Preclinical Testing of Nalfurafine as an Opioid-sparing Adjuvant that Potentiates Analgesia by the Mu Opioid Receptor-targeting Agonist Morphine

Kaski, Shane W; White, Allison N; Gross, Joshua; Trexler, Kristen R.; Wix, Kim; Harland, Aubrie A.; Prisinzano, Thomas E.; Aubé, Jeffrey; Kinsey, Steven G.; Kenakin, Terry; Siderovski, David P.; Setola, Vincent

doi:10.1124/jpet.118.255661

Cited by 39 publications

(37 citation statements)

References 85 publications

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“…agonists (DiMattio et al, 2015;White et al, 2015;Dunn et al, 2018Dunn et al, , 2019Ho et al, 2018;Kaski et al, 2019;Mores et al, 2019). In addition, a recent paper showed low intrinsic efficacy, rather than G-protein bias, could explain the reduced respiratory side effects in MOPr agonists (Gillis et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

“…In support of this, the biased agonist RB-64, showed no sedation, motor incoordination, or anhedonia-like effects in mice ( White et al, 2015 ) and the only clinically available KOPr agonist, nalfurafine, has been shown to be extremely G-protein biased ( Schattauer et al, 2017 ). However, few reports have fully explored biased signaling at KOPr and correlated this to antinociceptive effects and side effects in structurally similar agonists ( DiMattio et al, 2015 ; White et al, 2015 ; Dunn et al, 2018 , 2019 ; Ho et al, 2018 ; Kaski et al, 2019 ; Mores et al, 2019 ). In addition, a recent paper showed low intrinsic efficacy, rather than G-protein bias, could explain the reduced respiratory side effects in MOPr agonists ( Gillis et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

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Evaluation of Biased and Balanced Salvinorin A Analogs in Preclinical Models of Pain

et al. 2020

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In the search for safer, non-addictive analgesics, kappa opioid receptor (KOPr) agonists are a potential target, as unlike mu-opioid analgesics, they do not have abuse potential. Salvinorin A (SalA) is a potent and selective KOPr agonist, however, clinical utility is limited by the short duration of action and aversive side effects. Biasing KOPr signaling toward G-protein activation has been highlighted as a key cellular mechanism to reduce the side effects of KOPr agonists. The present study investigated KOPr signaling bias and the acute antinociceptive effects and side effects of two novel analogs of SalA, 16-Bromo SalA and 16-Ethynyl SalA. 16-Bromo SalA showed G-protein signaling bias, whereas 16-Ethynyl SalA displayed balanced signaling properties. In the dose-response tail-withdrawal assay, SalA, 16-Ethynyl SalA and 16-Bromo SalA were more potent than the traditional KOPr agonist U50,488, and 16-Ethynyl SalA was more efficacious. 16-Ethynyl SalA and 16-Bromo SalA both had a longer duration of action in the warm water tail-withdrawal assay, and 16-Ethynyl had greater antinociceptive effect in the hot-plate assay, compared to SalA. In the intraplantar 2% formaldehyde test, 16-Ethynyl SalA and 16-Bromo SalA significantly reduced both nociceptive and inflammatory pain-related behaviors. Moreover, 16-Ethynyl SalA and 16-Bromo SalA had no anxiogenic effects in the marble burying task, and 16-Bromo SalA did not alter behavior in the elevated zero maze. Overall, 16-Ethynyl SalA significantly attenuated acute pain-related behaviors in multiple preclinical models, while the biased KOPr agonist, 16-Bromo SalA, displayed modest antinociceptive effects, and lacked anxiogenic effects.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Evaluation of Biased and Balanced Salvinorin A Analogs in Preclinical Models of Pain

et al. 2020

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“…Although weaker evidence of punishment was observed with nalfurafine based on statistical analysis, the overall findings were consistent with a recent report of contingently administered nalfurafine and salvinorin A decreasing rates of oxycodone self-administration under a progressive-ratio schedule of reinforcement in rhesus monkeys (Zamarripa et al 2020). Considered alongside reports that nalfurafine and other G-protein biased KOR agonists attenuate the conditioned rewarding effects of MOR agonists (Kaski et al 2019; Tsuji et al 2001), these results suggest that the abuse-limiting effects of KOR agonists may be G-protein mediated. Furthermore, in light of evidence that the aversive effects of KOR agonists are beta-arrestin mediated (Bruchas and Chavkin 2010; Bruchas et al 2007), these results also suggest that aversion may not be a necessary component of KOR-mediated punishment.…”

Section: Discussionmentioning

confidence: 67%

Effects of Kappa Opioid Receptor Agonists on Fentanyl vs. Food Choice in Male and Female Rats: Contingent vs. Non-Contingent Administration

Townsend

2020

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RationaleStrategies are needed to decrease the abuse liability of mu opioid receptor (MOR) agonists. One strategy under consideration is to combine MOR agonists with kappa opioid receptor (KOR) agonists.ObjectivesThe effects of KOR-agonists (U50488, nalfurafine) on fentanyl-versus-food choice were compared under conditions where the KOR agonists were added to the self-administered fentanyl (contingent delivery) or administered as pretreatments (non-contingent delivery) in male and female rats. The effects of increasing and decreasing the magnitude of the alternative food reinforcer were also determined.MethodsRats were trained to respond under a concurrent schedule of fentanyl (0, 0.32-10 μg/kg/infusion) and food reinforcement. In Experiment 1, U50488 and nalfurafine were co-administered with fentanyl as fixed-proportion mixtures (contingent administration). In Experiment 2, U50488 (1-10 mg/kg) and nalfurafine (3.2-32 μg/kg) were administered as acute pretreatments (non-contingent administration). nor-BNI (32 mg/kg) was administered prior to contingent and non-contingent KOR-agonist treatment in Experiment 3. Experiment 4 evaluated the effects of increasing and decreasing the magnitude of the non-drug reinforcer.ResultsBoth U50488 and nalfurafine decreased fentanyl choice when administered contingently, demonstrating that KOR agonists punish opioid choice. Non-contingent U50488 and nalfurafine administration decreased rates of fentanyl and food self-administration without altering fentanyl choice. Both contingent and non-contingent U50488 and nalfurafine effects on fentanyl choice were attenuated by nor-BNI. Fentanyl choice was sensitive to increases and decreases in the magnitude of the non-drug reinforcer.ConclusionsThese results demonstrate that the effects of KOR agonists on fentanyl reinforcement are dependent upon the contingencies under which they are administered.

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“…Many studies have sought to measure the bias factor, to understand the lack of sideeffects traditionally associated with KOPr agonists, however, there have been mixed results (Table 1). In human embryonic kidney-293 (HEK293) cells, nalfurafine was a G-protein biased agonist compared to U50,488 (Kaski et al, 2019), with moderate G-protein bias at the rat KOPr and extreme G-protein bias at the human KOPr (Schattauer et al, 2017).…”

Section: Nalfurafinementioning

confidence: 99%

“…2). Mesyl SalB and EOM are G-protein biased at the human KOPr using U50,488 as a reference ligand (Kivell et al, 2018;Kaski et al, 2019). However, EOM SalB was also found to be β-arrestin biased at the mouse KOPr with dynorphin A 1-17 as the reference ligand (DiMattio et al, 2015).…”

Section: Salvinorin a Analoguesmentioning

confidence: 99%

Strategies for DevelopingκOpioid Receptor Agonists for the Treatment of Pain with Fewer Side Effects

Paton

Atigari

Kaska

et al. 2020

J Pharmacol Exp Ther

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Preclinical Testing of Nalfurafine as an Opioid-sparing Adjuvant that Potentiates Analgesia by the Mu Opioid Receptor-targeting Agonist Morphine

Cited by 39 publications

References 85 publications

Evaluation of Biased and Balanced Salvinorin A Analogs in Preclinical Models of Pain

Evaluation of Biased and Balanced Salvinorin A Analogs in Preclinical Models of Pain

Effects of Kappa Opioid Receptor Agonists on Fentanyl vs. Food Choice in Male and Female Rats: Contingent vs. Non-Contingent Administration

Strategies for DevelopingκOpioid Receptor Agonists for the Treatment of Pain with Fewer Side Effects

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