Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity

Morphine and structurally related derivatives are highly effective analgesics, and the mainstay in the medical management of moderate to severe pain. Pharmacological actions of opioid analgesics are primarily mediated through agonism at the µ opioid peptide (MOP) receptor, a G protein-coupled recept...

Descripción completa

Detalles Bibliográficos
Autores principales: Ben Haddou, Tanila, Béni, Szabolcs, Hosztafi, Sándor, Malfacini, Davide, Calo, Girolamo, Schmidhammer, Helmut, Spetea, Mariana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4053365/
https://www.ncbi.nlm.nih.gov/pubmed/24919067
http://dx.doi.org/10.1371/journal.pone.0099231
_version_ 1782320366321926144
author Ben Haddou, Tanila
Béni, Szabolcs
Hosztafi, Sándor
Malfacini, Davide
Calo, Girolamo
Schmidhammer, Helmut
Spetea, Mariana
author_facet Ben Haddou, Tanila
Béni, Szabolcs
Hosztafi, Sándor
Malfacini, Davide
Calo, Girolamo
Schmidhammer, Helmut
Spetea, Mariana
author_sort Ben Haddou, Tanila
collection PubMed
description Morphine and structurally related derivatives are highly effective analgesics, and the mainstay in the medical management of moderate to severe pain. Pharmacological actions of opioid analgesics are primarily mediated through agonism at the µ opioid peptide (MOP) receptor, a G protein-coupled receptor. Position 17 in morphine has been one of the most manipulated sites on the scaffold and intensive research has focused on replacements of the 17-methyl group with other substituents. Structural variations at the N-17 of the morphinan skeleton led to a diversity of molecules appraised as valuable and potential therapeutics and important research probes. Discovery of therapeutically useful morphine-like drugs has also targeted the C-6 hydroxyl group, with oxymorphone as one of the clinically relevant opioid analgesics, where a carbonyl instead of a hydroxyl group is present at position 6. Herein, we describe the effect of N-substituent variation in morphine and oxymorphone on in vitro and in vivo biological properties and the emerging structure-activity relationships. We show that the presence of a N-phenethyl group in position 17 is highly favorable in terms of improved affinity and selectivity at the MOP receptor, potent agonism and antinociceptive efficacy. The N-phenethyl derivatives of morphine and oxymorphone were very potent in stimulating G protein coupling and intracellular calcium release through the MOP receptor. In vivo, they were highly effective against acute thermal nociception in mice with marked increased antinociceptive potency compared to the lead molecules. It was also demonstrated that a carbonyl group at position 6 is preferable to a hydroxyl function in these N-phenethyl derivatives, enhancing MOP receptor affinity and agonist potency in vitro and in vivo. These results expand the understanding of the impact of different moieties at the morphinan nitrogen on ligand-receptor interaction, molecular mode of action and signaling, and may be instrumental to the development of new opioid therapeutics.
format Online
Article
Text
id pubmed-4053365
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-40533652014-06-18 Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity Ben Haddou, Tanila Béni, Szabolcs Hosztafi, Sándor Malfacini, Davide Calo, Girolamo Schmidhammer, Helmut Spetea, Mariana PLoS One Research Article Morphine and structurally related derivatives are highly effective analgesics, and the mainstay in the medical management of moderate to severe pain. Pharmacological actions of opioid analgesics are primarily mediated through agonism at the µ opioid peptide (MOP) receptor, a G protein-coupled receptor. Position 17 in morphine has been one of the most manipulated sites on the scaffold and intensive research has focused on replacements of the 17-methyl group with other substituents. Structural variations at the N-17 of the morphinan skeleton led to a diversity of molecules appraised as valuable and potential therapeutics and important research probes. Discovery of therapeutically useful morphine-like drugs has also targeted the C-6 hydroxyl group, with oxymorphone as one of the clinically relevant opioid analgesics, where a carbonyl instead of a hydroxyl group is present at position 6. Herein, we describe the effect of N-substituent variation in morphine and oxymorphone on in vitro and in vivo biological properties and the emerging structure-activity relationships. We show that the presence of a N-phenethyl group in position 17 is highly favorable in terms of improved affinity and selectivity at the MOP receptor, potent agonism and antinociceptive efficacy. The N-phenethyl derivatives of morphine and oxymorphone were very potent in stimulating G protein coupling and intracellular calcium release through the MOP receptor. In vivo, they were highly effective against acute thermal nociception in mice with marked increased antinociceptive potency compared to the lead molecules. It was also demonstrated that a carbonyl group at position 6 is preferable to a hydroxyl function in these N-phenethyl derivatives, enhancing MOP receptor affinity and agonist potency in vitro and in vivo. These results expand the understanding of the impact of different moieties at the morphinan nitrogen on ligand-receptor interaction, molecular mode of action and signaling, and may be instrumental to the development of new opioid therapeutics. Public Library of Science 2014-06-11 /pmc/articles/PMC4053365/ /pubmed/24919067 http://dx.doi.org/10.1371/journal.pone.0099231 Text en © 2014 Ben Haddou et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Ben Haddou, Tanila
Béni, Szabolcs
Hosztafi, Sándor
Malfacini, Davide
Calo, Girolamo
Schmidhammer, Helmut
Spetea, Mariana
Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity
title Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity
title_full Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity
title_fullStr Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity
title_full_unstemmed Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity
title_short Pharmacological Investigations of N-Substituent Variation in Morphine and Oxymorphone: Opioid Receptor Binding, Signaling and Antinociceptive Activity
title_sort pharmacological investigations of n-substituent variation in morphine and oxymorphone: opioid receptor binding, signaling and antinociceptive activity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4053365/
https://www.ncbi.nlm.nih.gov/pubmed/24919067
http://dx.doi.org/10.1371/journal.pone.0099231
work_keys_str_mv AT benhaddoutanila pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity
AT beniszabolcs pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity
AT hosztafisandor pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity
AT malfacinidavide pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity
AT calogirolamo pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity
AT schmidhammerhelmut pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity
AT speteamariana pharmacologicalinvestigationsofnsubstituentvariationinmorphineandoxymorphoneopioidreceptorbindingsignalingandantinociceptiveactivity

Ejemplares similares