Endogenous Orphanin FQ/Nociceptin Is Involved in the Development of Morphine Tolerance

Chung, Shinjae; Pohl, Sigrun; Zeng, Joanne; Civelli, Olivier; Reinscheid, Rainer K.

doi:10.1124/jpet.106.103960

Cited by 64 publications

(57 citation statements)

References 38 publications

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“…In support of these findings, it is notable that previous studies have shown that both NOP receptor KO (Ueda et al, 2000) and N/OFQ precursor KO (Chung et al, 2006) mice fail to develop tolerance to chronic morphine administration. Similar results are seen following administration of the NOP receptor antagonists (Zaratin et al, 2004;Chung et al, 2006).…”

Section: Endogenous N/ofq and The Plastic Changes That Underlie The Csupporting

confidence: 71%

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Endogenous Nociceptin (Orphanin FQ) Suppresses Basal Hedonic State and Acute Reward Responses to Methamphetamine and Ethanol, but Facilitates Chronic Responses

Sakoori

Murphy

2007

Neuropsychopharmacol

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The opioid peptide nociceptin (orphanin FQ) suppresses drug reward, drug self-administration, and impedes some of the processes believed to underlie the transition to addiction. As virtually all previous studies have used administration of nociceptin receptor agonists to evaluate the role of nociceptin on addiction-like behavior, the current study used a pharmacological (nociceptin receptor antagonist) and genetic (nociceptin receptor knockout mice) approach to elucidate the role of endogenous nociceptin. The nociceptin receptor antagonist UFP-101 induced a modest place preference, and enhanced the conditioned place preference induced by methamphetamine. In agreement with this, nociceptin receptor knockout mice had slightly enhanced methamphetamine and ethanol conditioned place preferences compared to wild-type mice. This effect did not appear to depend on differences in learning ability, as nociceptin receptor knockout mice had slightly weaker-conditioned place aversions to lithium chloride, the k-opioid receptor agonist, U50488H, and the general opiate antagonist, naloxone. The development of behavioral sensitization to methamphetamine was lower in nociceptin receptor knockout mice, and attenuated by UFP-101 administration to wild-type mice. Additionally, ethanol consumption and preference in a two-bottle choice test was lower in nociceptin receptor knockout mice, though ethanol-stimulated locomotion was stronger. Whereas the rewarding effect of methamphetamine and ethanol following chronic treatment, as measured by place conditioning, strengthened in wild-type mice, this effect was absent in nociceptin receptor knockout mice. These results suggest that endogenous N/OFQ suppresses basal and drug-stimulated increases in hedonic state, and plays either a permissive or facilitatory role in the development of addiction.

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Section: Endogenous N/ofq and The Plastic Changes That Underlie The Csupporting

confidence: 71%

“…Similar results are seen following administration of the NOP receptor antagonists (Zaratin et al, 2004;Chung et al, 2006). Additionally, mice with null mutations of the N/OFQ gene adapt poorly to repeated stress (Koster et al, 1999).…”

Section: Endogenous N/ofq and The Plastic Changes That Underlie The Csupporting

confidence: 66%

Endogenous Nociceptin (Orphanin FQ) Suppresses Basal Hedonic State and Acute Reward Responses to Methamphetamine and Ethanol, but Facilitates Chronic Responses

Sakoori

Murphy

2007

Neuropsychopharmacol

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“…Thus, we next investigated the effect of pretreatment with the selective ORL1 antagonist J-113397 on 030418 tolerance. The experimental results suggested that pharmacological blockade with J-113397 significantly prevented analgesic tolerance to morphine on d 7, which confirms earlier findings [30,31] . In contrast, pretreatment with J-113397 could not effectively alter the development of tolerance to 030418.…”

Section: Discussionsupporting

confidence: 80%

“…Many previous studies have used high doses of opioid drugs to induce and study tolerance [27,30,31] . As expected, repeated treatment with morphine (30 mg/kg, sc, thrice daily) induced the rapid development of analgesic tolerance.…”

Section: Development Of 030418 Tolerance and The Effect Of Pretreatmementioning

confidence: 99%

Pharmacological mechanisms underlying the antinociceptive and tolerance effects of the 6,14-bridged oripavine compound 030418

Wen¹,

Yu²,

Li³

et al. 2011

Acta Pharmacol Sin

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Aim: To investigate possible pharmacological mechanisms underlying the antinociceptive effect of and tolerance to N-methyl-7α-[(R)-1-hydroxy-1-methyl-3-(thien-3-yl)-propyl]-6,14-endo-ethanotetrahydronororipavine (030418), a derivative of thienorphine. Methods: The binding affinity and efficacy of 030418 were determined using receptor binding and guanosine 5′-O-(3-[ 35 S]thio)triphosphate ([ 35 S]GTPγS) assays in CHO-μ, CHO-κ, CHO-δ, and CHO-ORL1 cell membranes. The analgesic activity of and tolerance to 030418 were evaluated in thermal nociceptive tests in mice. The effects of 030418 on opioid receptors were further investigated using in vivo pharmacological antagonist blockade and in vitro tissue preparations. Results: The compound 030418 displayed high binding affinity to all subtypes of opioid receptors with K i values in the nanomolar range. In [ 35 S]GTPγS binding assay, the maximal stimulation of 030418 to μ-, κ-, δ-receptors and the ORL1 receptor was 89%, 86%, 67% and 91%, respectively. In hot-plate test, the antinociceptive effect of 030418 was more potent and longer than morphine. The nonselective opioid receptor antagonist naloxone could completely block 030418-induced antinociception, while both the μ-opioid receptor antagonist β-FNA and the κ-opioid receptor antagonist nor-BNI attenuated 030418-induced antinociception. In contrast, the ORL1 receptor antagonist J-113397 enhanced the antinociceptive effect of 030418. Additionally, chronic treatment with 030418 resulted in a dramatic development of tolerance that could not be effectively prevented by J-113397. In guinea pig ileum preparation, the existing action of 030418 could be removed with difficulty after prolonged washing. Conclusion:The compound 030418 is a novel agonist of opioid receptors with high efficiency, long-lasting effect and liability to tolerance, which may be closely correlated with the methyl group at the N 17 position and the high hydrophobicity of the C 7 -thiophene group in its chemical structure.

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“…Enhanced activities of anti-opioid neurons are suggested to be involved in the development of tolerance to central morphine. There are several antiopioid neuronal systems in the central nervous system, such as cholecystokinin (34), neuropeptide FF (35), and nociceptin systems (36). Since a complicated neuronal network is not present in the peripheral nervous system, peripheral opioid analgesia may be resistant to the development of tolerance.…”

Section: Discussionmentioning

confidence: 99%

Effects of Loperamide on Mechanical Allodynia Induced by Herpes Simplex Virus Type-1 in Mice

Sasaki¹,

Nakashima²,

Takasaki³

et al. 2007

J Pharmacol Sci

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Abstract. In the present study, we investigated whether the peripherally acting µ-opioid receptor agonist loperamide would inhibit allodynia in the non-inflamed dermatome of mice with herpetic pain. Subcutaneous (s.c.) injection of loperamide (1 and 3 mg / kg) inhibited allodynia. Local (intraplantar) injection of loperamide (1 and 5 µg / site) also produced an anti-allodynic effect. The peripheral opioid receptor antagonist naloxone methiodide (0.1 mg / kg, s.c.) and the µ-opioid receptor-selective antagonist β-funaltrexamine (40 nmol / site, intraplantar and 20 mg / kg, s.c.) antagonized the anti-allodynic effects of systemic and local loperamide. Local injection of loperamide into the contralateral hind paw was without effect, suggesting that the effect is mediated through local action, not systemic action. Acute and subacute tolerance did not develop to the anti-allodynic effect of loperamide. In addition, there were no cross-tolerance between local opioids (morphine and loperamide) and systemic morphine. These results suggest that stimulation of peripheral µ-opioid receptors suppresses herpetic allodynia without tolerance development. The non-narcotic µ-opioid receptor agonist loperamide may relieve acute herpetic pain in patients with herpes zoster.

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Endogenous Orphanin FQ/Nociceptin Is Involved in the Development of Morphine Tolerance

Cited by 64 publications

References 38 publications

Endogenous Nociceptin (Orphanin FQ) Suppresses Basal Hedonic State and Acute Reward Responses to Methamphetamine and Ethanol, but Facilitates Chronic Responses

Endogenous Nociceptin (Orphanin FQ) Suppresses Basal Hedonic State and Acute Reward Responses to Methamphetamine and Ethanol, but Facilitates Chronic Responses

Pharmacological mechanisms underlying the antinociceptive and tolerance effects of the 6,14-bridged oripavine compound 030418

Effects of Loperamide on Mechanical Allodynia Induced by Herpes Simplex Virus Type-1 in Mice

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