ABSTRACT
Synthetic opioids have been implicated as the single greatest contributor to rising drug-related fatalities in recent years. This study evaluated mu-opioid receptor (MOR) mediated effects of seven fentanyl-related substances that have emerged in the recreational drug marketplace, and for which there are no existing or only limited in vivo data. Adult male Swiss Webster mice were administered fentanyl-related substances and their effects on nociception and locomotion as compared to MOR agonist standards were observed. In locomotor activity tests, morphine (100, 180 mg/kg), fentanyl (1, 10 mg/kg), beta-methylfentanyl (10 mg/kg), para-methoxyfentanyl (10 mg/kg), fentanyl carbamate (100 mg/kg), and 3-furanylfentanyl (10 mg/kg), elicited significant (p ≤ 0.05) dose-dependent increases in locomotion. However, para-methylfentanyl and beta'-phenylfentanyl did not produce significant effects on locomotion at doses up to 100 mg/kg and phenylfentanyl (100 mg/kg) significantly decreased locomotion. In warm-water tail-withdrawal tests, all substances produced significant dose-dependent increases in antinociception with increasing ED50 values (95% CI) of fentanyl [0.08 mg/kg (0.04-0.16)] > para-methoxyfentanyl [0.43 mg/kg (0.23-0.77)] > 3-furanylfentanyl [0.51 mg/kg (0.36-0.74)] > beta-methylfentanyl [0.74 mg/kg (0.64-0.85)] > para-methylfentanyl [1.92 mg/kg (1.48-2.45)] > fentanyl carbamate [5.59 mg/kg (4.11-7.54)] > morphine [7.82 mg/kg (5.42-11.0)] > beta'-phenylfentanyl [19.4 mg/kg (11.0-34.4)] > phenylfentanyl [55.2 mg/kg (33.5-93.0)]. Naltrexone (1 mg/kg) increased ED50 values several fold with decreasing magnitudes of para-methylfentanyl (63.1×) > para-methoxyfentanyl (22.5×) > beta'-phenylfentanyl (21.0×) > 3-furanylfentanyl (20.6×) > beta-methylfentanyl (19.2×) > phenylfentanyl (5.23×) > fentanyl (3.95×) > fentanyl carbamate (2.21×) > morphine (1.48×). These findings expand upon in vivo results from previous studies and establish that the effects of these fentanyl related-related substances are at least in part mediated by the MOR.
Subject(s)
Fentanyl/pharmacology , Locomotion/drug effects , Nociception/drug effects , Receptors, Opioid, mu/metabolism , Analgesics, Opioid/pharmacology , Animals , Fentanyl/analogs & derivatives , Furans/pharmacology , Male , Mice , Morphine/pharmacology , Naltrexone/pharmacology , Narcotics/pharmacology , Receptors, Opioid/metabolism , Receptors, Opioid, mu/agonistsABSTRACT
BACKGROUND: Antagonism of peripheral opioid receptors by methylnaltrexone (MNTX) was recently proposed as a potential mechanism to attenuate the development of opioid analgesic tolerance based on experiments conducted in mice. However, reports indicate that MNTX is demethylated to naltrexone (NTX) in mice, and NTX may subsequently cross the blood-brain barrier to antagonize centrally-mediated opioid effects. The goal of this study was to determine whether MNTX alters centrally-mediated behaviors elicited by the opioid analgesics, morphine and oxycodone, and to quantify concentrations of MNTX and NTX in blood and brain following their administration in mice. METHODS: Combinations of MNTX and morphine were tested under acute and chronic conditions in thermal nociceptive assays. Effects of MNTX and NTX pretreatment were assessed in an oxycodone discrimination operant procedure. Blood and brain concentrations of these antagonists were quantified after their administration using liquid chromatography-mass spectrometry. RESULTS: MNTX dose-dependently attenuated acute and chronic morphine antinociception. MNTX and NTX dose-dependently antagonized the discriminative stimulus effects of oxycodone. MNTX and NTX were detected in both blood and brain after administration of MNTX, confirming its demethylation and demonstrating that MNTX itself can cross the blood-brain barrier. CONCLUSIONS: These results provide converging behavioral and analytical evidence that MNTX administration in mice attenuates centrally-mediated effects produced by opioid analgesics and results in functional concentrations of MNTX and NTX in blood and brain. Collectively, these findings indicate that MNTX cannot be administered systemically in mice for making inferences that its effects are peripherally restricted.
Subject(s)
Analgesics, Opioid/pharmacology , Blood-Brain Barrier/drug effects , Morphine/pharmacology , Naltrexone/analogs & derivatives , Narcotic Antagonists/pharmacology , Oxycodone/pharmacology , Analgesics, Opioid/antagonists & inhibitors , Animals , Blood-Brain Barrier/metabolism , Dose-Response Relationship, Drug , Male , Mice , Mice, Inbred C57BL , Morphine/antagonists & inhibitors , Naltrexone/metabolism , Naltrexone/pharmacology , Narcotic Antagonists/metabolism , Oxycodone/antagonists & inhibitors , Pain Measurement/drug effects , Pain Measurement/methods , Quaternary Ammonium Compounds/metabolism , Quaternary Ammonium Compounds/pharmacologyABSTRACT
The emergence of several fentanyl-related substances in the recreational drug marketplace has resulted in a surge of opioid overdose deaths in the United States. Many of these substances have never been examined in living organisms under controlled conditions. In the present study, seven fentanyl-related substances were tested in adult male Swiss Webster mice for their effects on locomotion and antinociception and compared to those of fentanyl and morphine. In locomotor activity tests, fentanyl (1, 10â¯mg/kg), morphine (100, 180â¯mg/kg), isobutyrylfentanyl (10â¯mg/kg), crotonylfentanyl (10â¯mg/kg), para-fluorobutyrylfentanyl (10, 100â¯mg/kg), para-methoxybutyrylfentanyl (10â¯mg/kg), thiophenefentanyl (100â¯mg/kg), and benzodioxolefentanyl (0.1â¯mg/kg) produced significant (pâ¯≤â¯0.05) dose-dependent increases in locomotion. Valerylfentanyl, however, was without effects on locomotion up to 100â¯mg/kg. In warm-water tail-withdrawal tests, all substances produced significant (pâ¯≤â¯0.05) dose-dependent increases in antinociception with increasing ED50 values (CI) of isobutyrylfentanyl [0.0768â¯mg/kg (0.044-0.128)]â¯>â¯fentanyl [0.0800â¯mg/kg (0.0403-0.164)]â¯>â¯para-methoxybutyrylfentanyl [0.106â¯mg/kg (0.0516-0.195)]â¯>â¯crotonylfentanyl [0.226â¯mg/kg (0.176-0.292)]â¯>â¯para-fluorobutyrylfentanyl [0.908â¯mg/kg (0.459-1.58)]â¯>â¯thiophenefentanyl [4.66â¯mg/kg (3.65-5.95)]â¯>â¯valerylfentanyl [6.43â¯mg/kg (3.91-10.5)]â¯>â¯morphine [7.82â¯mg/kg (5.42-11.0)]â¯>â¯benzodioxolefentanyl [46.3â¯mg/kg (25.8-83.4)]. Naltrexone (1â¯mg/kg) increased antinociceptive ED50 values several fold in decreasing magnitudes of isobutyrylfentanyl (233x)â¯>â¯para-methoxybutyrylfentanyl (37.7x)â¯>â¯thiophenefentanyl (34.6x)â¯>â¯valerylfentanyl (11.9x)â¯>â¯para-fluorobutyrylfentanyl (10.9x)â¯>â¯benzodioxolefentanyl (8.42x)â¯>â¯crotonylfentanyl (6.27x)â¯>â¯fentanyl (3.95x)â¯>â¯morphine (1.48x). These findings establish that locomotor and antinociceptive effects of several fentanyl-related substances are similar to those of morphine and fentanyl and are mediated by opioid receptors.
Subject(s)
Fentanyl/pharmacology , Motor Activity/drug effects , Narcotics/pharmacology , Nociception/drug effects , Pain Threshold/drug effects , Animals , Dose-Response Relationship, Drug , Male , Mice , Morphine/pharmacologyABSTRACT
BACKGROUND: Fentanyl and its structurally related compounds have emerged as the most significant contributors to opioid overdose fatalities in recent years. While there is abundant information about the pharmacological effects of fentanyl, far less is known of its more recently abused analogs. The objective of this study was to determine whether fentanyl and several fentanyl-related substances would engender oxycodone-like responding in a mouse model of oxycodone discrimination. Oxycodone was selected as the training drug due to its high selectivity for mu opioid receptors. Compounds that elicited oxycodone-like responding in this procedure would likely evoke overlapping subjective experiences. METHODS: Adult male C57BL/6 mice were trained to discriminate 1.3â¯mg/kg oxycodone from vehicle in a food-reinforced, two-lever choice procedure. Generalization tests were conducted with fentanyl and the following fentanyl-related compounds: ocfentanil, 3-furanyl fentanyl, crotonylfentanyl, and valerylfentanyl. RESULTS: Fentanyl and each of its analogs completely generalized to the 1.3â¯mg/kg oxycodone discriminative stimulus and naltrexone pretreatment significantly decreased oxycodone-like responding for each compound. Rank order potency for engendering oxycodone-appropriate responding was ocfentanilâ¯>â¯fentanyl > 3-furanyl fentanylâ¯≈â¯crotonylfentanylâ¯>â¯oxycodoneâ¯>â¯valerylfentanyl. Drug doses that evoked full substitution also significantly suppressed response rates compared to vehicle. CONCLUSIONS: These results indicate that the discriminative stimulus, and by extension, the interoceptive and subjective effects of the tested fentanyl analogs, overlap with those of oxycodone. These observations consequentially support the prediction that they would also engender the likelihood for abuse similar to oxycodone. This article is part of the Special Issue entitled 'Opioid Neuropharmacology: Advances in treating pain and opioid addiction'.