Your search keyword '"Myrick H"' showing total 4 results

1. Predictors of Naltrexone Response in a Randomized Trial: Reward-Related Brain Activation, OPRM1 Genotype, and Smoking Status.

Author

Schacht JP, Randall PK, Latham PK, Voronin KE, Book SW, Myrick H, and Anton RF

Subjects

Alcoholism genetics, Alcoholism physiopathology, Alcoholism psychology, Brain diagnostic imaging, Brain drug effects, Brain physiopathology, Brain Mapping, Cues, Female, Follow-Up Studies, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Pharmacogenomic Variants, Prognosis, Receptors, Opioid, mu genetics, Reward, Severity of Illness Index, Single-Blind Method, Smoking genetics, Smoking physiopathology, Smoking psychology, Visual Perception drug effects, Visual Perception physiology, Alcoholism drug therapy, Naltrexone therapeutic use, Narcotic Antagonists therapeutic use

Abstract

Naltrexone reduces drinking among individuals with alcohol use disorders (AUDs), but it is not effective for everyone. Variability in its effects on reward-related brain activation, genetic variation, and/or cigarette smoking may account for this mixed response profile. This randomized clinical trial tested the effects of naltrexone on drinking and alcohol cue-elicited brain activation, evaluated whether OPRM1 A118G genotype or smoking moderated these effects, and explored whether the effects of medication on cue-elicited activation predicted subsequent drinking. One hundred and fifty-two treatment-seeking individuals with alcohol dependence, half preselected to carry at least one A118G G (Asp) allele, were randomized to naltrexone (50 mg) or placebo for 16 weeks and administered an fMRI alcohol cue reactivity task at baseline and after 2 weeks of treatment. Naltrexone, relative to placebo, significantly reduced alcohol cue-elicited activation of the right ventral striatum (VS) between baseline and week 2 and reduced heavy drinking over 16 weeks. OPRM1 genotype did not significantly moderate these effects, but G-allele carriers who received naltrexone had an accelerated return to heavy drinking after medication was stopped. Smoking moderated the effects of medication on drinking, such that naltrexone was superior to placebo only among smokers. The degree of reduction in right VS activation between scans interacted with medication in predicting subsequent drinking, such that individuals with greater reduction in activation who received naltrexone, but not placebo, experienced the least heavy drinking during the following 14 weeks. These data replicate previous findings that naltrexone reduces heavy drinking and reward-related brain activation among treatment-seeking individuals with AUDs, and indicate that smoking and the magnitude of reduction in cue-elicited brain activation may predict treatment response.

Published

2017

2. Predictors of Naltrexone Response in a Randomized Trial: Reward-Related Brain Activation, OPRM1 Genotype, and Smoking Status.

Author

Schacht JP, Randall PK, Latham PK, Voronin KE, Book SW, Myrick H, and Anton RF

Abstract

This corrects the article DOI: 10.1038/npp.2017.74.

Published

2017

3. Interacting effects of naltrexone and OPRM1 and DAT1 variation on the neural response to alcohol cues.

Author

Schacht JP, Anton RF, Voronin KE, Randall PK, Li X, Henderson S, and Myrick H

Subjects

Adult, Alcohol Drinking genetics, Alcohol Drinking metabolism, Alcoholism drug therapy, Alcoholism metabolism, Female, Humans, Magnetic Resonance Imaging methods, Male, Naltrexone pharmacology, Narcotic Antagonists pharmacology, Narcotic Antagonists therapeutic use, Polymorphism, Genetic, Polymorphism, Single Nucleotide genetics, Protein Binding physiology, Receptors, Opioid, mu antagonists & inhibitors, Tandem Repeat Sequences genetics, Treatment Outcome, Young Adult, Alcoholism genetics, Cues, Dopamine Plasma Membrane Transport Proteins genetics, Genetic Variation genetics, Naltrexone therapeutic use, Receptors, Opioid, mu genetics

Abstract

Variation at a single nucleotide polymorphism in the μ-opioid receptor gene (OPRM1), A118G (Asn40Asp), may moderate naltrexone (NTX) effects in alcohol dependence. Both NTX and A118G variation have also been reported to affect alcohol cue-elicited brain activation. This study investigated whether sub-acute NTX treatment and A118G genotype interacted in their effects on cue-elicited activation of the ventral striatum (VS), medial prefrontal cortex (mPFC), and orbitofrontal cortex (OFC). Secondarily, variation at a variable number tandem repeat polymorphism in the dopamine transporter gene (DAT1/SLC6A3), which has been associated with increased reward-related activation in VS, was analyzed as a moderator of medication and A118G effects. Seventy-four non-treatment-seeking alcohol-dependent individuals, half preselected to carry at least one copy of the A118G G (Asp) allele, were randomized to NTX (50 mg) or placebo for 7 days, and performed an fMRI alcohol cue reactivity task on day 6. Region-of-interest analyses indicated no main effects of medication or A118G genotype. However, these factors interacted in their effects on OFC activation, such that, among NTX-treated individuals, G-allele carriers had less activation than A-allele homozygotes. DAT1 variation also moderated medication/A118G effects. There was a three-way interaction between medication and A118G and DAT1 genotypes on VS activation, such that, among G-allele carriers who received NTX, DAT1 10-repeat-allele (10R) homozygotes had less activation than 9-repeat-allele (9R) carriers. Further, 10R homozygotes who received NTX had less mPFC activation than 9R carriers. Polymorphic variation in OPRM1 and DAT1 should be considered in future studies of NTX, particularly regarding its effects on reward processing.

Published

2013

4. Differential brain activity in alcoholics and social drinkers to alcohol cues: relationship to craving.

Author

Myrick H, Anton RF, Li X, Henderson S, Drobes D, Voronin K, and George MS

Subjects

Adult, Alcoholic Beverages, Analysis of Variance, Beverages, Brain Mapping, Case-Control Studies, Demography, Female, Humans, Magnetic Resonance Imaging methods, Male, Middle Aged, Photic Stimulation, Rest, Time Factors, Alcohol Drinking physiopathology, Alcohol Drinking psychology, Alcoholism physiopathology, Alcoholism psychology, Brain physiopathology, Cues, Motivation, Social Behavior

Abstract

Using fMRI, our group previously found that after a sip of alcohol and exposure to alcohol beverage pictures, alcoholics compared to social drinkers had increased differential brain activity in the prefrontal cortex and anterior thalamus. This study extends this earlier work with several improvements including imaging the entire brain (rather than the anterior half previously) and recording craving, while the subjects viewed images within the scanner. In a Philips 1.5 T MRI scanner, 10 nontreatment-seeking alcoholics and 10 age-matched healthy social drinkers were given a sip of alcohol before viewing a 12 min randomized presentation of pictures of alcoholic beverages, nonalcoholic beverages, and two different visual control tasks. During picture presentation, changes in regional brain activity were measured in 15 transverse T2(*)-weighted blood oxygen level dependent slices. Subjects rated their urge to drink after each picture sequence. After a sip of alcohol, while viewing alcohol cues compared to viewing other beverage cues, the alcoholics, but not social drinkers, reported higher craving ratings and had increased activity in the prefrontal cortex and anterior limbic regions. Brain activity in the left nucleus accumbens, anterior cingulate, and left orbitofrontal cortex significantly correlated with subjective craving ratings in alcohol subjects but not in control subjects. This study suggests, as did our earlier study, that alcoholics and not social drinkers, when exposed to alcohol cues, have increased brain activity in areas that reportedly subserve craving for other addictive substances.

Published

2004