ol]-enkephalin; DMEM, Dulbecco’s modified Eagle’s medium; DOPr, d opioid receptor; GFP, Green Fluorescent Protein; HA, hemagglutinin; Human embryonic kidney 293 (HEK293), human embryonic kidney 293; HPMC, hydroxypropyl methylcellulose; MIA, mono-iodoacetate; pERK, phosphorylated ERK; PN6047, 3-[[4-(dimethylcarbamoyl)phenyl]-[1-(thiazol-5-ylmethyl)-4-piperidylidene]methyl]benzamide; PO, by mouth; PTZ, pentylenetetrazol; Rluc, Renilla Luciferase; SNL, sciatic nerve ligation
We report on PN6047 (3-[[4-(dimethylcarbamoyl) phenyl]-[1-(thiazol-5-ylmethyl)-4-piperidylidene]methyl]benzamide), a novel and selective d opioid receptor agonist structurally derived from SNC80

Summary

Introduction

Treatment of chronic pain remains a significant medical challenge; in terms of analgesics, m opioid ligands such as morphine are routinely, albeit inappropriately, prescribed at present. M opioid receptor ligands are effective in treating acute, severe pain, they often lack efficacy in chronic pain states (Glajchen (2001), and their clinical utility in such. Increasing evidence implicates the d opioid receptor as an attractive therapeutic target for various forms of chronic pain and certain emotional disorders, including depression and anxiety (Pradhan et al, 2011). In comparison with m receptor agonists, d receptor agonists are associated with a milder adverse effect profile with no respiratory depression (Gallantine and Meert, 2005), little or no gastrointestinal dysfunction (Gallantine and Meert, 2005; Feng et al, 2006), ABBREVIATIONS: BRET, bioluminescence resonance energy transfer; CPP, conditioned place preference; DADLE, [D-Ala, D-Leu5]-enkephalin; DAMGO, [D-Ala, N-MePhe, Gly-ol]-enkephalin; DMEM, Dulbecco’s modified Eagle’s medium; DOPr, d opioid receptor; GFP, Green Fluorescent Protein; HA, hemagglutinin; HEK293, human embryonic kidney 293; HPMC, hydroxypropyl methylcellulose; MIA, mono-iodoacetate; pERK, phosphorylated ERK; PN6047, 3-[[4-(dimethylcarbamoyl)phenyl]-[1-(thiazol-5-ylmethyl)-4-piperidylidene]methyl]benzamide; PO, by mouth; PTZ, pentylenetetrazol; Rluc, Renilla Luciferase; SNL, sciatic nerve ligation

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