Your search keyword '"Naltrexone metabolism"' showing total 20 results

1. Naltrexone protects against BDL-induced cirrhosis in Wistar rats by attenuating thrombospondin-1 and enhancing antioxidant defense system via Nrf-2.

Author

Hosseini-Fard SR, Dehpour AR, Emamgholipour S, and Golestani A

Subjects

Animals, Antioxidants metabolism, Antioxidants pharmacology, Bile Ducts metabolism, Ligation, Liver metabolism, Liver Cirrhosis pathology, Male, NADPH Oxidase 1 metabolism, Naltrexone metabolism, Naltrexone pharmacology, Necrosis metabolism, Rats, Rats, Wistar, Thrombospondin 1 metabolism, Transforming Growth Factor beta1 metabolism, Vascular Endothelial Growth Factor A metabolism

Abstract

Aims: It is well-established that thrombospondin-1 (THBS-1), vascular endothelial growth factor-A (VEGF-A), nuclear factor-erythroid 2-related factor 2 (Nrf-2), Kelch-like ECH-associated protein 1 (Keap-1), and transforming growth factor-beta 1 (TGF-β1) are the pivotal players of liver fibrosis. Recent studies have shown that endogenous opioid levels increase during liver cirrhosis. Therefore, the present study aimed to clarify the effect of naltrexone (NTX), an opioid antagonist, on the alteration of these factors following bile duct ligation (BDL)-induced liver cirrhosis., Main Methods: Wistar male rats (n = 50) were categorized equally into 5 groups (baseline, sham+saline, BDL + saline, sham+NTX (10 mg/kg of body weight (BW)), and BDL + NTX (10 mg/kg of BW)). At the end of the experiment, H&E staining was used to assess necrosis and lobular damage of hepatic tissue. The gene expression of THBS-1 and NADPH oxidase 1 (NOX-1) was measured by real time-PCR and VEGF-A, Nrf-2, Keap-1, and TGF-β1 protein levels were assessed by western blot. The antioxidant enzymes activity, total oxidant status (TOS) and MDA level were measured by commercial kits., Key Findings: Hepatic necrosis and lobular damage increased substantially and NTX reduced them markedly in the BDL group. Gene expression of hepatic THBS-1 and NOX-1, TOS and MDA levels increased markedly in the BDL + saline group, and Nrf-2 and VEGF-A values decreased significantly in the BDL + NTX group. NTX recovered THBS-1, NOX-1 and Nrf-2 in the BDL + NTX group, substantially (p-value ≤ 0.05)., Significance: Data showed that NTX treatment attenuates liver fibrosis mainly by lowering THBS-1 and NOX-1 and increasing Nrf-2 protein level and antioxidant enzymes., (Copyright © 2022. Published by Elsevier Inc.)

Published

2022

2. Preventive effects of naldemedine, peripherally acting μ-opioid receptor antagonist, on morphine-induced nausea and vomiting in ferrets.

Author

Kanemasa T, Matsuzaki T, Koike K, Hasegawa M, and Suzuki T

Subjects

Analgesics, Opioid administration & dosage, Animals, Constipation chemically induced, Ferrets, Male, Morphine adverse effects, Naltrexone metabolism, Naltrexone pharmacology, Narcotic Antagonists pharmacology, Receptors, Opioid, mu antagonists & inhibitors, Vomiting chemically induced, Naltrexone analogs & derivatives, Nausea drug therapy

Abstract

Aims: Naldemedine is a peripherally acting μ-opioid receptor antagonists (PAMORAs) indicated for the treatment of opioid-induced constipation (OIC). We investigated the preventive effect of naldemedine on morphine-induced nausea and vomiting in ferrets and conducted a pharmacokinetic/pharmacodynamic (PK/PD) analysis., Main Methods: The antiemetic effect of naldemedine was evaluated as the frequency and time of retching (rhythmic abdominal contractile motion) and vomiting (throwing up vomit or similar reactions) caused by morphine in ferrets. After a single oral administration of naldemedine to ferrets, the plasma concentrations of naldemedine and morphine were measured by liquid chromatography-tandem mass spectrometry., Key Findings: Naldemedine showed a potent and dose-dependent anti-emetic effects against morphine-induced emetic responses, for up to 6 h. The dose of naldemedine that produced half the maximal effect (ED 50 ) value for anti-emetic effect of naldemedine in the morphine-treated ferrets was 0.033 mg/kg. The PK/PD analysis revealed that the antiemetic effect was related to the plasma naldemedine concentration, with a half maximal effective concentration that produces half the maximal effect (EC 50 ) of 3.51 ng/mL. The plasma concentration producing an antiemetic effect was almost 200-fold lower than that inducing an anti-analgesic effect in rats., Significance: Naldemedine showed potent inhibition of morphine-induced vomiting for up to 6 h after dosing. These data suggest that naldemedine possesses antiemetic properties and could be effective against opioid-induced nausea and vomiting (OINV)., Competing Interests: Declaration of competing interest Some of the authors (TK, KK, MH, TM) are employee of Shionogi & Co., Ltd., a manufacture of naldemedine. TS has received funding from Shionogi & Co., Ltd., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

3. Binding, pharmacological and immunological profiles of the delta-selective opioid receptor antagonist HS 378.

Author

Spetea M, Harris HE, Berzetei-Gurske IP, Klareskog L, and Schmidhammer H

Subjects

Animals, Brain metabolism, Cells, Cultured, Guanosine 5'-O-(3-Thiotriphosphate) metabolism, Immunosuppressive Agents metabolism, Immunosuppressive Agents pharmacology, Rats, Rats, Sprague-Dawley, Receptors, Opioid, delta metabolism, T-Lymphocytes drug effects, T-Lymphocytes immunology, Lymphocyte Activation drug effects, Naltrexone analogs & derivatives, Naltrexone metabolism, Naltrexone pharmacology, Narcotic Antagonists metabolism, Narcotic Antagonists pharmacology, Receptors, Opioid, delta antagonists & inhibitors

Abstract

HS 378 is a recently developed indolomorphinan with high selectivity and antagonist potency at the delta-opioid receptor. The present study was performed to characterize the opioid binding properties and pharmacological and immunological activity of HS 378 and to compare them with those of two well-known delta-opioid receptor antagonists, naltrindole (NTI) and naltriben (NTB). In vitro opioid receptor binding profiles were determined in rat brain homogenates. HS 378 showed 4.7- and 2.4-fold higher mu/delta selectivity compared to NTI and NTB, respectively. In the [35S]GTPgammaS functional assay carried out in cell lines expressing cloned human opioid receptors, HS 378 was found to be a pure delta-opioid receptor antagonist. In vitro, exposure of HS 378 resulted in an apparent dose-related suppression of concanavalin A induced rat T-lymphocyte proliferation with an IC50 value of 0.54 microM. NTI showed also immunosuppression with an IC50 value of 6.93 microM, whereas NTB had no effect. The IC50 of HS 378 was 13 times lower than that of NTI and 8 times higher than that of cyclosporin A. Taken together, our findings indicate that the small molecule HS 378 has properties that may be of therapeutic value in the setting of human inflammatory diseases.

Published

2001

4. [125I-Tyr1]biphalin binding to opioid receptors of rat brain and NG108-15 cell membranes.

Author

Slaninova J, Appleyard SM, Misicka A, Lipkowski AW, Knapp RJ, Weber SJ, Davis TP, Yamamura HI, and Hruby VJ

Subjects

Animals, Cell Line, Cell Membrane metabolism, Iodine Radioisotopes, Morphine metabolism, Naltrexone analogs & derivatives, Naltrexone metabolism, Narcotic Antagonists metabolism, Oligopeptides metabolism, Radioligand Assay, Rats, Brain metabolism, Enkephalins metabolism, Receptors, Opioid metabolism

Abstract

Mono iodinated analogues of biphalin [(Tyr-D-Ala-Gly-Phe-NH-)2], both nonradioactive [I-Tyr1]biphalin and radioactive [125I-Tyr1]biphalin have been synthesized. The radioligand binding profiles of these compounds for two types of tissues, rat brain membranes, and NG108-15 cell membranes were identical to the parent biphalin. This is additional evidence for the hypothesis that biphalin behaves like a monomeric ligand and that only one intact tyrosine is necessary for high biological activity. The second tyrosine could be used for successful radioiodination which may greatly simplify biochemical and pharmacological studies of biphalin. The results of receptor binding studies show that the binding of both biphalin and [I-Tyr1]biphalin to the delta and mu opioid receptors are not independent. [125I-Tyr1]Biphalin binds to delta receptors as shown in NG108-15 cell membranes. Nevertheless, [125I]biphalin binding to delta receptors in rat brain membranes was hardly evident and mu receptor binding predominated or at least was much more readily detectable in this preparation.

Published

1998

5. In vivo labeling of delta opioid receptors in mouse brain by [3H]benzylidenenaltrexone, a ligand selective for the delta 1 subtype.

Author

Lever JR, Stathis M, Kinter CM, and Scheffel U

Subjects

Animals, Benzylidene Compounds pharmacokinetics, Corpus Striatum metabolism, Male, Mice, Naltrexone metabolism, Naltrexone pharmacokinetics, Naltrexone pharmacology, Radioligand Assay, Receptors, Opioid, delta antagonists & inhibitors, Receptors, Opioid, delta drug effects, Tritium, Benzylidene Compounds metabolism, Naltrexone analogs & derivatives, Receptors, Opioid, delta metabolism

Abstract

(E)-7-Benzylidenenaltrexone (BNTX) is a selective ligand for the putative delta 1 (delta 1) opioid receptor. To explore the feasibility of labeling delta 1 sites in vivo; we determined the cerebral distribution of radioactivity after systemic administration of [3H]BNTX to CD1 mice. Uptake was highest in striatum and lowest in cerebellum throughout the 4 hr time course. Specific radioligand binding, approximated as the difference in radioactivity concentrations between striatum and cerebellum, peaked at 0.32 percent injected dose/g at 30 min and comprised a modest 23% of total striatal radioactivity. For seven brain regions, radioactivity concentrations correlated with delta site densities known from prior in vitro studies (rS = 0.79, p = 0.03), and also with the uptake of N1'-([11C]methyl)naltrindole in vivo (rS = 0.78, p = 0.04) in mice. Specific binding in striatum, olfactory tubercles and cortical regions was saturable by BNTX, and was inhibited stereoselectively by the optical isomers of naloxone. Naltrindole and naltriben (NTB), delta antagonists, blocked 65-99% of [3H]BNTX specific binding at a dosage of 5.0 mumol/kg. Similar doses of the mu antagonist cyprodime, or the kappa agonist U50,488H, did not inhibit binding. Adjusted for the four-fold greater brain penetration of NTB relative to BNTX, dose-response studies suggested that delta 1 selective BNTX (ED50 = 1.51 mumol/kg) was 50% more potent than delta 2 selective NTB (ED50 = 0.56 mumol/kg) in blocking specific [3H]BNTX binding in striatum. In CXBK mice, a strain with functional delta 1 but not delta 2 receptors in antinociceptive assays, radioligand uptake and distribution proved similar to that in CD1 mice. In sum, [3H]BNTX labels murine delta opioid receptors in vivo with a low extent of specific binding. The data is consistent with, but not conclusive for, selective labeling of the delta 1 subtype.

Published

1996

6. Identification of a human delta opioid receptor: cloning and expression.

Author

Knapp RJ, Malatynska E, Fang L, Li X, Babin E, Nguyen M, Santoro G, Varga EV, Hruby VJ, and Roeske WR

Subjects

Amino Acid Sequence, Animals, Base Sequence, Cell Line, Consensus Sequence, Enkephalins metabolism, Humans, Mice, Molecular Sequence Data, Naltrexone analogs & derivatives, Naltrexone metabolism, Narcotic Antagonists metabolism, Oligopeptides metabolism, Open Reading Frames, Receptors, Opioid, delta chemistry, Receptors, Opioid, delta metabolism, Sequence Alignment, Transfection, Cloning, Molecular, Receptors, Opioid, delta genetics

Abstract

The delta opioid receptor is an important target for analgesic drug development. This report describes the identification of delta opioid receptor clones from human cDNA libraries and the preparation of a human delta receptor cDNA in the pcDNA3 expression vector for transfection studies. The cDNA encodes a 372 amino acid protein that has 93% amino acid identity to mouse and rat delta receptors. COS-7 cells transfected with this clone express over 1.0 pmol receptor/mg protein when measured by saturation binding with [3H]naltrindole. The delta receptor selective ligands NTB, BNTX, [4'-Cl-Phe4]DPDPE and [D-Ala2,Glu4]deltorphin all have Ki values under 10 nM while the affinities of the mu and kappa opioid receptor ligands CTAP and U-69593, respectively, are over 4.0 microM. Agonists show binding to multiple affinity states of the receptor consistent with the presence of G-protein coupled and uncoupled forms of the expressed receptor. The 8-fold higher affinity of NTB relative to BNTX suggests that the human delta receptor is of the delta 2 subtype.

Published

1994

7. Opiate antagonist binding sites in discrete brain regions of spontaneously hypertensive and normotensive Wistar-Kyoto rats.

Author

Rahmani NH, Gulati A, and Bhargava HN

Subjects

Animals, Binding Sites, Naltrexone pharmacokinetics, Narcotic Antagonists pharmacokinetics, Rats, Rats, Inbred Strains, Spinal Cord metabolism, Tissue Distribution, Brain metabolism, Naltrexone metabolism, Narcotic Antagonists metabolism

Abstract

The binding of 3H-naltrexone, an opiate receptor antagonist, to membranes of discrete brain regions and spinal cord of 10 week old spontaneously hypertensive (SHR) and normotensive Wistar-Kyoto (WKY) rats was determined. The brain regions examined were hypothalamus, amygdala, hippocampus, corpus striatum, pons and medulla, midbrain and cortex. 3H-Naltrexone bound to membranes of brain regions and spinal cord at a single high affinity site with an apparent dissociation constant value of 3 nM. The highest density of 3H-naltrexone binding sites were in hippocampus and lowest in the cerebral cortex. The receptor density (Bmax value) and apparent dissociation constant (Kd value) values of 3H-naltrexone to bind to opiate receptors on the membranes of amygdala, hippocampus, corpus striatum, pons and medulla, midbrain, cortex and spinal cord of WKY and SHR rats did not differ. The Bmax value of 3H-naltrexone binding to membranes of hypothalamus of SHR rats was 518% higher than WKY rats but the Kd values in the two strains did not differ. It is concluded that SHR rats have higher density of opiate receptors labeled with 3H-naltrexone in the hypothalamus only, in comparison with WKY rats, and that such a difference in the density of opiate receptors may be related to the elevated blood pressure in SHR rats.

Published

1991

8. Seasonal variation in the apparent number of binding sites for 3H-opioid agonists and antagonists.

Author

Codd EE and Byrne WL

Subjects

Animals, Binding Sites, Dihydromorphine metabolism, Female, Kinetics, Male, Mice, Morphine metabolism, Naloxone metabolism, Naltrexone metabolism, Brain metabolism, Endorphins metabolism, Enkephalin, Methionine analogs & derivatives, Enkephalins metabolism, Morphinans metabolism, Receptors, Opioid physiology, Seasons

Published

1981

9. Testosterone does not influence opiate binding sites in the male rat brain.

Author

Cicero TJ, Newman KS, and Meyer ER

Subjects

Alanine metabolism, Animals, Dihydromorphine metabolism, Hypothalamus metabolism, Male, Naltrexone metabolism, Rats, Receptors, Opioid drug effects, Brain metabolism, Castration, Receptors, Opioid metabolism, Testosterone pharmacology

Abstract

It has been reported previously that castration produces testosterone-reversible increases in the density of 3H-naltrexone binding sites in the male rat brain. Unfortunately, we were unable to replicate these observations in a comprehensive series of studies. Specifically, we found that castration failed to produce changes in the Kd or Bmax of opiate binding sites in whole male rat brain, or in the hypothalamus, utilizing 3H-dihydromorphine (a mu receptor ligand), 3H-D-alanine, D-leucine enkephalin (delta) or 3H-naltrexone (ubiquitous). Furthermore, we found that the relative proportion of mu and delta binding sites in brain was unchanged by castration. The reasons for the discrepancy between the present results and those previously reported are unclear, but it appears that the provocative hypothesis that testosterone influences opioid receptors in brain must be carefully reevaluated.

Published

1983

10. Ethanol inhibits the naloxone-induced release of luteinizing hormone-releasing hormone from the hypothalamus of the male rat.

Author

Cicero TJ, Newman KS, Gerrity M, Schmoeker PF, and Bell RD

Subjects

Animals, Cell Membrane metabolism, Dose-Response Relationship, Drug, Drug Antagonism, Gonadotropin-Releasing Hormone pharmacology, Hypothalamus drug effects, Male, Naloxone metabolism, Naltrexone metabolism, Pituitary Gland drug effects, Rats, Rats, Inbred Strains, Ethanol pharmacology, Gonadotropin-Releasing Hormone metabolism, Hypothalamus metabolism, Luteinizing Hormone blood, Naloxone pharmacology

Abstract

It has been inferred that ethanol suppresses the secretion of luteinizing hormone (LH) in the male by depressing the release of LH-releasing hormone (LH-RH) from the hypothalamus. Direct support for this inference has been difficult to obtain, however, because of significant technical difficulties in measuring LH-RH release under in vivo conditions. To circumvent these problems, we made use of the opiate antagonist naloxone, as a neuroendocrine probe, to elicit the release of LH-RH under in vivo conditions. We found that ethanol was a potent suppressor of the increase in serum LH levels evoked by naloxone at extremely low blood ethanol concentrations ( less than 60 mg/dl). Furthermore, we observed that the antagonism between ethanol and naloxone appeared to be competitive in nature since a fixed dose of ethanol (1 g/kg, blood ethanol concentration 60 mg/dl) shifted the naloxone dose-response curve significantly to the right and high doses of the antagonist overcame ethanol's effects. Finally, we found that the interaction between ethanol and naloxone took place at the level of the hypothalamus. Our results, therefore, seem to provide the first in vivo evidence supporting the widely-held hypothesis that ethanol reduces serum LH levels by depressing the hypothalamically-medicated release of LH-RH. The mechanisms underlying ethanol's depression of naloxone-induced increases in the release of LH-RH are not fully understood at this time, but one prominent possibility is that ethanol enhances the synthesis or release of endogenous opioids which in turn override naloxone's effects.

Published

1982

11. Isolation of selective 3H-chlornaltrexamine-bound complexes, possible opioid receptor components in brains of mice.

Author

Caruso TP, Larson DL, Portoghese PS, and Takemori AE

Subjects

Animals, Chromatography, Gel, Dextrorphan pharmacology, In Vitro Techniques, Mice, Naltrexone metabolism, Naltrexone pharmacology, Nitrogen Mustard Compounds metabolism, Receptors, Opioid isolation & purification, Brain metabolism, Naloxone analogs & derivatives, Naltrexone analogs & derivatives, Receptors, Opioid metabolism

Published

1980

12. Lack of effect of the opioid antagonist, naltrexone, on the in situ growth of C-1300, N1E-115 and NS206 murine neuroblastoma tumor cell lines.

Author

Horn PT and Mirkin BL

Subjects

Animals, Body Weight, Chi-Square Distribution, Endorphins antagonists & inhibitors, Male, Mice, Mice, Inbred A, Naltrexone metabolism, Neoplasm Transplantation, Neoplasms, Experimental, Neuroblastoma metabolism, Receptors, Opioid metabolism, Tumor Cells, Cultured, Endorphins metabolism, Naltrexone pharmacology, Neuroblastoma drug therapy

Abstract

Attempts have been made to confirm previously reported results which demonstrated that the opioid antagonist, naltrexone, altered the in situ growth of murine neuroblastoma tumors. Adult male A/J mice were injected with tumor cells from three different cell lines of murine neuroblastoma; the spontaneously arising C-1300 line, the adrenergic clonal line N1E-115, and the cholinergic clonal line NS20Y. Naltrexone was administered daily in doses of 0.1, 0.4, or 10.0 mg/kg subcutaneously, to replicate the reported experimental design. In contrast to previous studies, we were unable to demonstrate any effect of naltrexone on in situ growth or other characteristics of tumors produced by the C-1300, N1E-115 or NS20Y murine neuroblastoma cell lines. Ligand binding studies have demonstrated the presence of high levels of opiate binding sites on membranes prepared from the NS20Y clonal cell line and low levels on the membranes of the C1300 tumor line.

Published

1989

13. Oxymorphone-naltrexonazine, a mixed opiate agonist-antagonist.

Author

Galetta S, Hahn EF, Nishimura S, and Pasternak GW

Subjects

Analgesia, Animals, Binding, Competitive, Brain metabolism, Dihydromorphine antagonists & inhibitors, Dihydromorphine metabolism, Enkephalin, Leucine analogs & derivatives, Enkephalin, Leucine antagonists & inhibitors, Enkephalin, Leucine metabolism, Enkephalin, Leucine-2-Alanine, Male, Mice, Mice, Inbred ICR, Naltrexone chemical synthesis, Naltrexone metabolism, Naltrexone pharmacology, Oxymorphone chemical synthesis, Oxymorphone metabolism, Oxymorphone pharmacology, Rats, Rats, Inbred Strains, Receptors, Opioid drug effects, Sodium pharmacology, Endorphins antagonists & inhibitors, Hydromorphone analogs & derivatives, Naltrexone analogs & derivatives, Oxymorphone analogs & derivatives, Receptors, Opioid metabolism

Abstract

Previous studies from our laboratories have reported the synthesis and pharmacological characteristics of a series of symmetrical opiate azines: naloxonazine, oxymorphonazine and naltrexonazine. We have now synthesized and characterized in binding assays and in vivo two asymmetrical azines: oxymorphone-naltrexonazine and oxymorphone-3-methoxynaltrexonazine. Oxymorphone-naltrexonazine, which theoretically could interact with the receptor as either an agonist or antagonist, displayed antagonist properties in vitro and in vivo. Oxymorphone-3-methoxynaltrexonazine, which theoretically could bind only as an agonist, possessed agonist properties in binding studies and was a potent analgesic in vivo.

Published

1987

14. Inhibition of drug metabolism by chronically administered naltrexone.

Author

Lehman TM, Pyati P, and Peterson GR

Subjects

Animals, Cytochrome P-450 Enzyme System metabolism, Depression, Chemical, Drug Implants, Liver enzymology, Liver metabolism, Male, Mice, Mixed Function Oxygenases metabolism, Naltrexone metabolism, Pharmaceutical Preparations blood, Time Factors, Naloxone analogs & derivatives, Naltrexone pharmacology, Pharmaceutical Preparations metabolism

Published

1979

15. Enhancement of opiate-induced depressions in serum luteinizing hormone levels by the prior administration of naloxone in the male rat.

Author

Cicero TJ, Owens DP, Schmoeker PF, and Meyer ER

Subjects

Animals, Binding, Competitive, Brain metabolism, Dose-Response Relationship, Drug, Gonadotropin-Releasing Hormone pharmacology, Kinetics, Male, Morphine metabolism, Morphine pharmacology, Naltrexone metabolism, Rats, Rats, Inbred Strains, Receptors, Opioid metabolism, Luteinizing Hormone blood, Naloxone pharmacology, Narcotics pharmacology

Abstract

The effects of naloxone pretreatment on opiate agonist-induced depressions in serum luteinizing hormone (LH) levels were examined in male rats. Our results demonstrated a pronounced enhancement of morphine's actions 6 hours after the administration of naloxone (0.5 mg/kg). This effect was characterized by a 10 fold reduction in the ED50 (1.26 mg/kg versus 0.13 mg/kg in saline- and naloxone-pretreated rats, respectively) and much greater depressions in serum LH levels at each dose of morphine. The actions of naloxone were not confined to morphine, since similar increased potencies were found for opioid agonists with selectivity for a variety of opioid receptor subtypes. Because naloxone did not alter the uptake of subsequently administered morphine into brain, our results cannot be explained on the basis of an increased availability of the agonist. Rather, it appears that naloxone pretreatment induces a change in the sensitivity of those receptors involved in the effects of opioid agonists on LH.

Published

1984

16. Selective proliferation of brain kappa opiate receptors in spontaneously hypertensive rats.

Author

Bhargava HN and Das S

Subjects

Animals, Binding, Competitive, Cyclazocine analogs & derivatives, Cyclazocine metabolism, Ethylketocyclazocine, Kinetics, Male, Naltrexone metabolism, Oligopeptides metabolism, Rats, Rats, Inbred WKY, Receptors, Opioid, kappa, Brain metabolism, Enkephalin, Leucine analogs & derivatives, Rats, Inbred SHR metabolism, Rats, Inbred Strains metabolism, Receptors, Opioid metabolism

Abstract

The binding of tritiated ligands for various opiate receptor subtypes to brain membranes prepared from spontaneously hypertensive rats and normotensive Wistar-Kyoto rats was determined. The density (Bmax) or the apparent dissociation constant (Kd) for the binding of the mu-ligand (naltrexone) and delta-ligand (Tyr-D-Ser-Gly-Phe-Leu-Thr) to brain membranes of hypertensive and normotensive rats did not differ. However, the Bmax for the binding of kappa-ligand (ethylketocyclazocine, EKC) to brain membranes after the suppression of mu and delta-sites by 100 nM each of unlabeled D-Ala2-MePhe4-Gly-ol5-enkephalin and D-Ala2-D-Leu5-enkephalin, respectively, was significantly greater in hypertensive rats compared to normotensive rats. The Kd values for the binding of 3H-EKC in the two groups did not differ. The binding of 3H-EKC in brain regions was in the order: hypothalamus greater than midbrain greater than striatum greater than cortex greater than pons + medulla. The increase in the binding of 3H-EKC in the brain of hypertensive rats compared to normotensive rats was due to increased binding in the hypothalamus and cortex. These results provide for the first time evidence of selective proliferation of kappa-opiate receptors in the brain of hypertensive rats, and suggest that brain kappa-opiate receptors may play an important role in the pathophysiology of hypertension.

Published

1986

17. Comparative in vivo distribution of opiate agonists and antagonists by means of double isotope techniques.

Author

Fishman J, Hahn EF, and Norton BI

Subjects

Animals, Autoradiography, Blood-Brain Barrier, Carbon Radioisotopes, Dose-Response Relationship, Drug, Liver metabolism, Male, Morphine blood, Naloxone blood, Naltrexone blood, Naltrexone metabolism, Rats, Time Factors, Tritium, Brain metabolism, Morphine metabolism, Naloxone metabolism

Published

1975

18. Evidence from opiate binding studies that heroin acts through its metabolites.

Author

Inturrisi CE, Schultz M, Shin S, Umans JG, Angel L, and Simon EJ

Subjects

Animals, Cell Membrane metabolism, Heroin pharmacology, Male, Morphine pharmacology, Morphine Derivatives pharmacology, Naltrexone metabolism, Rats, Rats, Inbred Strains, Receptors, Opioid drug effects, Structure-Activity Relationship, Brain metabolism, Heroin metabolism, Receptors, Opioid metabolism

Abstract

The relative affinity to opiate receptors of heroin, 6-acetylmorphine and morphine was estimated by determining their ability to displace specifically bound 3H-naltrexone from rat brain opiate binding sites. In vitro hydrolysis of heroin to 6-acetylmorphine was monitored in the binding assay filtrate by use of a quantitative HPLC procedure. The rate of heroin hydrolysis was significantly slower at 0 degrees C than at 37 degrees C. The displacement of 1 nM 3H-naltrexone by unlabeled ligand at concentrations ranging from 7 to 500 nM was measured at 0 degrees C for 120 minutes, yielding IC50 values of heroin = 483 nM, 6-acetylmorphine = 73 nM and morphine = 53 nM. When the binding data for heroin were recalculated to include the displacement that could be attributed to the 6-acetylmorphine derived from heroin degradation during the incubation, all of the apparent heroin binding was accounted for by the 6-acetylmorphine. These results are consistent with previous reports of the low binding affinity of morphine congeners (e.g., codeine) that lack a free phenolic 3-hydroxyl group and support the view that heroin is a prodrug which serves to determine the distribution of its intrinsically active metabolites, 6-acetylmorphine and morphine.

Published

1983

19. Quaternary derivatives of narcotic antagonists: stereochemical requirements at the chiral nitrogen for in vitro and in vivo activity.

Author

Bianchetti A, Nisato D, Sacilotto R, Dragonetti M, Picerno N, Tarantino A, Manara L, Angel LM, and Simon EJ

Subjects

Animals, Cell Membrane metabolism, Naltrexone metabolism, Nitrogen, Rats, Receptors, Opioid drug effects, Stereoisomerism, Structure-Activity Relationship, Brain metabolism, Narcotic Antagonists pharmacology, Receptors, Opioid metabolism

Abstract

We have studied three pairs of diastereoisomers of quaternary narcotic antagonists and their parent tertiary amines, levallorphan, nalorphine and naloxone, to see how configuration about the chiral nitrogen affects in vitro and in vivo activity. In each series only the diastereoisomer obtained by methylation of the N-allyl substituted tertiary amine (N-methyl diast.) was potent in displacing 3H-naltrexone from rat brain membranes (Ki 10(-8) - 10(-7)M) and as pure morphine antagonist in the guinea-pig ileum (Ki 10(-8)-10(-7)M). Conversely, diastereoisomers obtained by reacting N-methyl substituted tertiary amines with allyl halide (N-allyl diast.) did not displace 3H-naltrexone, up to 10(-6)M, and had negligible antagonist activity and slight agonist action in the guinea-pig ileum. In vivo findings (charcoal meal transit test in mice) were generally consistent with those in vitro. Thus only the N-methyl but not the N-allyl diast. inhibited morphine constipation and behaved as pure antagonists.

Published

1983

20. Opiate receptor: irreversible inactivation by an alkylating local anesthetic.

Author

Craviso GL and Musacchio JM

Subjects

Animals, Binding, Competitive, Kinetics, Levorphanol metabolism, Lidocaine pharmacology, Ligands, Male, Mice, Naltrexone metabolism, Stereoisomerism, Temperature, Alkylating Agents, Brain metabolism, Lidocaine analogs & derivatives, Receptors, Drug drug effects

Published

1976