Synthesis, Opioid Receptor Binding, and Biological Activities of Naltrexone-Derived Pyrido- and Pyrimidomorphinans

Ananthan, Subramaniam; Kezar, Hollis S.; Carter, Ronald L.; Saini, Surendra Kumar; Rice, Kenner C.; Wells, J. H.; Davis, Peg; Xu, Heng; Dersch, Christina M.; Bilsky, Edward J.; Porreca, Frank; Rothman, Richard B.

doi:10.1021/jm990039i

Cited by 75 publications

(73 citation statements)

References 43 publications

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“…1A), where TFL in mice treated with 1 bolus of the highest doses remained above baseline levels for 180 minutes. The calculated intracerebroventricular A 50 was 0.93 mg [95% confidence interval (CI) 5 0.62-1.39 mg] in mice, similar to the published data for morphine (A 50 5 0.68 mg, 95% CI 5 0.51-0.92 mg; Ananthan et al, 1999).…”

Section: Ty027 Produces Antinociception In Noninjured Animalssupporting

confidence: 85%

Building a Better Analgesic: Multifunctional Compounds that Address Injury-Induced Pathology to Enhance Analgesic Efficacy while Eliminating Unwanted Side Effects

Largent-Milnes

Brookshire

Skinner

et al. 2013

J Pharmacol Exp Ther

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The most highly abused prescription drugs are opioids used for the treatment of pain. Physician-reported drug-seeking behavior has resulted in a significant health concern among doctors trying to adequately treat pain while limiting the misuse or diversion of pain medications. In addition to abuse liability, opioid use is associated with unwanted side effects that complicate pain management, including opioid-induced emesis and constipation. This has resulted in restricting long-term doses of opioids and inadequate treatment of both acute and chronic debilitating pain, demonstrating a compelling need for novel analgesics. Recent reports indicate that adaptations in endogenous substance P/neurokinin-1 receptor (NK 1 ) are induced by chronic pain and sustained opioid exposure, and these changes may contribute to processes responsible for opioid abuse liability, emesis, and analgesic tolerance. Here, we describe a multifunctional mu-/delta-opioid agonist/NK 1 antagonist compound [Tyr-D-Ala-Gly-Phe-Met-Pro-Leu-Trp-NH-Bn(CF 3 ) 2 (TY027)] that has a preclinical profile of excellent antinociceptive efficacy, low abuse liability, and no opioid-related emesis or constipation. In rodent models of acute and neuropathic pain, TY027 demonstrates analgesic efficacy following central or systemic administration with a plasma half-life of more than 4 hours and central nervous system penetration. These data demonstrate that an innovative opioid designed to contest the pathology created by chronic pain and sustained opioids results in antinociceptive efficacy in rodent models, with significantly fewer side effects than morphine. Such rationally designed, multitargeted compounds are a promising therapeutic approach in treating patients who suffer from acute and chronic pain.

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Section: Ty027 Produces Antinociception In Noninjured Animalssupporting

confidence: 85%

Building a Better Analgesic: Multifunctional Compounds that Address Injury-Induced Pathology to Enhance Analgesic Efficacy while Eliminating Unwanted Side Effects

Largent-Milnes

Brookshire

Skinner

et al. 2013

J Pharmacol Exp Ther

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“…However, clinical trials of naltrexone treatment for alcohol dependence study doses up to 100 mg. Naltrexone, at 25 mg, should have produced a nearly complete blockade of m-opiate receptors (Lee et al, 1988). But, it is possible that higher naltrexone doses would have produced greater effects via d-or k-opiate receptors, where it has nearly 16.7-fold and 5.6-fold lower affinity, respectively (Ananthan et al, 1999). Second, this study was conducted in healthy human subjects without a family history of alcohol dependence.…”

Section: Discussionmentioning

confidence: 99%

Potentiation of Low Dose Ketamine Effects by Naltrexone: Potential Implications for the Pharmacotherapy of Alcoholism

Krystal

Madonick

Perry

et al. 2006

Neuropsychopharmacol

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The interplay of opiate and NMDA glutamate receptors may contribute to psychosis, cognitive function, alcoholism, and substance dependence. Ketamine and ethanol block the NMDA glutamate receptor. The purpose of this randomized double-blind, placebocontrolled human laboratory study was to evaluate whether the interactive effects of drugs acting at opiate and NMDA glutamate receptors might partially explain the efficacy of naltrexone for the treatment of alcoholism, that is, whether naltrexone 25 mg pretreatment would modulate ketamine effects in healthy human subjects. Two groups of healthy subjects were studied. An initial group (n ¼ 31) received a perception-altering subanesthetic dose of ketamine (bolus of 0.23 mg/kg over 1 min followed by a 60-min infusion of 0.58 mg/kg or saline bolus and infusion). A second group (n ¼ 24) completed the same testing procedures, but received a subperceptual ketamine dose (bolus 0.081 mg/kg over 10 min followed by an infusion of 0.4 mg/kg/h). Ketamine produced positive symptoms, negative symptoms, emotional discomfort, and cognitive effects as measured by the Positive and Negative Syndrome Scale (PANSS) in a doserelated fashion. The lower ketamine dose produced subjective effects similar to two standard ethanol drinks, whereas the higher ketamine dose produced effects similar to five standard drinks. Although naltrexone produced no significant behavioral effects, it significantly magnified the increase in the total PANSS score produced by the lower subperceptual dose of ketamine, but not the higher perception-altering dose of ketamine. These data suggest that the interplay of opiate receptor antagonism and NMDA receptor antagonism may be relevant to the protective effects of naltrexone on alcohol consumption via potentiation of dysphoric effects associated with the NMDA receptor antagonist effects of ethanol. However, these data suggest that at levels of NMDA receptor antagonism associated with heavy drinking, this protective effect of naltrexone on drinking is no longer present.

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“…Detailed on-line protocols are available for all assays at the NIMH-PDSP web site (http:͞͞pdsp.cwru.edu). opioid radioligand-binding assays in situ in guinea pig brain and opioid receptor (MOR)-and ␦ opioid receptor (DOR)-binding assays in rat brain were performed as previously detailed (11). Initial screening assays were performed by using 10 M Salvinorin A or 10 M LSD by using quadruplicate determinations and the percent inhibition of specific binding determined.…”

Section: Methodsmentioning

confidence: 99%

Salvinorin A: A potent naturally occurring nonnitrogenous κ opioid selective agonist

Roth

Baner

Westkaemper

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

736

739

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Salvia divinorum, whose main active ingredient is the neoclerodane diterpene Salvinorin A, is a hallucinogenic plant in the mint family that has been used in traditional spiritual practices for its psychoactive properties by the Mazatecs of Oaxaca, Mexico. More recently, S. divinorum extracts and Salvinorin A have become more widely used in the U.S. as legal hallucinogens. We discovered that Salvinorin A potently and selectively inhibited 3 H-bremazocine binding to cloned opioid receptors. Salvinorin A had no significant activity against a battery of 50 receptors, transporters, and ion channels and showed a distinctive profile compared with the prototypic hallucinogen lysergic acid diethylamide. Functional studies demonstrated that Salvinorin A is a potent opioid agonist at cloned opioid receptors expressed in human embryonic kidney-293 cells and at native opioid receptors expressed in guinea pig brain. Importantly, Salvinorin A had no actions at the 5-HT 2A serotonin receptor, the principal molecular target responsible for the actions of classical hallucinogens. Salvinorin A thus represents, to our knowledge, the first naturally occurring nonnitrogenous opioid-receptor subtype-selective agonist. Because Salvinorin A is a psychotomimetic selective for opioid receptors, opioid-selective antagonists may represent novel psychotherapeutic compounds for diseases manifested by perceptual distortions (e.g., schizophrenia, dementia, and bipolar disorders). Additionally, these results suggest that opioid receptors play a prominent role in the modulation of human perception.

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Synthesis, Opioid Receptor Binding, and Biological Activities of Naltrexone-Derived Pyrido- and Pyrimidomorphinans

Cited by 75 publications

References 43 publications

Building a Better Analgesic: Multifunctional Compounds that Address Injury-Induced Pathology to Enhance Analgesic Efficacy while Eliminating Unwanted Side Effects

Building a Better Analgesic: Multifunctional Compounds that Address Injury-Induced Pathology to Enhance Analgesic Efficacy while Eliminating Unwanted Side Effects

Potentiation of Low Dose Ketamine Effects by Naltrexone: Potential Implications for the Pharmacotherapy of Alcoholism

Salvinorin A: A potent naturally occurring nonnitrogenous κ opioid selective agonist

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