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Morphine self-administration is inhibited by the antioxidant N‐acetylcysteine and the anti-inflammatory ibudilast; an effect enhanced by their co-administration
by
Quintanilla, María Elena
, Israel, Yedy
, Morales, Paola
, Acuña, Tirso
, Santapau, Daniela
, Riveras, Gabriel
, Ezquer, Fernando
, Gallardo, Javiera
, Rebolledo, Rocío
, Herrera-Marschitz, Mario
in
Acetylcysteine
/ Acetylcysteine - administration & dosage
/ Acetylcysteine - pharmacology
/ Analysis
/ Animal models
/ Animals
/ Anti-inflammatory agents
/ Anti-Inflammatory Agents - administration & dosage
/ Anti-Inflammatory Agents - pharmacology
/ Anti-inflammatory drugs
/ Antioxidants
/ Antioxidants - administration & dosage
/ Antioxidants - pharmacology
/ Astrocytes
/ Biology and Life Sciences
/ Cocaine
/ Drinking water
/ Drug abuse
/ Drug addiction
/ Drug dependence
/ Drug dosages
/ Drug self-administration
/ Drug withdrawal
/ Excitatory Amino Acid Transporter 2 - metabolism
/ Females
/ Glutamate
/ Glutamatergic transmission
/ Glutamic acid transporter
/ Health aspects
/ Hippocampus
/ Hippocampus - drug effects
/ Hippocampus - metabolism
/ Homeostasis
/ Indolizines
/ Laboratory animals
/ Maintenance
/ Male
/ Medicine and Health Sciences
/ Methadone
/ Microglia
/ Morphine
/ Morphine - administration & dosage
/ Morphine - pharmacology
/ Morphine Dependence - drug therapy
/ Morphine Dependence - metabolism
/ Narcotics
/ Neuronal-glial interactions
/ Nucleus accumbens
/ Nucleus Accumbens - drug effects
/ Nucleus Accumbens - metabolism
/ Opioids
/ Oxidative stress
/ Oxidative Stress - drug effects
/ Pharmacology
/ Polyethylene glycol
/ Product recalls
/ Pyrazoles
/ Pyridines - administration & dosage
/ Pyridines - pharmacology
/ Rats
/ Rats, Wistar
/ Remifentanil
/ Self Administration
/ Testing
/ Tumor necrosis factor-TNF
2024
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Morphine self-administration is inhibited by the antioxidant N‐acetylcysteine and the anti-inflammatory ibudilast; an effect enhanced by their co-administration
by
Quintanilla, María Elena
, Israel, Yedy
, Morales, Paola
, Acuña, Tirso
, Santapau, Daniela
, Riveras, Gabriel
, Ezquer, Fernando
, Gallardo, Javiera
, Rebolledo, Rocío
, Herrera-Marschitz, Mario
in
Acetylcysteine
/ Acetylcysteine - administration & dosage
/ Acetylcysteine - pharmacology
/ Analysis
/ Animal models
/ Animals
/ Anti-inflammatory agents
/ Anti-Inflammatory Agents - administration & dosage
/ Anti-Inflammatory Agents - pharmacology
/ Anti-inflammatory drugs
/ Antioxidants
/ Antioxidants - administration & dosage
/ Antioxidants - pharmacology
/ Astrocytes
/ Biology and Life Sciences
/ Cocaine
/ Drinking water
/ Drug abuse
/ Drug addiction
/ Drug dependence
/ Drug dosages
/ Drug self-administration
/ Drug withdrawal
/ Excitatory Amino Acid Transporter 2 - metabolism
/ Females
/ Glutamate
/ Glutamatergic transmission
/ Glutamic acid transporter
/ Health aspects
/ Hippocampus
/ Hippocampus - drug effects
/ Hippocampus - metabolism
/ Homeostasis
/ Indolizines
/ Laboratory animals
/ Maintenance
/ Male
/ Medicine and Health Sciences
/ Methadone
/ Microglia
/ Morphine
/ Morphine - administration & dosage
/ Morphine - pharmacology
/ Morphine Dependence - drug therapy
/ Morphine Dependence - metabolism
/ Narcotics
/ Neuronal-glial interactions
/ Nucleus accumbens
/ Nucleus Accumbens - drug effects
/ Nucleus Accumbens - metabolism
/ Opioids
/ Oxidative stress
/ Oxidative Stress - drug effects
/ Pharmacology
/ Polyethylene glycol
/ Product recalls
/ Pyrazoles
/ Pyridines - administration & dosage
/ Pyridines - pharmacology
/ Rats
/ Rats, Wistar
/ Remifentanil
/ Self Administration
/ Testing
/ Tumor necrosis factor-TNF
2024
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Morphine self-administration is inhibited by the antioxidant N‐acetylcysteine and the anti-inflammatory ibudilast; an effect enhanced by their co-administration
by
Quintanilla, María Elena
, Israel, Yedy
, Morales, Paola
, Acuña, Tirso
, Santapau, Daniela
, Riveras, Gabriel
, Ezquer, Fernando
, Gallardo, Javiera
, Rebolledo, Rocío
, Herrera-Marschitz, Mario
in
Acetylcysteine
/ Acetylcysteine - administration & dosage
/ Acetylcysteine - pharmacology
/ Analysis
/ Animal models
/ Animals
/ Anti-inflammatory agents
/ Anti-Inflammatory Agents - administration & dosage
/ Anti-Inflammatory Agents - pharmacology
/ Anti-inflammatory drugs
/ Antioxidants
/ Antioxidants - administration & dosage
/ Antioxidants - pharmacology
/ Astrocytes
/ Biology and Life Sciences
/ Cocaine
/ Drinking water
/ Drug abuse
/ Drug addiction
/ Drug dependence
/ Drug dosages
/ Drug self-administration
/ Drug withdrawal
/ Excitatory Amino Acid Transporter 2 - metabolism
/ Females
/ Glutamate
/ Glutamatergic transmission
/ Glutamic acid transporter
/ Health aspects
/ Hippocampus
/ Hippocampus - drug effects
/ Hippocampus - metabolism
/ Homeostasis
/ Indolizines
/ Laboratory animals
/ Maintenance
/ Male
/ Medicine and Health Sciences
/ Methadone
/ Microglia
/ Morphine
/ Morphine - administration & dosage
/ Morphine - pharmacology
/ Morphine Dependence - drug therapy
/ Morphine Dependence - metabolism
/ Narcotics
/ Neuronal-glial interactions
/ Nucleus accumbens
/ Nucleus Accumbens - drug effects
/ Nucleus Accumbens - metabolism
/ Opioids
/ Oxidative stress
/ Oxidative Stress - drug effects
/ Pharmacology
/ Polyethylene glycol
/ Product recalls
/ Pyrazoles
/ Pyridines - administration & dosage
/ Pyridines - pharmacology
/ Rats
/ Rats, Wistar
/ Remifentanil
/ Self Administration
/ Testing
/ Tumor necrosis factor-TNF
2024
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Morphine self-administration is inhibited by the antioxidant N‐acetylcysteine and the anti-inflammatory ibudilast; an effect enhanced by their co-administration
Journal Article
Morphine self-administration is inhibited by the antioxidant N‐acetylcysteine and the anti-inflammatory ibudilast; an effect enhanced by their co-administration
2024
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Overview
The treatment of opioid addiction mainly involves the medical administration of methadone or other opioids, aimed at gradually reducing dependence and, consequently, the need for illicit opioid procurement. Thus, initiating opioid maintenance therapy with a lower level of dependence would be advantageous. There is compelling evidence indicating that opioids induce brain oxidative stress and associated glial activation, resulting in the dysregulation of glutamatergic homeostasis, which perpetuates drug intake. The present study aimed to determine whether inhibiting oxidative stress and/or neuroinflammation reduces morphine self-administration in an animal model of opioid dependence.
Morphine dependence, assessed as voluntary morphine self-administration, was evaluated in Wistar-derived UChB rats. Following an extended period of morphine self-administration, animals were administered either the antioxidant N-acetylcysteine (NAC; 40 mg/kg/day), the anti-inflammatory ibudilast (7.5 mg/kg/day) or the combination of both agents. Oxidative stress and neuroinflammation were evaluated in the hippocampus, a region involved in drug recall that feeds into the nucleus accumbens, where the levels of the glutamate transporters GLT-1 and xCT were further assessed.
Daily administration of either NAC or ibudilast led to a mild reduction in voluntary morphine intake, while the co-administration of both therapeutic agents resulted in a marked inhibition (-57%) of morphine self-administration. The administration of NAC or ibudilast markedly reduced both the oxidative stress induced by chronic morphine intake and the activation of microglia and astrocytes in the hippocampus. However, only the combined administration of NAC + ibudilast was able to restore the normal levels of the glutamate transporter GLT-1 in the nucleus accumbens.
Separate or joint administration of an antioxidant and anti-inflammatory agent reduced voluntary opioid intake, which could have translational value for the treatment of opioid use disorders, particularly in settings where the continued maintenance of oral opioids is a therapeutic option.
Publisher
Public Library of Science
Subject
/ Acetylcysteine - administration & dosage
/ Acetylcysteine - pharmacology
/ Analysis
/ Animals
/ Anti-Inflammatory Agents - administration & dosage
/ Anti-Inflammatory Agents - pharmacology
/ Antioxidants - administration & dosage
/ Cocaine
/ Excitatory Amino Acid Transporter 2 - metabolism
/ Females
/ Male
/ Medicine and Health Sciences
/ Morphine
/ Morphine - administration & dosage
/ Morphine Dependence - drug therapy
/ Morphine Dependence - metabolism
/ Nucleus Accumbens - drug effects
/ Nucleus Accumbens - metabolism
/ Opioids
/ Oxidative Stress - drug effects
/ Pyridines - administration & dosage
/ Rats
/ Testing
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