Biased Opioid Antagonists as Modulators of Opioid Dependence: Opportunities to Improve Pain Therapy and Opioid Use Management

Sadée, Wolfgang; Oberdick, John; Wang, Zaijie

doi:10.3390/molecules25184163

Cited by 9 publications

(19 citation statements)

References 63 publications

(123 reference statements)

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“…Alternatively, 6BN may interact in novel ways with the opioid receptor, possibly binding with high affinity to a distinct receptor conformation involved in the development of dependence. For example, Jeske (Jeske 2019) has proposed a receptor model with distinct peripheral and central mu opioid receptor forms that could in part account for the observed peripheral selectivity of 6BN, even in rhesus monkeys where it readily penetrates the adult's brain (J. Oberdick, unpublished results; see also (Sadee et al, 2020)). It appears that our current understanding of the molecular pharmacology of opioid receptors is incomplete-requiring a new approach to account for the high potency of 6BN in selectively preventing opioid withdrawal behavior in dependent animals, as observed here and in mice (Oberdick et al, 2016;Sadee et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

Pharmacological Prevention of Neonatal Opioid Withdrawal in a Pregnant Guinea Pig Model

et al. 2021

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Newborns exposed to prenatal opioids often experience intense postnatal withdrawal after cessation of the opioid, called neonatal opioid withdrawal syndrome (NOWS), with limited pre- and postnatal therapeutic options available. In a prior study in pregnant mice we demonstrated that the peripherally selective opioid antagonist, 6β-naltrexol (6BN), is a promising drug candidate for preventive prenatal treatment of NOWS, and a therapeutic mechanism was proposed based on preferential delivery of 6BN to fetal brain with relative exclusion from maternal brain. Here, we have developed methadone (MTD) treated pregnant guinea pigs as a physiologically more suitable model, enabling detection of robust spontaneous neonatal withdrawal. Prenatal MTD significantly aggravates two classic maternal separation stress behaviors in newborn guinea pigs: calling (vocalizing) and searching (locomotion) - natural attachment behaviors thought to be controlled by the endogenous opioid system. In addition, prenatal MTD significantly increases the levels of plasma cortisol in newborns, showing that cessation of MTD at birth engages the hypothalamic-pituitary-adrenal (HPA) axis. We find that co-administration of 6BN with MTD prevents these withdrawal symptoms in newborn pups with extreme potency (ID50 ∼0.02 mg/kg), at doses unlikely to induce maternal or fetal withdrawal or to interfere with opioid antinociception based on many prior studies in rodents and non-human primates. Furthermore, we demonstrate a similarly high potency of 6BN in preventing opioid withdrawal in adult guinea pigs (ID50 = 0.01 mg/kg). This high potency appears to run counter to our pharmacokinetic studies showing slow 6BN transit of both the placenta and maternal blood brain barrier in guinea pigs, and calls into question the preferential delivery mechanism. Rather, it suggests a novel receptor mechanism to account for the selectively high potency of 6BN to suppress opioid dependence at all developmental stages, even in adults, as compared to its well-established low potency as a classical opioid antagonist. In conclusion, 6BN is an attractive compound for development of a preventive therapy for NOWS.

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Section: Discussionmentioning

confidence: 99%

Pharmacological Prevention of Neonatal Opioid Withdrawal in a Pregnant Guinea Pig Model

et al. 2021

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“…Referred to as shape-shifters [16], GPCRs exist in multiple silent and active conformations signaling along diverse pathways. Ligands can interact preferentially with each of these states, leading to design of biased agonists and antagonists with favorable pharmacological properties [6,7,29]. Receptor states are stabilized by allosteric interactions with other membrane components such as cholesterol and proteins, generating receptor ensembles poised for ligand activation or already basally active in a ligand-free form.…”

Section: Gpcrs Displaying Documented Ligand-free Signalingmentioning

confidence: 99%

Ligand-Free Signaling of G-Protein-Coupled Receptors: Physiology, Pharmacology, and Genetics

Sadee

2023

Molecules

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G-protein-coupled receptors (GPCRs) are ubiquitous sensors and regulators of cellular functions. Each GPCR exists in complex aggregates with multiple resting and active conformations. Designed to detect weak stimuli, GPCRs can also activate spontaneously, resulting in basal ligand-free signaling. Agonists trigger a cascade of events leading to an activated agonist-receptor G-protein complex with high agonist affinity. However, the ensuing signaling process can further remodel the receptor complex to reduce agonist affinity, causing rapid ligand dissociation. The acutely activated ligand-free receptor can continue signaling, as proposed for rhodopsin and μ opioid receptors, resulting in robust receptor activation at low agonist occupancy with enhanced agonist potency. Continued receptor stimulation can further modify the receptor complex, regulating sustained ligand-free signaling—proposed to play a role in opioid dependence. Basal, acutely agonist-triggered, and sustained elevated ligand-free signaling could each have distinct functions, reflecting multi-state conformations of GPCRs. This review addresses basal and stimulus-activated ligand-free signaling, its regulation, genetic factors, and pharmacological implications, focusing on opioid and serotonin receptors, and the growth hormone secretagogue receptor (GHSR). The hypothesis is proposed that ligand-free signaling of 5-HT2A receptors mediate therapeutic effects of psychedelic drugs. Research avenues are suggested to close the gaps in our knowledge of ligand-free GPCR signaling.

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“…While the rewarding, addictive and consequent withdrawal effects associated with opioid use are major side effects, their complex and multi-faceted nature as well as the myriad of approaches used to investigate them are outside the scope of this review. The mechanisms underlying these behaviours, as well as the methods used to study them in preclinical models are elegantly reviewed elsewhere (Banks & Negus, 2017;Charbogne, Kieffer, & Befort, 2014;Kreek, et al, 2012;Negus & Moerke, 2019;Rodríguez-Arias, Aguilar, Manzanedo, & Miñarro, 2010;Sadee, Oberdick, & Wang, 2020;Swain, Gewirtz, & Harris, 2021)…”

Section: -Introductionmentioning

confidence: 99%

Experimental considerations for the assessment of in vivo and in vitro opioid pharmacology

Hill

Canals

2022

Pharmacology & Therapeutics

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Morphine and other mu-opioid receptor (MOR) agonists remain the mainstay treatment of acute and prolonged pain states worldwide. The major limiting factor for continued use of these current opioids is the high incidence of side effects that result in loss of life and loss of quality of life. The development of novel opioids bereft, or much less potent, at inducing these side effects remains an intensive area of research, with multiple pharmacological strategies being explored. However, as with many G protein-coupled receptors (GPCRs), translation of promising candidates from in vitro characterisation to successful clinical candidates still represents a major challenge and attrition point. This review summarises the preclinical animal models used to evaluate the key opioid-induced behaviours of antinociception, respiratory depression, constipation and opioid-induced hyperalgesia and tolerance.We highlight the influence of distinct variables in the experimental protocols, as well as the potential implications for differences in receptor reserve in each system. Finally, we discuss how methods to assess opioid action in vivo and in vitro relate to each other in the context of bridging the translational gap in opioid drug discovery.

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Biased Opioid Antagonists as Modulators of Opioid Dependence: Opportunities to Improve Pain Therapy and Opioid Use Management

Cited by 9 publications

References 63 publications

Pharmacological Prevention of Neonatal Opioid Withdrawal in a Pregnant Guinea Pig Model

Pharmacological Prevention of Neonatal Opioid Withdrawal in a Pregnant Guinea Pig Model

Ligand-Free Signaling of G-Protein-Coupled Receptors: Physiology, Pharmacology, and Genetics

Experimental considerations for the assessment of in vivo and in vitro opioid pharmacology

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