The mixed-action delta/mu opioid agonist MMP-2200 does not produce conditioned place preference but does maintain drug self-administration in rats, and induces in vitro markers of tolerance and dependence

Stevenson, Glenn W.; Luginbuhl, Amy; Dunbar, Catherine; LaVigne, Justin; Dutra, Julio; Atherton, Phillip; Bell, Brooke E; Cone, Katherine; Giuvelis, Denise; Polt, Robin; Streicher, John M.; Bilsky, Edward J.

doi:10.1016/j.pbb.2015.02.022

Cited by 27 publications

(29 citation statements)

References 29 publications

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“…Although the similar withdrawal-like naltrexone-elicited effects on food-maintained responding were unexpected, it remains the case that dependence on M6S may have developed more slowly with M6S than with morphine. In that regard, similar results have been observed with a mixed l/d opioid glycopeptide, 37,47 where it was suggested that heterodimerization of l/d opioid receptors (modulating neuronal network effects of l-and d-containing neurons at a level above the individual receptor) or additional cellular regulators in neurons could modulate the induction of tolerance and dependence at the receptor level, slowing tolerance development. Indeed, it has been previously reported that drugs with affinity for l and j opioid receptors demonstrated different results across tests of thermal nociception, schedule-controlled responding and drug self-administration, and our previous and present reports with the mixed l/d opioid agonist M6S contributes to this growing body of literature demonstrating that novel drug-receptor interactions may elicit distinct effects across experimental endpoints (e.g.…”

Section: Discussionsupporting

confidence: 74%

“…One common adverse effect limiting the chronic use of μ opioid agonists is their notorious liability for abuse, physical dependence, and addiction . Prescription μ opioids are not only abused, but are also responsible for severe morbidity and death from overdose . The present report provides an initial characterization of the morphine‐like discriminative stimulus effects and physical dependence properties of the novel mixed‐action μ/δ opioid M6S in rats.…”

Section: Discussionmentioning

confidence: 89%

“…35 Prescription l opioids are not only abused, but are also responsible for severe morbidity and death from overdose. 36,37 The present report provides an initial characterization of the morphine-like discriminative stimulus effects and physical dependence properties of the novel mixed-action l/d opioid M6S in rats. Here we demonstrate that, unlike morphine and fentanyl, M6S did not fully substitute for morphine in drug discrimination, although this is likely due to the limited dose range tested.…”

Section: Discussionmentioning

confidence: 93%

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Evaluation of morphine‐like effects of the mixed mu/delta agonist morphine‐6‐O‐sulfate in rats: Drug discrimination and physical dependence

Yadlapalli

Bommagani

Mahelona

et al. 2018

Pharmacology Res & Perspec

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Morphine‐6‐O‐sulfate (M6S) is as a mixed‐action mu/delta (μ/δ) opioid receptor agonist with high potency and analgesic efficacy. These studies used assays of drug discrimination and schedule‐controlled responding to assess abuse‐liability, tolerance, and physical dependence as compared to morphine in rats. Attempts to train 0.3 mg/kg (IP) M6S from saline failed, but all rats rapidly acquired the discrimination when the training dose was changed to 3.0 mg/kg morphine, and substitution tests showed that morphine and fentanyl both fully substituted for the training dose, M6S and M3A6S (3‐O‐acetyl ester of M6S) only partially substituted, and salvinorin A did not elicit morphine‐like effects. Tolerance to response rate‐decreasing effects was studied in rats administered either 1.0 or 3.0 mg/kg morphine or M6S before food‐reinforced operant sessions. At both unit doses, tolerance to M6S‐elicited rate suppression developed more slowly than tolerance to morphine‐induced reductions in response rates. To assess dependence, rats were maintained on 1.0 mg/kg morphine or 1.0 mg/kg M6S until food‐reinforced response rates were stable for at least 5 days. Rats were then administered saline or increasing doses of the opioid antagonist naltrexone (NTX) (0.3, 1.0, 3.0, or 10.0 mg/kg) in order to determine antagonist‐precipitated withdrawal. NTX precipitated withdrawal was similar in both morphine‐maintained and M6S‐maintained rats. In conclusion, the mixed μ/δ agonist activity of M6S failed to completely protect against the development of physical dependence, but delayed tolerance development to behavioral effects and resulted in decreased morphine‐like subjective effects, perhaps implying a decreased abuse liability over μ agonists.

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Section: Discussionsupporting

confidence: 74%

Section: Discussionmentioning

confidence: 89%

Section: Discussionmentioning

confidence: 93%

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Evaluation of morphine‐like effects of the mixed mu/delta agonist morphine‐6‐O‐sulfate in rats: Drug discrimination and physical dependence

Yadlapalli

Bommagani

Mahelona

et al. 2018

Pharmacology Res & Perspec

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“…Accordingly, much effort has been dedicated to the development of new MOR agonists retaining potent analgesic effects, while mitigating or eliminating the deleterious side effects of the agents currently in use. 1–8 …”

Section: Introductionmentioning

confidence: 99%

Synthetic and Receptor Signaling Explorations of the Mitragyna Alkaloids: Mitragynine as an Atypical Molecular Framework for Opioid Receptor Modulators

et al. 2016

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Mu-opioid receptor agonists represent mainstays of pain management. However, the therapeutic use of these agents is associated with serious side effects, including potentially lethal respiratory depression. Accordingly, there is a longstanding interest in the development of new opioid analgesics with improved therapeutic profiles. The alkaloids of the Southeast Asian plant Mitragyna speciosa, represented by the prototypical member mitragynine, are an unusual class of opioid receptor modulators with distinct pharmacological properties. Here we describe the first receptor-level functional characterization of mitragynine and related natural alkaloids at the mu-, kappa-, and delta-opioid receptors. These results show that mitragynine and the oxidized analog 7-hydroxymitragynine, are partial agonists of the human mu-opioid receptor and competitive antagonists at the kappa- and delta-opioid receptors. We also show that mitragynine and 7-hydroxymitragynine are G-protein-biased agonists of the mu-opioid receptor, which do not recruit β-arrestin following receptor activation. Therefore, the Mitragyna alkaloid scaffold represents a novel framework for the development of functionally biased opioid modulators, which may exhibit improved therapeutic profiles. Also presented is an enantioselective total synthesis of both (-)-mitragynine and its unnatural enantiomer, (+)-mitragynine, employing a proline-catalyzed Mannich-Michael reaction sequence as the key transformation. Pharmacological evaluation of (+)-mitragynine revealed its much weaker opioid activity. Likewise, the intermediates and chemical transformations developed in the total synthesis allowed the elucidation of previously unexplored structure-activity relationships (SAR) within the Mitragyna scaffold. Molecular docking studies, in combination with the observed chemical SAR, suggest that Mitragyna alkaloids adopt a binding pose at the mu-opioid receptor that is distinct from that of classical opioids.

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“…Recent studies have investigated the pathways correlated with tolerance mechanisms in these receptors, especially in the face of morphine. Activation of β-arrestin-2, ERK1/2, and phosphorylated counterpart of ERK1/2 proteins was proved to be the most signaling pathways leading to µ-receptor downregulation and nally, drug dependence and antinociceptive tolerance [6][7][8].…”

Section: Introductionmentioning

confidence: 99%

Unlike Morphine, Long-Term Exposure to Analgesic Mitragynine, 7-Hydroxymitragynine, Paynantheine, and Speciociliatine Alkaloids Does Not Contribute to Antinociceptive Tolerance of μ-Opioid Receptors

Elahian¹,

Zahedian²,

Safaei³

et al. 2020

Preprint

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Abstract Background: Opioids are the most well known antinociceptive alkaloids all over the world, but tolerance and physical dependence are their dominant concerns in clinical applications. In contrast, monoterpene alkaloids are newly considered for their roles in pain management.Methods: In this regard, the clinical safety of mitragynine, 7-hydroxymitragynine, speciociliatine, and paynantheine was determined by cytotoxicity, antioxidant, and antigenotoxicity assays. In parallel alkaloids were studied on β-arrestin-2, ERK1/2, and p-ERK1/2 transcription and translation levels during three days on SH-SY5Y cells. Results: Results confirmed alkaloid- and concentration- dependency of the cytotoxicity, antigenotoxicity, and antioxidant activity. Although morphine was recorded as the safest alkaloid here, speciociliatine and mitragynine represented around 1200- and 20- fold higher DNA protection capacity than morphine, respectively. Monoterpene alkaloids transiently made the transcript ocean turbulent, but western blot analyses have proved significant down-regulation of targeted proteins in SH-SY5Y cells during the experiment days. Conclusions: Data indicated that monoterpene alkaloid derivatives are putative analgesic agents that do not stimulate opioid receptor tolerance and suggesting that patients may benefit from their antinociceptive activities without physical dependence or tolerance concerns in future clinics.

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The mixed-action delta/mu opioid agonist MMP-2200 does not produce conditioned place preference but does maintain drug self-administration in rats, and induces in vitro markers of tolerance and dependence

Cited by 27 publications

References 29 publications

Evaluation of morphine‐like effects of the mixed mu/delta agonist morphine‐6‐O‐sulfate in rats: Drug discrimination and physical dependence

Evaluation of morphine‐like effects of the mixed mu/delta agonist morphine‐6‐O‐sulfate in rats: Drug discrimination and physical dependence

Synthetic and Receptor Signaling Explorations of the Mitragyna Alkaloids: Mitragynine as an Atypical Molecular Framework for Opioid Receptor Modulators

Unlike Morphine, Long-Term Exposure to Analgesic Mitragynine, 7-Hydroxymitragynine, Paynantheine, and Speciociliatine Alkaloids Does Not Contribute to Antinociceptive Tolerance of μ-Opioid Receptors

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