Your search keyword '"Harry L. June"' showing total 36 results

1. Early life stress is a risk factor for excessive alcohol drinking and impulsivity in adults and is mediated via a CRF/GABAA mechanism

Author

Marjorie C. Gondré-Lewis, Kaitlin T. Warnock, Hong Wang, Harry L. June, Kimberly A. Bell, Holger Rabe, Veera Venkata Naga Phani Babu Tiruveedhula, James Cook, Hartmut Lüddens, and Laure Aurelian

Subjects

Male, 0301 basic medicine, Corticotropin-Releasing Hormone, Physiology, Self Administration, Rats, Sprague-Dawley, Behavioral Neuroscience, 0302 clinical medicine, GABA receptor, Risk Factors, Antalarmin, Prefrontal cortex, GABAA receptor, Maternal Deprivation, Amygdala, Vitamin B 12, Psychiatry and Mental health, Neuropsychology and Physiological Psychology, medicine.anatomical_structure, Female, medicine.symptom, Psychology, medicine.drug, Clinical psychology, medicine.medical_specialty, Alcohol Drinking, medicine.drug_class, Prefrontal Cortex, Binge drinking, Impulsivity, Receptors, Corticotropin-Releasing Hormone, Article, 03 medical and health sciences, Internal medicine, medicine, Animals, Pyrroles, Benzodiazepine, Ethanol, Endocrine and Autonomic Systems, Receptors, GABA-A, Rats, Pyrimidines, 030104 developmental biology, Endocrinology, Impulsive Behavior, Conditioning, Operant, Stress, Psychological, 030217 neurology & neurosurgery

Abstract

Childhood stress and trauma are associated with substance use disorders in adulthood, but the neurological changes that confer increased vulnerability are largely unknown. In this study, maternal separation (MS) stress, restricted to the pre-weaning period, was used as a model to study mechanisms of protracted effects of childhood stress/traumatic experiences on binge drinking and impulsivity. Using an operant self-administration model of binge drinking and a delay discounting assay to measure impulsive-like behavior, we report that early life stress due to MS facilitated acquisition of binge drinking and impulsivity during adulthood in rats. Previous studies have shown heightened levels of corticotropin releasing factor (CRF) after MS, and here, we add that MS increased expression levels of GABA(A) α2 subunit in central stress circuits. To investigate the precise role of these circuits in regulating impulsivity and binge drinking, the CRF1 receptor antagonist antalarmin and the novel GABA(A) α2 subunit ligand 3-PBC were infused into the central amygdala (CeA) and medial prefrontal cortex (mPFC). Antalarmin and 3-PBC at each site markedly reduced impulsivity and produced profound reductions on binge-motivated alcohol drinking, without altering responding for sucrose. Furthermore, whole-cell patch-clamp studies showed that low concentrations of 3-PBC directly reversed the effect of relatively high concentrations of ethanol on α2β3γ2 GABA(A) receptors, by a benzodiazepine site-independent mechanism. Together, our data provide strong evidence that maternal separation, i.e. early life stress, is a risk factor for binge drinking, and is linked to impulsivity, another key risk factor for excessive alcohol drinking. We further show that pharmacological manipulation of CRF and GABA receptor signaling is effective to reverse binge drinking and impulsive-like behavior in MS rats. These results provide novel insights into the role of the brain stress systems in the development of impulsivity and excessive alcohol consumption.

Published

2016

2. Deficits in substance P mRNA levels in the CeA are inversely associated with alcohol-motivated responding

Author

Andrew Rong Song Tzeng Yang, Heon Soo Yi, Jacek Mamczarz, Harry L. June, and Bang H. Hwang

Subjects

Male, medicine.medical_specialty, Substance P, Alcohol, In situ hybridization, Anxiety, Amygdala, Article, Cellular and Molecular Neuroscience, chemistry.chemical_compound, In vivo, Internal medicine, medicine, Animals, RNA, Messenger, Receptor, In Situ Hybridization, Motivation, Ethanol, Central nucleus of the amygdala, Central Nervous System Depressants, Rats, Behavior, Addictive, Alcoholism, Endocrinology, medicine.anatomical_structure, chemistry, Autoradiography

Abstract

In the present study, in vitro and in vivo studies were conducted to determine the relationship between innate substance P (SP) levels and alcohol-motivated behavior in alcohol-preferring (P) and nonpreferring (NP) rat lines. In Experiment 1, in situ hybridization and quantitative autoradiography were used to detect and measure SP mRNA levels in discrete brain loci of the P and NP rats. The results indicated significantly lower SP mRNA levels in the central nucleus of the amygdala (CeA) of P compared with those of NP rats. Experiment 2 evaluated the effects of SP, microinfused into the CeA, on alcohol (10%, v/v) and sucrose (2%, w/v) motivated responding in the P rat. The results revealed that, when infused into the CeA (1–8 μg), SP reduced alcohol responding by 48–85% of control levels, with no effects on sucrose responding. Neuroanatomical control infusions (1–8 μg) into the caudate putamen (CPu) also failed to significantly alter alcohol- or sucrose-motivated behaviors. Given the selective reductions on alcohol (compared to sucrose) responding by direct intracranial infusion of SP, the data suggest that deficits in SP signaling within the CeA (an anxiety regulating locus) are inversely associated with alcohol-motivated behaviors. Activation of SP receptors in the CeA may reduce anxiety-like behavior in the P rat and contribute to reductions on alcohol responding. The SP system may be a suitable target for the development of drugs to reduce alcohol-drinking behavior in humans. Synapse 63:972–981, 2009. © 2009 Wiley-Liss, Inc.

Published

2009

3. Selective GABAA ??5 Benzodiazepine Inverse Agonist Antagonizes the Neurobehavioral Actions of Alcohol

Author

Scott C. Harvey, Katrina L. Foster, Rancia Cummings, Marin Garcia, James H. Woods, Dynesha Mason, Harry L. June, Xiaoyan Li, Jason B. Cook, James M. Cook, Shannan McCane, Collette Grey, William J. A. Eiler, and Peter F. McKay

Subjects

medicine.medical_specialty, medicine.drug_class, Medicine (miscellaneous), Motor Activity, Pharmacology, Toxicology, Hippocampus, Open field, GABA Antagonists, Benzodiazepines, chemistry.chemical_compound, Internal medicine, medicine, Animals, Inverse agonist, GABA-A Receptor Agonists, Receptor, Benzodiazepine, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, Rats, Inbred Strains, Rats, Psychiatry and Mental health, Endocrinology, chemistry, Flumazenil, Sedative, ZK-93426, Arousal, Alcohol Deterrents, medicine.drug

Abstract

Background Previous research has implicated the alpha5-containing GABAA receptors of the hippocampus in the reinforcing properties of alcohol. In the present study, a selective GABAA alpha5 benzodiazepine inverse agonist (e.g., RY 023) was used in a series of in vivo and in vitro studies to determine the significance of the alpha5-receptor in the neurobehavioral actions of alcohol. Methods In experiment one, systemic injections of RY 023 (1 to 10 mg/kg IP) dose-dependently reduced ethanol-maintained responding by 52% to 86% of controls, whereas bilateral hippocampal infusions (0.3 to 20 microg) reduced responding by 66% to 84% of controls. Saccharin responding was reduced only with the highest intraperitoneal (e.g., 10 mg) and microinjected (e.g., 20 microg) doses. In experiment two, RY 023 (3.0 to 15 mg/kg IP) reversed the motor-impairing effects of a moderate dose of alcohol (0.75 g/kg) on an oscillating bar task in the absence of intrinsic effects. In the open field, RY 023 (3.0 to 7.5 mg/kg) produced intrinsic effects alone but attenuated the suppression of the 1.25 g/kg ethanol dose. Because the diazepam-insensitive receptors (e.g., alpha4 and alpha6) have been suggested to play a role in alcohol motor impairing and sedative actions, experiment three compared the efficacy of RY 023 with Ro 15-4513 and two prototypical benzodiazepine antagonists (e.g., flumazenil and ZK 93426) across the alpha4beta3gamma2-, alpha5beta3gamma2-, and alpha6beta3gamma2-receptor subtypes in Xenopus oocytes. Results RY 023 produced classic inverse agonism at all receptor subtypes, whereas Ro15-4513 and the two antagonists displayed a neutral or agonistic profile at the diazepam-insensitive receptors. Conclusions Overall, the results extend our previous findings by demonstrating that an alpha5-subtype ligand is capable of attenuating not only the rewarding action of alcohol but also its motor impairing and sedative effects. We propose that these actions are mediated in part by the alpha5-receptors of the hippocampus. The hippocampal alpha5-receptors could represent novel targets in understanding the neuromechanisms regulating the neurobehavioral actions of alcohol in humans.

Published

2005

4. GABAA and Opioid Receptors of the Central Nucleus of the Amygdala Selectively Regulate Ethanol-Maintained Behaviors

Author

Harry L. June, Dana Milbourne, Wenyuan Yin, Katrina L. Foster, Peter F. McKay, Regat Seyoum, P V V S Sarma, and James M. Cook

Subjects

Male, Sucrose, medicine.medical_specialty, Time Factors, Microinjections, medicine.drug_class, Narcotic Antagonists, Pharmacology, Naltrexone, Opioid receptor, Internal medicine, mental disorders, medicine, Animals, GABA-A Receptor Antagonists, Receptor, Opioidergic, Analysis of Variance, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, Central nucleus of the amygdala, Putamen, Rats, Inbred Strains, Amygdala, Receptors, GABA-A, Rats, Behavior, Addictive, Alcoholism, Psychiatry and Mental health, Endocrinology, Opioid, Receptors, Opioid, Conditioning, Operant, Female, Reinforcement, Psychology, Opioid antagonist, Carbolines, medicine.drug

Abstract

The present study tested the hypothesis that GABA(A) and opioid receptors within the central nucleus of the amygdala (CeA) regulate ethanol (EtOH), but not sucrose-maintained responding. To accomplish this, betaCCt, a mixed benzodiazepine (BDZ) agonist-antagonist with binding selectivity at the alpha1 subunit-containing GABA(A) receptor, and the nonselective opioid antagonist, naltrexone, were bilaterally infused directly into the CeA of alcohol-preferring rats. The results demonstrated that in HAD-1 and P rat lines, betaCCt (5-60 microg) reduced EtOH-maintained responding by 56-89% of control levels. On day 2, betaCCt (10-40 microg) continued to suppress EtOH maintained responding in HAD-1 rats by as much as 60-85% of control levels. Similarly, naltrexone (0.5-30 microg) reduced EtOH-maintained responding by 56-75% of control levels in P rats. betaCCt and naltrexone exhibited neuroanatomical and reinforcer specificity within the CeA. Specifically, no effects on EtOH-maintained responding were observed following infusion into the caudate putamen (CPu), a locus several millimeters dorsal to the CeA. Additionally, responding maintained by sucrose, when presented concurrently with ethanol (EtOH) or presented alone, was not altered by betaCCt. Naltrexone reduced sucrose-maintained responding only under the 5 microg dose condition when sucrose was presented alone, however, it did not alter sucrose responding when given concurrently with EtOH. These results support the hypothesis that GABA(A) and opioid receptors within the CeA can selectively regulate EtOH-maintained responding. The CeA may represent a novel target site in the development of prototypical GABA(A) and opioidergic receptor ligands, which selectively reduce alcohol abuse in humans.

Published

2003

5. Differential Responding for Brain Stimulation Reward and Sucrose in High-Alcohol-Drinking (HAD) and Low-Alcohol-Drinking (LAD) Rats

Author

Jacob Masters, Regat Seyoum, James E. Woods, Lorie La Duff, Harry L. June, Annabel Chen, Peter F. McKay, and Michael J. Lewis

Subjects

Male, medicine.medical_specialty, Sucrose, Reinforcement Schedule, Alcohol Drinking, Medicine (miscellaneous), Alcohol, Stimulation, Selective breeding, Toxicology, Developmental psychology, chemistry.chemical_compound, Reward, Species Specificity, Internal medicine, medicine, Reaction Time, Animals, Reinforcement, Medial forebrain bundle, Ethanol, Brain, Rats, Psychiatry and Mental health, Endocrinology, chemistry, Brain stimulation reward, Psychology

Abstract

Background: This study examined the associations among selective breeding for alcohol preference, intake of sweet solutions, and responding for brain stimulation reward (BSR), a nonoral reinforcer, in alcohol-preferring high–alcohol-drinking (HAD)-1 and nonpreferring low–alcohol-drinking (LAD)-1 rats. Methods: Adult male HAD-1 and LAD-1 rats were trained to lever press for medial forebrain bundle stimulation. Current intensity was varied in separate sessions to generate a rate/intensity function. To further examine BSR responding, the animals responded for stimulation at 100 Hz and at a fixed current intensity on an FR1 schedule. In subsequent sessions, the schedule was increased to FR6 and then to FR12. To examine responding for the sucrose solution, we trained a separate group of HAD-1/LAD-1 rats to bar press for sucrose on an FR1 schedule. Similar to the BSR experiment, in following sessions, the schedule was increased to an FR6 and then to an FR12 schedule. Results: No significant differences were observed between the two rat lines across a range of current intensities. As the reinforcement schedule increased, HAD-1 rats exhibited a dramatic decrease in BSR responding, whereas the LAD-1 rats displayed a more protracted reduction. In contrast to BSR, marked elevations in responding were observed for sucrose as the schedule increased. However, in HAD-1 rats, response rates were similar on the FR6 and FR12 schedules, whereas LAD-1 rats showed a reduction in response rates from the FR6 to FR12 schedule. Furthermore, HAD-1 rats exhibited significantly more responses compared with LAD-1 rats across the three reinforcement schedules. An analysis of the response profile for the three reinforcement schedules suggested that few if any postreinforcement pauses were exhibited when the reinforcer was BSR compared with sucrose in both lines. Conclusion: Medial forebrain bundle BSR is a powerful reinforcer in both HAD-1 and LAD-1 lines. However, BSR responding was not associated with selective breeding for alcohol preference. In contrast, selective breeding for alcohol preference was associated with sucrose consumption, especially as the amount of work increased. The lack of correspondence between BSR and sweet taste rewards in HAD-1 and LAD-1 lines may suggest important differences yet an overlapping brain reward mechanism in the control of motivated behaviors in these selected lines.

Published

2003

6. The GABAAReceptor α1Subtype in the Ventral Pallidum Regulates Alcohol-Seeking Behaviors

Author

Katrina L. Foster, Chunrong Ma, Shannan McCane, Regat Seyoum, Harry L. June, Scott C. Harvey, Michelle R. Carroll, Collette Grey, Pete F. McKay, Dynesha Mason, James M. Cook, Cecily M. Jones, Rancia Cummings, and James E. Woods

Subjects

Male, Agonist, Patch-Clamp Techniques, Microinjections, medicine.drug_class, Pharmacology, Nucleus accumbens, Globus Pallidus, Ligands, Binding, Competitive, Partial agonist, RNA, Complementary, GABA Antagonists, Ventral pallidum, Benzodiazepines, Xenopus laevis, medicine, Animals, Protein Isoforms, Patch clamp, ARTICLE, GABA Modulators, Receptor, Appetitive Behavior, Benzodiazepine, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, Drug Administration Routes, General Neuroscience, Rats, Inbred Strains, Receptors, GABA-A, Recombinant Proteins, Rats, Alcoholism, Disease Models, Animal, Protein Subunits, Oocytes, Reinforcement, Psychology, Carbolines, Synaptosomes

Abstract

We investigated the potential role of the alpha1-containing GABA(A) receptor in regulating the reinforcing properties of alcohol. To accomplish this, we developed 3-propoxy-beta-carboline hydrochloride (3-PBC), a mixed agonist-antagonist benzodiazepine site ligand with binding selectivity at the alpha1 receptor. We then tested the capacity of 3-PBC to block alcohol-maintained responding in the ventral pallidum (VP), a novel alcohol reward substrate, which primarily expresses the alpha1-receptor isoform. Our results demonstrated that bilateral microinfusion of 3-PBC (0.5-40 microg) in the anterior and medial VP produced marked reductions in alcohol-maintained responding in a genetically selected rodent model of alcohol drinking. The VP infusions showed both neuroanatomical and reinforcer specificity because no effects were seen in sites dorsal to the VP (e.g., nucleus accumbens, caudate putamen). The saccharin-maintained responding was reduced only with the highest dose (40 microg). Parenteral injections of 3-PBC (1-20 mg/kg) also showed a similar selectivity on alcohol-maintained responding. Complementary in vitro studies revealed that 3-PBC exhibited a low partial agonist efficacy profile at recombinant diazepam-sensitive receptors (e.g., alpha1beta3gamma2, alpha2beta3gamma, and alpha3beta3gamma2). The selective suppression of 3-PBC on alcohol-maintained responding after central and parenteral administrations, together with its low-efficacy agonist profile, suggest that the reduction in alcohol-maintained behaviors was not attributable to a general suppression on consummatory behaviors. These results demonstrate that the alpha1-containing GABA(A) receptors in both the anterior and medial VP are important in regulating the reinforcing properties of alcohol. These receptors represent novel targets in the design and development of pharmacotherapies for alcohol-dependent subjects.

Published

2002

7. CRF-amplified neuronal TLR4/MCP-1 signaling regulates alcohol self-administration

Author

Kimberly A. Bell, Laure Aurelian, Irina Balan, Harry L. June, Kaitlin T. Warnock, Juan Liu, Adam C. Puche, and Dominique Bollino

Subjects

medicine.medical_specialty, Alcohol Drinking, Corticotropin-Releasing Hormone, Genetic Vectors, Binge drinking, Self Administration, Biology, medicine.disease_cause, Binge Drinking, Cell Line, Mice, Internal medicine, medicine, Animals, Simplexvirus, Genetic Predisposition to Disease, RNA, Small Interfering, Receptor, Chemokine CCL2, Pharmacology, Neurons, Ethanol, Monocyte, Central nucleus of the amygdala, Alcohol dependence, Central Amygdaloid Nucleus, Ventral Tegmental Area, Central Nervous System Depressants, Rats, Ventral tegmental area, Toll-Like Receptor 4, Psychiatry and Mental health, medicine.anatomical_structure, Endocrinology, Herpes simplex virus, Immunology, TLR4, Original Article

Abstract

Alcohol dependence is a complex disorder that initiates with episodes of excessive alcohol drinking known as binge drinking. It has a 50–60% risk contribution from inherited susceptibility genes; however, their exact identity and function are still poorly understood. We report that alcohol-preferring P rats have innately elevated levels of Toll-like receptor 4 (TLR4) and monocyte chemotactic protein-1 (MCP-1) that colocalize in neurons from the central nucleus of the amygdala (CeA) and ventral tegmental area (VTA). To examine the potential role of a TLR4/MCP-1 signal, we used Herpes Simplex Virus (HSV) vectors (amplicons) that retain in vivo neurotropism. Infusion of amplicons for TLR4 or MCP-1 siRNA into the CeA or VTA from the P rats inhibited target gene expression and blunted binge drinking. A similarly delivered amplicon for scrambled siRNA did not inhibit TLR4 or MCP-1 expression nor reduce binge drinking, identifying a neuronal TLR4/MCP-1 signal that regulates the initiation of voluntary alcohol self-administration. The signal was sustained during alcohol drinking by increased expression of corticotropin-releasing factor and its feedback regulation of TLR4 expression, likely contributing to the transition to alcohol dependence.

Published

2014

8. The novel benzodiazepine inverse agonist RO19-4603 antagonizes ethanol motivated behaviors: neuropharmacological studies

Author

Lucas Torres, Charity R Cason, Bang H. Hwang, Harry L. June, James M. Murphy, and Misty R Braun

Subjects

Male, Alcohol Drinking, Microinjections, medicine.drug_class, Pharmacology, Nucleus accumbens, chemistry.chemical_compound, Reward, Chloride Channels, medicine, Animals, Inverse agonist, GABA-A Receptor Antagonists, Molecular Biology, Saccharin, Benzodiazepine, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, General Neuroscience, Brain, Central Nervous System Depressants, Azepines, Receptors, GABA-A, medicine.disease, Rats, Ventral tegmental area, medicine.anatomical_structure, chemistry, Anesthesia, Conditioning, Operant, Female, Neurology (clinical), Diazepam, Ingestive behaviors, Alcohol Deterrents, Developmental Biology, medicine.drug

Abstract

The novel imidazothienodiazepine inverse agonist RO19-4603 has been reported to attenuate EtOH intake in home cage drinking tests for at least 24 h post-drug administration after systemic administration. In the present study, selectively bred alcohol-preferring (P) rats were trained under a concurrent (FR4–FR4) operant schedule to press one lever for EtOH (10% v/v) and another lever for saccharin (0.05% or 0.75% g/v), then dose-response and timecourse effects of RO19-4603 were evaluated. Systemic RO19-4603 injections (0.0045–0.3 mg/kg; i.p.) profoundly reduced EtOH responding by as much as 97% of vehicle control on day 1. No effects were seen on saccharin responding except with the highest dose level (0.3 mg/kg). In a second experiment, microinjections of RO19-4603 (2–100 ng) directly into the nucleus accumbens (NA) suppressed EtOH responding on day 1 by as much as 53% of control: Control injections dorsal to the NA or ventral tegmental area did not significantly alter EtOH or saccharin responding. On day 2, rats in both experiments received no RO19-4603 treatments; however, all 7 of the i.p. doses, and all 3 of the intra-NA infusions continued to significantly suppress EtOH responding by 43–85% of vehicle control levels. In addition, i.p. injections of RO19-4603 produced a dose-dependent decrease in the slope of the cumulative record for EtOH responding, while concomitantly producing a dose-dependent increase in the slope for saccharin responding. RO19-4603's actions appear to be mediated via recognition sites at GABAA-BDZ receptors which regulate EtOH reinforcement, and not via mechanisms regulating ingestive behaviors. Based on recent in situ hybridization studies in our laboratory, we hypothesize that occupation of α4 containing GABAA diazepam insensitive (DI) receptors in the NA, may mediate in part, the RO19-4603 suppression of EtOH responding in EtOH-seeking P rats.

Published

1998

9. Effects of the benzodiazepine inverse agonist RO19-4603 alone and in combination with the benzodiazepine receptor antagonists flumazenil, ZK 93426 and CGS 8216, on ethanol intake in alcohol-preferring (P) rats

Author

Rhonda Cox, Lucas Torres, Jackie J. Mellor-Burke, Margaret L. Hite, Harry L. June, Scott E. Duemler, Charity R Cason, Terri L. Greene, Ting-Kai Li, Lawrence Lumeng, James M. Murphy, and John A. Williams

Subjects

medicine.medical_specialty, Benzodiazepine, Ethanol, medicine.drug_class, General Neuroscience, Antagonist, Pharmacology, chemistry.chemical_compound, Endocrinology, chemistry, Flumazenil, Internal medicine, medicine, Inverse agonist, ZK-93426, Neurology (clinical), CGS-8216, Molecular Biology, Saccharin, Developmental Biology, medicine.drug

Abstract

The present study investigated dose dependence and time course effects of the benzodiazepine (BDZ) partial inverse agonist, RO19-4603 (0.005–0.30 mg/kg) alone, and in combination with the BDZ receptor antagonists flumazenil, ZK 93426, and CGS 8216 (20 mg/kg) in selectively bred alcohol-preferring (P) rats provided a two-bottle choice test between ethanol (EtOH) (10% v/v), and a palatable saccharin (0.0125% g/v) solution. A single dose of R019-4603 as low as 0.009 mg/kg selectively reduced EtOH drinking during the initial 15 min of a 4 h access to 19−0% of control levels on day 1. The 0.08, 0.15 and 0.30 mg/kg doses of R019-4603 significantly reduced total EtOH intake in the 4 h access period to 57−45% of controls on day 1. On day 2, no R019-4603 injections were given; however, six of the seven doses of R019-4603 (0.009, 0.02, 0.04, 0.08, 0.15, and 0.30 mg/kg) continued to reduce EtOH intake to 42−3% of control levels at the initial 15 min interval, while the 0.005, 0.009, 0.08, and 0.30 mg/kg doses reduced total 4 h EtOH intake to 60-42% of controls. Saccharin intake was either not altered by R019-4603 or showed increases during the initial 15 min intervals and the total 4 h sessions on days 1 and 2. Food intake was also unaffected by R019-4603. The CGS 8216, but neither flumazenil nor ZK 93426, reliably reversed the RO19-4603-induced suppression of EtOH intake on days 1 and 2. That certain BDZ inverse agonists can attenuate motivated behavior for EtOH reinforcement over a prolonged time course may provide a possible therapeutic approach to reducing EtOH consumption associated with alcoholism.

Published

1996

10. Amitifadine, a triple monoamine uptake inhibitor, reduces binge drinking and negative affect in an animal model of co-occurring alcoholism and depression symptomatology

Author

Kaitlin T. Warnock, Andrew R.S.T. Yang, Heon S. Yi, Harry L. June, Timothy Kelly, Anthony S. Basile, and Phil Skolnick

Subjects

Male, medicine.medical_specialty, Imipramine, Amitifadine, Clinical Biochemistry, Binge drinking, Motor Activity, Toxicology, Affect (psychology), Biochemistry, Article, Binge Drinking, Behavioral Neuroscience, chemistry.chemical_compound, Internal medicine, medicine, Animals, Humans, Biogenic Monoamines, Psychiatry, Biological Psychiatry, Depression (differential diagnoses), Pharmacology, Aza Compounds, Ethanol, Depression, Anhedonia, Bridged Bicyclo Compounds, Heterocyclic, Rats, Affect, Alcoholism, Disease Models, Animal, Monoamine neurotransmitter, Endocrinology, chemistry, medicine.symptom, Psychology, medicine.drug, Behavioural despair test

Abstract

The co-occurrence of alcoholism and depression is highly prevalent and difficult to treat. In an animal model of binge drinking that exhibits abstinence-induced behaviors reminiscent of negative affective states, the triple monoamine uptake inhibitor, amitifadine, produced a selective, dose dependent attenuation of binge drinking. Amitifadine also reversed abstinence-induced increases in the intracranial self-stimulation threshold, a model of anhedonia, and immobility in the forced swim test, reflecting behavioral despair. In view of the safety profile of amitifadine in humans, including low risk for weight gain, lack of sexual side effects, and low potential for abuse, we hypothesize that amitifadine will be effective in treating co-occurring alcoholism and depression.

Published

2012

11. Interactions of Ro15-4513, Ro15-1788 (flumazenil) and ethanol on measures of exploration and locomotion in rats

Author

Harry L. June and Michael J. Lewis

Subjects

Flumazenil, Male, Azides, medicine.medical_specialty, Receptor complex, Intrinsic activity, medicine.drug_class, Environment, Motor Activity, Pharmacology, Anxiolytic, Rats, Sprague-Dawley, Benzodiazepines, Internal medicine, mental disorders, medicine, Animals, Inverse agonist, Ro15-4513, Dose-Response Relationship, Drug, Ethanol, Antagonist, Receptors, GABA-A, Receptor antagonist, Rats, Endocrinology, Anti-Anxiety Agents, Exploratory Behavior, Psychology, medicine.drug

Abstract

The present study investigated the role of the GABAA-benzodiazepine (BDZ) receptor complex in mediating ethanol (ETOH)-induced increases in exploration (head-dipping) and locomotion of rats in a holeboard test. Male Sprague-Dawley rats were selected based on low basal exploratory rates to increase the likelihood that ETOH would increase these behaviors. The effects of the BDZ partial inverse agonist, Ro15-4513 (2.5 mg/kg), and the BDZ receptor antagonist, Ro15-1788 (flumazenil) (8.0 mg/kg), alone, and in combination with ETOH (0.25, 0.50 and 0.75 g/kg, IP) were investigated. The 0.25 and 0.50 g/kg doses of ETOH markedly increased both exploration and locomotion in low exploratory rats. The ETOH-induced increases were prevented by Ro15-4513 on both measures at a dose that produced no observable intrinsic action; however, this apparent lack of intrinsic activity on exploration may have been related to the low basal rates of responding in the subjects. The BDZ antagonist, flumazenil, completely reversed the antagonistic action produced by Ro15-4513 of the ETOH-induced stimulant effects on locomotion, however, flumazenil exerted only a marginal statistically significant effect on Ro15-4513's actions on head-dipping. When flumazenil was given alone, it increased head-dipping, but was without effect on locomotion. Flumazenil did not affect ETOH-induced increases in locomotion; however, ETOH and flumazenil appeared to show agonistic effects on exploration. The different effects exerted by flumazenil alone, and in combination with ETOH on head-dipping and locomotion suggest that the actions of flumazenil on these behaviors are mediated through separate mechanisms. The research further suggests that both the anxiolytic and locomotor activational effects of ETOH are mediated through the GABAA-BDZ receptor complex.

Published

1994

12. SYNERGISTIC EFFECTS OF ETHANOL AND COCAINE ON BRAIN STIMULATION REWARD

Author

Michael J. Lewis and Harry L. June

Subjects

Male, Reinforcement Schedule, Central nervous system, Hypothalamus, Experimental and Cognitive Psychology, Stimulation, Pharmacology, Drug synergism, Behavioral Neuroscience, chemistry.chemical_compound, Cocaine, medicine, Animals, Electric stimulation, Ethanol, Behavior, Animal, Dose-Response Relationship, Drug, Drug Synergism, Electric Stimulation, Electrodes, Implanted, Rats, medicine.anatomical_structure, chemistry, Facilitation, Brain stimulation reward, Psychology, Neuroscience, psychological phenomena and processes, Research Article

Abstract

The effects of two widely abused drugs, ethanol and cocaine, were examined alone and in combination on intracranial reward processes. In agreement with previous research, higher doses of both cocaine and ethanol alone produced facilitation of behavior maintained by brain stimulation reward. Low intraperitoneal doses of ethanol and cocaine, which alone did not affect performance, were found to reduce stimulation reward threshold and modestly increase response rate. The enhancement of brain stimulation reward by the combination of ethanol and cocaine suggests that both drugs may produce their rewarding effects through common neuronal substrates and that they may potentiate the abuse of each other.

Published

1994

13. Effects of the triple monoamine uptake inhibitor DOV 102,677 on alcohol-motivated responding and antidepressant activity in alcohol-preferring (P) rats

Author

Andrew R S T, Yang, Heon S, Yi, Kaitlin T, Warnock, Jacek, Mamczarz, Harry L, June, Nikhil, Mallick, Philip A, Krieter, Leonardo, Tonelli, Phil, Skolnick, and Anthony S, Basile

Subjects

Male, Sucrose, Dose-Response Relationship, Drug, Ethanol, Depression, Drug Evaluation, Preclinical, Central Nervous System Depressants, Bridged Bicyclo Compounds, Heterocyclic, Article, Rats, Rats, Sprague-Dawley, Alcoholism, Disease Models, Animal, Sweetening Agents, Animals, Neurotransmitter Uptake Inhibitors, Swimming

Abstract

Concurrent inhibitors of dopamine, norepinephrine, and serotonin uptake have been proposed as novel antidepressants. Given the high comorbidity between alcoholism and depression, we evaluated the activity of DOV 102,677 (DOV) on alcohol-maintained responding and performance in the forced swim test (FST), a model of antidepressant (AD) activity, using alcohol-preferring (P) rats. Following training to lever press for either alcohol (10% v/v) or sucrose (3, 2%, w/v) on a fixed-ratio 4 (FR4) schedule, DOV (1.56 to 50 mg/kg; PO) was given 25 minutes or 24 hours prior to evaluation. The effects of DOV (12.5 to 50 mg/kg; PO) in the FST were evaluated 25 minutes posttreatment. DOV (6.25 to 50 mg/kg) dose-dependently reduced alcohol-maintained responding by 59 to 88% at 25 minutes posttreatment, without significantly altering sucrose responding. The reduction in alcohol responding (44% at 50 mg/kg) was sustained for up to 120 hours after a single dose. Administration of a single dose of DOV (25, 50 mg/kg) 24 hours before testing suppressed alcohol responding for 48 hours by 59 to 62%. DOV (12.5 to 50 mg/kg) also dose-dependently reduced immobility of P rats in the FST. DOV produces both prolonged and selective reductions of alcohol-motivated behaviors in P rats. The elimination kinetics of DOV suggests that its long duration of action may be due to an active metabolite. DOV also produced robust AD-like effects in P rats. We propose that DOV may be useful in treating comorbid alcoholism and depression in humans.

Published

2011

14. Ethanol-induced stimulation and depression on measures of locomotor activity: Effects of basal activity levels in rats

Author

Timothy O. Moore, Harry L. June, and Michael J. Lewis

Subjects

Male, medicine.medical_specialty, Health (social science), medicine.drug_class, medicine.medical_treatment, Stimulation, Motor Activity, Toxicology, Biochemistry, Locomotor activity, Rats, Sprague-Dawley, Behavioral Neuroscience, chemistry.chemical_compound, Basal (phylogenetics), Internal medicine, medicine, Animals, Ethanol, Dose-Response Relationship, Drug, General Medicine, Rats, Stimulant, Dose–response relationship, Endocrinology, Neurology, chemistry, Anesthesia, Toxicity, Depressant

Abstract

Male Sprague-Dawley rats selected for low (LA) and high activity (HA) were used to investigate the biphasic actions of ethanol (EtOH) (20% v/v) on spontaneous measures of activity. Following IP injections of low to moderate doses of EtOH (0.10 g/kg and 0.50 g/kg), horizontal and vertical activities were assessed at 0-10- and 30-40-min intervals. Rats preselected for LA exhibited an increase in performance on both measures. The stimulatory effect, however, was observed only during the 0-10-min session with the lowest dose of EtOH (0.10 g/kg). The 0.50-g/kg dose had no effect on either measure at the 0-10-min interval; however, both doses suppressed activity at the 30-40-min interval. In contrast, activity was suppressed in HA animals independent of the EtOH dose level or time interval. These results demonstrate that basal response profiles are important predictors of behavioral activation following low stimulant doses of EtOH. Moreover, the results demonstrate the importance of selecting animals for basal activity levels to reliably interpret the mechanisms controlling the stimulant and depressant effects of EtOH.

Published

1993

15. α4-Containing GABA(A) Receptors are Required for Antagonism of Ethanol-Induced Motor Incoordination and Hypnosis by the Imidazobenzodiazepine Ro15-4513

Author

Sangeetha V. Iyer, Rodrigo eBenavides, Dev eChandra, James M Cook, Sundari eRallapalli, Harry L. June, and Gregg E Homanics

Subjects

Ataxia, medicine.drug_class, alcohol antagonist, extrasynaptic GABAA receptor, Pharmacology, Ro15-4513, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Pharmacology (medical), Receptor, 030304 developmental biology, Original Research, 0303 health sciences, Benzodiazepine, Ethanol, GABAA receptor, Chemistry, alcohol, lcsh:RM1-950, lcsh:Therapeutics. Pharmacology, Mechanism of action, alcohol receptor, medicine.symptom, benzodiazepine, Antagonism, 030217 neurology & neurosurgery, medicine.drug

Abstract

Alcohol (ethanol) is widely consumed for its desirable effects but unfortunately has strong addiction potential. Some imidazobenzodiazepines such as Ro15-4513 are able to antagonize many ethanol-induced behaviors. Controversial biochemical and pharmacological evidence suggest that the effects of these ethanol antagonists and ethanol are mediated specifically via overlapping binding sites on α4/δ-containing GABAA-Rs. To investigate the requirement of α4-containing GABAA-Rs in the mechanism of action of Ro15-4513 on behavior, wildtype (WT) and α4 knockout (KO) mice were compared for antagonism of ethanol-induced motor incoordination and hypnosis. Motor effects of ethanol were tested in two different fixed speed rotarod assays. In the first experiment, mice were injected with 2.0 g/kg ethanol followed 5 min later by 10 mg/kg Ro15-4513 (or vehicle) and tested on a rotarod at 8 rpm. In the second experiment, mice received a single injection of 1.5 g/kg ethanol +/- 3 mg/kg Ro15-4513 and were tested on a rotarod at 12 rpm. In both experiments, the robust Ro15-4513 antagonism of ethanol-induced motor ataxia that was observed in WT mice was absent in KO mice. A loss of righting reflex (LORR) assay was used to test Ro15-4513 (20 mg/kg) antagonism of ethanol (3.5 g/kg)-induced hypnosis. An effect of sex was observed on the LORR assay, so males and females were analyzed separately. In male mice, Ro15-4513 markedly reduced ethanol-induced LORR in WT controls, but α4 KO mice were insensitive to this effect of Ro15-4513. In contrast, female KO mice did not differ from WT controls in the antagonistic effects of Ro15-4513 on ethanol-induced LORR. We conclude that Ro15-4513 requires α4-containing receptors for antagonism of ethanol-induced LORR (in males) and motor ataxia.

Published

2010

16. Operant Self-Administration Models for Testing the Neuropharmacological Basis of Ethanol Consumption in Rats

Author

Nicholas W. Gilpin and Harry L. June

Subjects

Taste, Alcohol, Self Administration, Article, chemistry.chemical_compound, Neuropharmacology, Alcohol-Induced Disorders, Nervous System, Species Specificity, Neuropsychology, Animals, Operant conditioning, Motivation, Ethanol, General Neuroscience, Rats, Inbred Strains, Rats, Alcoholism, Disease Models, Animal, chemistry, Conditioning, Conditioning, Operant, Alcohol intake, Self-administration, Psychology, Energy Intake, Neuroscience

Abstract

Operant self-administration procedures are used to assess the neural basis of ethanol-seeking behavior under a wide range of experimental conditions. Rats do not spontaneously self-administer ethanol in pharmacologically meaningful amounts. This unit provides a step-by-step guide for training rats to self-administer quantities of ethanol that produce moderate to high blood-alcohol content. Different protocols are used for rats that are genetically heterogeneous versus rats that are selectively bred for high alcohol preference. Also, these protocols have different sets of advantages and disadvantages, for example, control for caloric intake or taste between two solutions that maintain operant lever-press behavior. Basic self-administration protocols can also be altered to focus on different aspects of the motivational properties of ethanol (for example, those related to dependence). This unit provides multiple protocols for producing alcohol intake in rats that can be pharmacologically probed relative to a variety of control conditions.

Published

2010

17. Failure of Ro15-4513 to alter an ethanol-induced taste aversion

Author

Harry L. June, Leslie H. Hicks, Pamela L. June, Kevin R. Domangue, Guy Lummis, and Michael J. Lewis

Subjects

Male, Agonist, Azides, Taste, Receptor complex, medicine.drug_class, Clinical Biochemistry, Pharmacology, Toxicology, Biochemistry, Benzodiazepines, Behavioral Neuroscience, chemistry.chemical_compound, Saccharin, medicine, Animals, Ro15-4513, Biological Psychiatry, Ethanol, Classical conditioning, Rats, Inbred Strains, Rats, chemistry, Anesthesia, Taste aversion, Conditioning, Psychology, psychological phenomena and processes, medicine.drug

Abstract

The ability of Ro15-4513, an imidazobenzodiazepine inverse benzodiazepine agonist, to attenuate/block the acquisition of an ethanol (ETOH)-induced conditioned taste aversion (CTA) was investigated in two experiments. Experiment 1 examined the effects of Ro15-4513 (3 mg/kg) on rats' consumption of a novel saccharin solution under a traditional CTA paradigm. Experiment 2 examined the effects of Ro15-4513 (3 mg/kg) on rats' consumption of a novel saccharin solution under a preexposure CTA paradigm. Under the preexposure paradigm, rats were given Ro15-4513 immediately before each of five daily consecutive preexposure treatments prior to the initial conditioning day. To obtain maximal preexposure and unconditioned stimulus effects, a 2-g/kg dose of ETOH (20% v/v) was used in the present study. As previously reported, animals given ETOH following 20-min access to a novel saccharin solution established moderate to strong aversions, with the degree of aversion being directly related to the number of conditioning days. Experiment 1 showed that Ro15-4513 failed to alter the CTA induced by ETOH. Experiment 2 further showed that Ro15-4513 failed to block the preexposure effect exerted on the ETOH-mediated CTA. The results confirm previous reports regarding the failure of Ro15-4513 to disrupt an ETOH-induced CTA. These data are in agreement with a number of behavioral studies demonstrating the failure of Ro15-4513 to antagonize certain actions of ETOH. Moreover, the present study along with a previous report suggests that ETOH-induced CTA's do not appear to be mediated via actions at the GABA-BDZ receptor complex.

Published

1992

18. Neurobehavioral studies of ethanol reward and activation

Author

Michael J. Lewis and Harry L. June

Subjects

Health (social science), medicine.drug_class, medicine.medical_treatment, Central nervous system, Stimulation, Motor Activity, Pharmacology, Toxicology, Nervous System, Biochemistry, Behavioral Neuroscience, chemistry.chemical_compound, Neurochemical, Reward, medicine, Animals, Nervous System Physiological Phenomena, Ethanol, Behavior, Animal, General Medicine, Electric Stimulation, Stimulant, medicine.anatomical_structure, Neurology, chemistry, Facilitation, Brain stimulation reward, Depressant, Psychology, Neuroscience

Abstract

Although generally considered to be a depressant drug, ethanol has both stimulant and depressant effects on behavior. This biphasic action of ethanol may be related to its reinforcing effects and to the neurobehavioral events that occur with changes in blood alcohol concentration (BAC). Ethanol was found to reduce the threshold and increase response rates for brain stimulation reward (BSR) at lateral hypothalamic, but not ventral noradrenergic bundle brain sites. These effects were also found to only occur when testing occurred on the ascending limb of the BAC. Studies of the effects of ethanol on open-field activity showed that the stimulant effects of low doses of ethanol were also seen only during the ascending limb of the BAC; depression was usually found during the descending limb. Neurochemical data from other investigators suggest that the facilitation of BSR and stimulation of activity may be mediated by mesolimbie dopamine systems.

Published

1990

19. Dopamine and benzodiazepine-dependent mechanisms regulate the EtOH-enhanced locomotor stimulation in the GABAA alpha1 subunit null mutant mice

Author

Harry L June, Katrina L Foster, William J A Eiler, Joshua Goergen, Jason B Cook, Nathan Johnson, Boikai Mensah-Zoe, Jothan O Simmons, Wenyuan Yin, James M Cook, and Gregg E Homanics

Subjects

Flumazenil, Male, medicine.medical_specialty, medicine.drug_class, Dopamine, Stimulation, Self Administration, Pharmacology, Motor Activity, chemistry.chemical_compound, Benzodiazepines, Mice, Eticlopride, Internal medicine, Salicylamides, medicine, Animals, Humans, Drug Interactions, GABA Modulators, Mice, Knockout, SCH-23390, Benzodiazepine, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, Dopaminergic, Central Nervous System Depressants, Benzazepines, medicine.disease, Receptors, GABA-A, Mice, Inbred C57BL, Psychiatry and Mental health, Endocrinology, chemistry, Dopamine Antagonists, Reinforcement, Psychology, Ingestive behaviors, medicine.drug, Carbolines

Abstract

The present study investigated the role of the alpha1-containing GABA(A) receptors in the neurobehavioral actions of alcohol. In Experiment 1, mice lacking the alpha1 subunit (alpha1 (-/-)) were tested for their capacity to initiate operant-lever press responding for alcohol or sucrose. Alcohol intake in the home cage was also measured. In Experiment 2, the alpha1 (-/-) mice were injected with a range of alcohol doses (0.875-4.0 g/kg; i.p.) to evaluate the significance of the alpha1 subunit in alcohol's stimulant actions. In Experiment 3, we determined if the alcohol-induced stimulant effects were regulated via dopaminergic (DA) or benzodiazepine (BDZ)-dependent mechanisms. To accomplish this, we investigated the capacity of DA (eticlopride, SCH 23390) and BDZ (flumazenil, betaCCt) receptor antagonists to attenuate the alcohol-induced stimulant actions. Compared with wild-type mice (alpha1 (+/+)), the null mutants showed marked reductions in both EtOH and sucrose-maintained responding, and home-cage alcohol drinking. The null mutants also showed significant increases in locomotor behaviors after injections of low-moderate alcohol doses (1.75-3.0 g/kg). betaCCt, flumazenil, eticlopride, and SCH 23390 were able to attenuate the alcohol-induced stimulation in mutant mice, in the absence of intrinsic effects. These data suggest the alpha1 receptor plays an important role in alcohol-motivated behaviors; however, it also appears crucial in regulating the reinforcing properties associated with normal ingestive behaviors. Deleting the alpha1 subunit of the GABA(A) receptor appears to unmask alcohol's stimulatory effects; these effects appear to be regulated via an interaction of both DA- and GABA(A) BDZ-dependent mechanisms.

Published

2006

20. Blockade of GABA(A) receptors within the extended amygdala attenuates D(2) regulation of alcohol-motivated behaviors in the ventral tegmental area of alcohol-preferring (P) rats

Author

William J. A. Eiler and Harry L. June

Subjects

Male, medicine.medical_specialty, endocrine system, Mesolimbic pathway, Nucleus accumbens, Article, GABA Antagonists, Cellular and Molecular Neuroscience, Eticlopride, Extended amygdala, Dopamine, Internal medicine, mental disorders, Salicylamides, medicine, Animals, reproductive and urinary physiology, Pharmacology, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, Receptors, Dopamine D2, Ventral Tegmental Area, Central Nervous System Depressants, Amygdala, Receptors, GABA-A, Rats, Ventral tegmental area, Behavior, Addictive, Pyridazines, Drug Combinations, medicine.anatomical_structure, Endocrinology, nervous system, Dopamine receptor, GABAergic, Conditioning, Operant, Dopamine Antagonists, Female, Psychology, psychological phenomena and processes, medicine.drug

Abstract

The dopamine (DA) mesolimbic pathway, which originates from DA cell bodies within the ventral tegmental area (VTA), has been shown by various studies to play a role in the mediation of various drugs of abuse including alcohol (EtOH). It has been suggested that the VTA's control of EtOH reward is mediated in part by the D2 receptors within the VTA. These receptors may be under the regulation of reciprocal GABAergic inputs from forebrain components of the mesolimbic path such as the nucleus accumbens (NAcc), a classic EtOH reward substrate, and the bed nucleus of the stria terminalis, a substrate recently implicated in EtOH reinforcement, forming a self-regulating feedback loop. To test this hypothesis, D2 regulation of EtOH self-administration (SA) was evaluated by the microinfusion of the D2 antagonist eticlopride into the VTA of P rats, which produced profound reductions in EtOH SA in the highest (20.0 and 40.0microg) doses tested in both BST/VTA and NAcc/VTA implanted P rats. To determine the role of GABA in the mediation of EtOH SA, a 32.0ng dose the non-selective GABA antagonist SR 95531 was microinfused into the BST producing no effect on responding for EtOH and into the NAcc which lead to a reduction in EtOH responding. Finally, the hypothesis that GABA innervation of the VTA from the mesolimbic forebrain may influence EtOH SA was examined by the simultaneous infusion of eticlopride (40.0microg) into the VTA and SR 95531 (32.0ng) into either the BST or NAcc. This combination infusion completely attenuated the reduction in EtOH SA observed with the 40.0microg dose of eticlopride alone in both groups of animals. These results suggest that while the D2 receptors within the VTA regulate EtOH-motivated behaviors, this is modulated by GABAergic input from the mesolimbic forebrain, specifically from the BST and NAcc.

Published

2006

21. Decreased reward during acute alcohol withdrawal in rats selectively bred for low alcohol drinking

Author

Edward J. Rausch, Julia A. Chester, Harry L. June, and Janice C. Froehlich

Subjects

Male, medicine.medical_specialty, Health (social science), Alcohol Drinking, Alcohol, ACUTE ALCOHOL WITHDRAWAL, Stimulation, Toxicology, Biochemistry, Dysphoria, Stereotaxic Techniques, Behavioral Neuroscience, chemistry.chemical_compound, Drug withdrawal, Reward, Internal medicine, medicine, Animals, Medial forebrain bundle, Ethanol, Brain, Central Nervous System Depressants, General Medicine, medicine.disease, Electric Stimulation, Electrodes, Implanted, Rats, Substance Withdrawal Syndrome, Endocrinology, Neurology, chemistry, High alcohol, Anesthesia, Conditioning, Operant, Brain stimulation reward, medicine.symptom, Psychology

Abstract

We have previously hypothesized that increased sensitivity to the dysphoric-like or aversive effects of alcohol withdrawal following an initial exposure to alcohol might be associated with a genetic propensity to avoid alcohol. A decrease in brain reward function, as measured by an elevation in intracranial self-stimulation (ICSS) reward threshold, is one of the few methods available to model dysphoric-like or aversive effects of drug withdrawal in rats. We compared brain reward function during withdrawal following an initial exposure to alcohol in alcohol-naive rats selectively bred for high (HAD1 line) versus low (LAD1 line) voluntary alcohol consumption. Male HAD1 (n = 5) and LAD1 (n = 6) rats were implanted with unilateral electrodes in the medial forebrain bundle and trained to bar press for delivery of a 100 μA current that varied in frequency from 45 to 200 Hz. Responding for ICSS was generally stable within subjects across multiple experimental sessions on a given day and across several consecutive days prior to alcohol or water administration. ICSS responding was assessed in both rat lines prior to and at 12, 14, 16, 18, 20, and 24 h following a single intragastric infusion of alcohol (4.0 g/kg body weight) or water. Rats of the LAD1 line, but not those of the HAD1 line, exhibited a decrease in brain reward function as evidenced by a decrease in bar-press responding for ICSS and an increase in ICSS stimulation threshold during alcohol withdrawal. The results suggest that rats selectively bred for low alcohol drinking may experience dysphoric-like effects during withdrawal from an initial exposure to alcohol, while rats selectively bred for high alcohol drinking may not.

Published

2005

22. Central opioid receptors differentially regulate the nalmefene-induced suppression of ethanol- and saccharin-reinforced behaviors in alcohol-preferring (P) rats

Author

Peter F. McKay, Marin Garcia, William J. A. Eiler, Dynesha Mason, Regat Seyoum, Harry L. June, Collette Grey, Stephanie E Hawkins, Katrina L. Foster, Shannan McCane, and Rancia Cummings

Subjects

Microinjections, medicine.drug_class, Narcotic Antagonists, Nucleus accumbens, Pharmacology, Functional Laterality, chemistry.chemical_compound, Saccharin, Opioid receptor, mental disorders, medicine, Animals, Nalmefene, Dose-Response Relationship, Drug, Ethanol, Narcotic antagonist, Brain, Central Nervous System Depressants, Rats, Inbred Strains, Naltrexone, Rats, Ventral tegmental area, Behavior, Addictive, Psychiatry and Mental health, medicine.anatomical_structure, nervous system, chemistry, Opioid, Receptors, Opioid, Conditioning, Operant, Female, Opiate, Psychology, Reinforcement, Psychology, psychological phenomena and processes, medicine.drug

Abstract

The exact opioid-sensitive receptors participating in EtOH-seeking behaviors remains unclear. Previous studies have reported higher densities of micro-opioid receptor binding in the nucleus accumbens (NACC) of P relative to NP rats; however, no differences were seen in delta-receptor binding. In contrast to the NACC, substantially lower levels of micro-receptor binding have been observed in the ventral tegmental area (VTA) of both P and NP rats, albeit no line differences have been observed. In the present study, opioid receptors in the NACC, VTA, and hippocampus were evaluated for their capacity to regulate both EtOH- and saccharin-motivated behaviors in the genetically selected alcohol-preferring (P) rat. To accomplish this, nalmefene, an opiate antagonist with preferential binding affinity for the micro-opioid receptor was unilaterally or bilaterally infused during concurrent availability of 1 h daily EtOH (10% v/v) and saccharin (0.025 or 0.050% w/v) solutions. Rats performed under a two-lever fixed ratio (FR) schedule in which four responses on one lever produced the EtOH solution, and four on a second lever produced the saccharin solution. The results demonstrated that when responding maintained by both EtOH and saccharin are matched at basal levels, unilateral (1-60 microg) or bilateral (0.5-10 microg) microinjections of nalmefene into the NACC produced selective dose-dependent reductions on responding maintained by EtOH. Unilateral (40, 60 microg) and bilateral (10 microg) VTA infusions were also observed to selectively reduced EtOH responding; however, greater nalmefene doses were required and the magnitude of suppression on EtOH responding was markedly less compared with the NACC. The greater sensitivity of nalmefene to suppress EtOH responding in the NACC is likely due to the greater number of opioid receptors in the NACC relative to the VTA. Only bilateral infusion of the 40 microg dose in the NACC and VTA suppressed responding maintained by both EtOH and saccharin. In contrast, intrahippocampal infusions dose dependently suppressed EtOH- and saccharin-maintained responding over a range of doses (1-20 microg). The present study provides evidence that nalmefene suppresses EtOH-motivated behaviors via blockade of opioid receptors within the NACC and VTA, and under various dose conditions both reinforcer and neuroanatomical specificity can be observed.

Published

2003

23. The reinforcing properties of alcohol are mediated by GABA(A1) receptors in the ventral pallidum

Author

Shannan McCane, Wenyuan Yin, Marin Garcia, Peter F. McKay, Dynesha Mason, Katrina L. Foster, William J. A. Eiler, Harry L. June, Collette Grey, Phil Skolnick, Regat Seyoum, James E. Woods, Scott C. Harvey, Chunrong Ma, Cecily M. Jones, Rancia Cummings, Michelle R. Carroll, P V V S Sarma, and James M. Cook

Subjects

Sucrose, Patch-Clamp Techniques, Time Factors, Microinjections, medicine.drug_class, Xenopus, Self Administration, Pharmacology, Nucleus accumbens, Motor Activity, Globus Pallidus, Partial agonist, Chlordiazepoxide, Membrane Potentials, Ventral pallidum, Adenosine A1 receptor, Saccharin, medicine, Inverse agonist, Animals, Drug Interactions, GABA-A Receptor Agonists, GABA-A Receptor Antagonists, Receptor, gamma-Aminobutyric Acid, Benzodiazepine, Ethanol, Drug Administration Routes, Body Weight, Receptors, GABA-A, Rats, Neostriatum, Psychiatry and Mental health, Alcoholism, Disease Models, Animal, Protein Subunits, Biochemistry, Alcohols, Sweetening Agents, Oocytes, Conditioning, Operant, Female, Reinforcement, Psychology, medicine.drug, Carbolines

Abstract

It has been hypothesized that alcohol addiction is mediated, at least in part, by specific gamma-aminobutyric acid(A) (GABA(A)) receptors within the ventral pallidum (VP). Among the potential GABA(A) receptor isoforms regulating alcohol-seeking behaviors within the VP, the GABA(A) alpha1 receptor subtype (GABA(A1)) appears pre-eminent. In the present study, we developed beta-carboline-3-carboxylate-t-butyl ester (betaCCt), a mixed agonist-antagonist benzodiazepine (BDZ) site ligand, with binding selectivity at the A1 receptor to explore the functional role of VP(A1) receptors in the euphoric properties of alcohol. The in vivo actions of betaCCt were then determined following microinfusion into the VP, a novel alcohol reward substrate that primarily expresses the A1 receptor. In two selectively bred rodent models of chronic alcohol drinking (HAD-1, P rats), bilateral microinfusion of betaCCt (0.5-40 microg) produced marked reductions in alcohol-reinforced behaviors. Further, VP infusions of betaCCt exhibited both neuroanatomical and reinforcer specificity. Thus, no effects on alcohol-reinforced behaviors were observed following infusion in the nucleus accumbens (NACC)/caudate putamen (CPu), or on response maintained by saccharin. Parenteral-administered betaCCt (1-40 mg/kg) was equally effective and selective in reducing alcohol-reinforced behaviors in P and HAD-1 rats. Additional tests of locomotor activity revealed that betaCCt reversed the locomotor sedation produced by both chlordiazepoxide (10 mg/kg) and EtOH (1.25 g/kg), but was devoid of intrinsic effects when given alone. Studies in recombinant receptors expressed in Xenopus oocytes revealed that betaCCt acted as a low-efficacy partial agonist at alpha3beta3gamma2 and alpha4beta3gamma2 receptors and as a low-efficacy inverse agonist at alpha1beta3gamma2, alpha2beta3gamma2, and alpha5beta3gamma2 receptors. The present study indicates that betaCCt is capable of antagonizing the reinforcing and the sedative properties of alcohol. These anti-alcohol properties of betaCCt are primarily mediated via the GABA(A1) receptor. betaCCt may represent a prototype of a pharmacotherapeutic agent to effectively reduce alcohol drinking behavior in human alcoholics.

Published

2003

24. A high affinity ligand for GABAA-receptor containing alpha5 subunit antagonizes ethanol's neurobehavioral effects in Long-Evans rats

Author

Katrina L. Foster, La Shone Williams, Marin Garcia, Shannan McCane, Collette Grey, James M. Cook, Harry L. June, Peter F. McKay, Xiaohui He, Dynesha Mason, and Rancia Cummings

Subjects

Male, endocrine system, medicine.medical_specialty, medicine.drug_class, Sedation, Alcohol, Motor Activity, Ligands, Open field, chemistry.chemical_compound, Benzodiazepines, Internal medicine, mental disorders, medicine, Inverse agonist, Animals, Drug Interactions, Rats, Long-Evans, GABA-A Receptor Antagonists, Receptor, Pharmacology, Benzodiazepine, Ethanol, Behavior, Animal, GABAA receptor, Rats, Protein Subunits, Endocrinology, chemistry, medicine.symptom, Reinforcement, Psychology

Abstract

Previously, we reported that the GABA(A)receptor containing alpha(5)subunit played a significant role in the reinforcing actions of EtOH in rats selectively bred to consume alcohol. However, the role of the alpha(5) receptor in regulating the neurobehavioral effects of EtOH in outbred rats is not known.In the present study, RY024, a novel benzodiazepine (BDZ) inverse agonist with high affinity (K(d) approximately 0.40 nM) and selectivity (approximately 67.3-fold) for the alpha(5)receptor, was investigated for its capacity to antagonize EtOH's reinforcing, motor impairing, and sedative effects in Long-Evans rats.Rats were trained to lever press for EtOH under a fixed-ratio 1 schedule of reinforcement. Subsequent studies evaluated EtOH's motor-impairing effects in an oscillating bar task, while EtOH's sedative effects were measured in the open field.RY024 (0.125-3.5 mg/kg; IP) markedly reduced EtOH-maintained responding with no effects on water responding, except for the highest dose. RY024 (3.0-15 mg/kg; IP) also reversed the motor impairing effects of a moderate (0.75 g/kg), and intoxicating EtOH dose (1.25 g/kg) in the absence of intrinsic effects. Finally, RY024 (7.5 mg/kg) attenuated the sedation produced by the 1.25 g/kg EtOH dose; however, it failed to attenuate the sedation induced by the 0.75 g/kg EtOH dose. Given alone, RY024 exhibited intrinsic effects in the open field.The results suggest the GABA(A)receptor containing alpha(5)subtype plays an important role in regulating the reinforcing, motor-impairing, and sedative effects of alcohol in outbred rats.

Published

2003

25. D1 dopamine receptor regulates alcohol-motivated behaviors in the bed nucleus of the stria terminalis in alcohol-preferring (P) rats

Author

Katrina L. Foster, Harry L. June, Chaz Mailey, Regat Seyoum, and William J. A. Eiler

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Naltrexone, Cellular and Molecular Neuroscience, Eticlopride, Dopamine, Internal medicine, Neural Pathways, Salicylamides, medicine, Animals, Injections, Intraventricular, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, Receptors, Dopamine D2, Receptors, Dopamine D1, Dopamine antagonist, Benzazepines, Rats, Ventral tegmental area, Behavior, Addictive, Stria terminalis, Alcoholism, medicine.anatomical_structure, Endocrinology, Dopamine receptor, Conditioning, Operant, Dopamine Antagonists, Female, Septal Nuclei, Psychology, Opioid antagonist, medicine.drug

Abstract

Recent studies have implicated the bed nucleus of the stria terminalis (BST) as a potential brain substrate for mediating drug-related behaviors. Neuroanatomical studies have demonstrated that reciprocal projections exist from the BST to the ventral tegmental area (VTA), a dopamine reward substrate proposed to play a role in alcohol abuse. In the present study, we evaluated the role of the D(1) and D(2) dopamine receptors of the BST in regulating alcohol and sucrose-motivated behaviors. Alcohol-preferring (P) rats were trained under an FR4 operant schedule to self-administer either EtOH (10% v/v) or sucrose (2% w/v). Following training, we evaluated the capacity of a competitive D(1) (SCH 23390; 0.5-20.0 microg) and a D(2) (eticlopride; 0.5-20.0 microg) dopamine antagonist to selectively reduce EtOH-maintained responding. Naltrexone, (5-30.0 microg), the nonselective opioid antagonist, was used as a reference agent. The results showed that SCH 23390 dose-dependently reduced alcohol-motivated responding. Responding was reduced with the 20.0 microg dose to about 97% of control levels. SCH 23390 also reduced sucrose responding; however, the magnitude of effects was substantially lower with the highest doses (2.5, 20.0 microg) (68-79% of control levels). In contrast, eticlopride failed to significantly alter alcohol responding and reduced sucrose responding only with the 10.0 microg dose. Unlike the dopamine antagonists, all naltrexone doses failed to alter EtOH or sucrose-maintained responding. The results suggest a salient role for the D(1), but not the D(2) and opioid receptors in selectively modulating EtOH-motivated behaviors in the BST.

Published

2003

26. Preclinical Models to Evaluate Potential Pharmacotherapeutic Agents in Treating Alcoholism and Studying the Neuropharmacological Bases of Ethanol‐Seeking Behaviors in Rats

Author

Harry L. June

Subjects

Male, medicine.medical_specialty, Reinforcement Schedule, Alcohol Drinking, Ethanol, Alcohol addiction, General Neuroscience, Drug Evaluation, Preclinical, Naltrexone, Rats, Behavior, Addictive, Alcoholism, Disease Models, Animal, medicine, Animals, Female, Psychiatry, Psychology

Abstract

The unit outlines four basic protocols designed to systematically evaluate the capacity of potential pharmacotherapeutic agents to effectively treat alcohol addiction and dependence in rats. Also included are procedures designed to study the neural mechanisms regulating alcohol-seeking behaviors.

Published

2002

27. GABA(A) receptors containing (alpha)5 subunits in the CA1 and CA3 hippocampal fields regulate ethanol-motivated behaviors: an extended ethanol reward circuitry

Author

Stephanie Rock, La Shone Williams, Rancia Cummings, Shannan McCane, Scott C. Harvey, Xiaohui He, Katrina L. Foster, Marin Garcia, Dynesha Mason, Collette Grey, James M. Cook, Timothy B. Johnson, Harry L. June, and Peter F. McKay

Subjects

medicine.medical_specialty, Patch-Clamp Techniques, Microinjections, Xenopus, Gene Expression, Self Administration, Nucleus accumbens, Hippocampus, Nucleus Accumbens, GABA Antagonists, chemistry.chemical_compound, Saccharin, Reward, Internal medicine, GABA-A receptor complex, mental disorders, medicine, Inverse agonist, Animals, Genetic Predisposition to Disease, GABA-A Receptor Agonists, GABA-A Receptor Antagonists, ARTICLE, Receptor, GABA Agonists, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, Chemistry, General Neuroscience, Ventral Tegmental Area, Rats, Inbred Strains, GABA receptor antagonist, Receptors, GABA-A, Rats, Ventral tegmental area, Behavior, Addictive, Protein Subunits, medicine.anatomical_structure, Endocrinology, Oocytes, RNA, ZK-93426, Female, Drug Antagonism

Abstract

GABA receptors within the mesolimbic circuitry have been proposed to play a role in regulating alcohol-seeking behaviors in the alcohol-preferring (P) rat. However, the precise GABA(A) receptor subunit(s) mediating the reinforcing properties of EtOH remains unknown. We examined the capacity of intrahippocampal infusions of an alpha5 subunit-selective ( approximately 75-fold) benzodiazepine (BDZ) inverse agonist [i.e., RY 023 (RY) (tert-butyl 8-(trimethylsilyl) acetylene-5,6-dihydro-5-methyl-6-oxo-4H-imidazo [1,5a] [1,4] benzodiazepine-3-carboxylate)] to alter lever pressing maintained by concurrent presentation of EtOH (10% v/v) and a saccharin solution (0.05% w/v). Bilateral (1.5-20 microgram) and unilateral (0.01-40 microgram) RY dose-dependently reduced EtOH-maintained responding, with saccharin-maintained responding being reduced only with the highest doses (e.g., 20 and 40 microgram). The competitive BDZ antagonist ZK 93426 (ZK) (7 microgram) reversed the RY-induced suppression on EtOH-maintained responding, confirming that the effect was mediated via the BDZ site on the GABA(A) receptor complex. Intrahippocampal modulation of the EtOH-maintained responding was site-specific; no antagonism by RY after intra-accumbens [nucleus accumbens (NACC)] and intraventral tegmental [ventral tegmental area (VTA)] infusions was observed. Because the VTA and NACC contain very high densities of alpha1 and alpha2 subunits, respectively, we determined whether RY exhibited a "negative" or "neutral" pharmacological profile at recombinant alpha1beta3gamma2, alpha2beta3gamma2, and alpha5beta3gamma2 receptors expressed in Xenopus oocytes. RY produced "classic" inverse agonism at all alpha receptor subtypes; thus, a neutral efficacy was not sufficient to explain the failure of RY to alter EtOH responding in the NACC or VTA. The results provide the first demonstration that the alpha5-containing GABA(A) receptors in the hippocampus play an important role in regulating EtOH-seeking behaviors.

Published

2001

28. The delta 2-opioid receptor antagonist naltriben reduces motivated responding for ethanol

Author

Shannan McCane, Ting-Kai Li, Harry L. June, Janice C. Froehlich, Richard W. Zink, and Philip S. Portoghese

Subjects

Reinforcement Schedule, Alcohol Drinking, medicine.drug_class, Narcotic Antagonists, (+)-Naloxone, Pharmacology, chemistry.chemical_compound, Opioid receptor, Receptors, Opioid, delta, medicine, Animals, Saccharin, Motivation, Ethanol, Naloxone, Antagonist, Central Nervous System Depressants, Rats, Inbred Strains, Receptor antagonist, Naltrexone, Rats, chemistry, Naltriben, Conditioning, Operant, Female, Psychology, Self-administration, Opioid antagonist, medicine.drug, Alcohol Deterrents

Abstract

Rationale: Given that alcoholics drink for different reasons, it is not likely that a single pharmacotherapeutic agent will be equally effective for all alcoholics. Hence, the development of new pharmacotherapeutic agents that are capable of reducing alcohol intake remains an important focus in the field of alcohol research. Objective: The objective of the present study was to examine the effects of the δ2 receptor antagonist naltriben (0.60–4.0 mg/kg) on operant responding maintained by the presentation of ethanol (EtOH) or saccharin in alcohol-preferring (P) rats. Methods: P rats were trained under a concurrent schedule [fixed ratio (FR)4–FR4] to press one lever for EtOH (10% v/v) and another for saccharin (0.0125–0.05% w/v) during a 60-min session. Naloxone, a non-specific opioid receptor antagonist, served as a reference antagonist. Results: When responding maintained by EtOH and saccharin were equated under baseline conditions, naloxone (0.003125–0.75 mg/kg) reduced levels of EtOH-maintained responding by 46–82%. None of the naloxone doses significantly reduced responding maintained by saccharin. Naltriben (0.9–4.0 mg/kg) reduced EtOH-maintained responding by 44–76%, while saccharin-maintained responding was reduced only by the highest dose of naltriben (4.0 mg/kg). Analysis of the EtOH within-session response pattern revealed that naloxone suppressed EtOH-maintained responding during the entire operant session and led to early termination of responding. Low doses of naltriben (0.90 mg/kg and 1.2 mg/kg) suppressed responding during the latter portion of the operant session, while higher doses (2.0, 3.0, 4.0 mg/kg) decreased responding during the entire session and led to early termination of responding. Conclusions: The results of the present study strengthen previous reports from our laboratory suggesting that naltriben, the selective δ2 opioid receptor antagonist, suppresses EtOH self-administration in rats selectively bred for high EtOH consumption. The results also suggest that naltriben may be a potential candidate for use as a pharmacotherapeutic agent in the treatment of EtOH dependence.

Published

1999

29. Buprenorphine alters ethanol self-administration in rats: dose-response and time-dependent effects

Author

Harry L. June, Charity R Cason, Michael J. Lewis, and Shen-Hsing Annabel Chen

Subjects

Male, Thebaine, Time Factors, Drinking, Self Administration, Pharmacology, Partial agonist, Rats, Sprague-Dawley, chemistry.chemical_compound, medicine, Animals, Ethanol, Dose-Response Relationship, Drug, business.industry, Buprenorphine, Rats, Analgesics, Opioid, Dose–response relationship, chemistry, Opioid, Toxicity, business, Self-administration, medicine.drug

Abstract

Buprenorphine is a partial opioid agonist derived from thebaine and has high affinity for mu and kappa opioid receptors. The present study investigated dose-response (0.03, 0.15, 0.3, 3 mg/kg) and time-dependent effects of buprenorphine (1.5 or 4 h post-treatment) on EtOH self-administration in outbred Sprague-Dawley rats. Freely feeding and drinking rats were trained to initiate EtOH self-administration for 1 h daily using the ascending concentration procedure, wherein they were provided with increasing concentrations of EtOH at 2, 5, 7, 9 and 11% (v/v), respectively. Water was concurrently available with each concentration. Animals were maintained on a given concentration of EtOH for 5 days. By day 21, animals began their stabilization on the 11% regimen and remained on this concentration throughout the remainder of the study. EtOH and water consumption were recorded daily at both 10- and 60-min intervals. At 1.5 h post-buprenorphine, all test doses greatly suppressed both EtOH and water intake at the 10-min interval. At the 60-min interval, all but the lowest dose (0.03 mg/kg) significantly suppressed EtOH intake, while only the highest dose (3 mg/kg) suppressed water intake. In contrast to the suppressant profile observed at 1.5 h post-buprenorphine, at 4 h post-buprenorphine the lower doses (0.03 and 0.15 mg/kg) significantly increased EtOH intake while the higher doses (0.3 and 3 mg/kg) continued to suppress intake. None of the doses of buprenorphine altered water intake 4 h post-buprenorphine. The results support previous research demonstrating the utility of low doses of buprenorphine in suppressing behavior rewarded by a non-opioid drug.

Published

1998

30. The effects of the novel benzodiazepine receptor inverse agonist Ru 34000 on ethanol-maintained behaviors

Author

Anila Ricks-Cord, Jana Delong, Charity R Cason, La Franze Durr, Connease Warren-Reese, Harry L. June, and Mary W Eggers

Subjects

Male, Receptor complex, medicine.drug_class, Injections, Subcutaneous, Pharmacology, chemistry.chemical_compound, medicine, Inverse agonist, Animals, GABA-A Receptor Agonists, Receptor, Saccharin, GABA Agonists, Injections, Intraventricular, Benzodiazepine, Behavior, Animal, Dose-Response Relationship, Drug, Ethanol, Chemistry, GABAA receptor, Ventral Tegmental Area, Central Nervous System Depressants, Rats, Inbred Strains, Rats, Pyrimidines, Mechanism of action, Flumazenil, Conditioning, Operant, medicine.symptom, Reinforcement, Psychology, Injections, Intraperitoneal, medicine.drug

Abstract

Ru 34000 [5-ethyl-7-methoxy-imidazo (1,2-a) pyrimidin-2-yl cyclopropyl methanone] is a novel imidazopyrimidine benzodiazepine inverse agonist that exhibits low affinity for central benzodiazepine receptors (Ki approximately 0.98 microM). The present study examined the in vivo actions of Ru 34000 (0.5-5 mg/kg) following intraperitoneal (i.p.), subcutaneous (s.c), oral (p.o.), and intraventral tegmental administration in alcohol-preferring (P) rats trained under a concurrent operant schedule (FR4-FR4) for ethanol (10% v/v) and a palatable saccharin (0.025% or 0.75% w/v) reinforcer. Ru 34000 (i.p., s.c., p.o.) markedly reduced ethanol responding by 28-96% of control levels without affecting saccharin responding, except for the highest dose level. Clear dose-dependent suppressant effects were observed with all routes of administration on ethanol responding. Flumazenil [ethyl-8-fluro-5, 6-dihydro-5-methyl-6-4H-imidazo [1,5-a]-[1,4]-benzodiazepine-3-carboxylate] (6 mg/kg; i.p.), a benzodiazepine receptor antagonist reversed the Ru 34000-reduction of ethanol responding, suggesting that the effects were mediated at the benzodiazepine receptor. Bilateral microinjections of Ru 34000 (50, 100, 200 ng) into the ventral tegmental area dose-dependently reduced ethanol responding by as much as 97% of control levels. The results suggest that the in vivo actions of Ru 34000 are determined not only by its binding affinity, but also by its bioavailability at active benzodiazepine sites and route of drug administration. Low affinity imidazopyrimidines may be useful pharmacological probes to further understand the role of the GABA(A)-benzodiazepine receptor complex in ethanol motivated behaviors.

Published

1998

31. GABAA-benzodiazepine receptors in the striatum are involved in the sedation produced by a moderate, but not an intoxicating ethanol dose in outbred Wistar rats

Author

Tong Gan, James M. Cook, Harry L. June, Charity R Cason, Ruiyan Lui, and Greg Cheatham

Subjects

Flumazenil, Male, medicine.medical_specialty, Azides, medicine.drug_class, GABA Agents, Xenopus, Striatum, Open field, Benzodiazepines, Internal medicine, medicine, Inverse agonist, Animals, Hypnotics and Sedatives, GABA-A Receptor Agonists, Rats, Wistar, Receptor, Molecular Biology, Benzodiazepine, Analysis of Variance, Ethanol, GABAA receptor, Chemistry, General Neuroscience, Antagonist, Receptors, GABA-A, Corpus Striatum, Rats, Pyridazines, Endocrinology, Oocytes, GABAergic, Neurology (clinical), Alcoholic Intoxication, Developmental Biology

Abstract

The role of the dorsal striatum in mediating the sedation produced by a moderate (0.75 g/kg) and an intoxicating (1.25 g/kg) EtOH dose was investigated in the open field by determining the capacity of direct intrastriatal injections of RY 008, a partial inverse agonist of the benzodiazepine (BDZ) receptor, to antagonize EtOH's effects. SR 95531, the competitive high-affinity GABA A antagonist was used as a reference compound. Intrastriatal RY 008 (50, 500 ng) and SR 95531 (50 ng) antagonized the sedation produced by the 0.75 g/kg EtOH dose. However, RY 008 did not alter the sedation produced by the 1.25 g/kg dose. RY 008 alone was without effect. RY 008 also failed to negatively modulate GABAergic function at α 1 β 2 γ 2 or α 6 β 2 γ 2 receptor subtypes expressed in Xenopus oocytes . Intrastriatal modulation of the moderate EtOH dose was site specific: no antagonism by RY 008 after intraaccumbens infusions was observed. The results suggest that central GABA A -BDZ receptors in the dorsal striatum play an important role in mediating the sedation produced by a moderate EtOH dose in the open field.

Published

1998

32. Benzodiazepine receptor ligands with different intrinsic efficacies alter ethanol intake in alcohol-nonpreferring (NP) rats

Author

Margaret Lin, James M. Murphy, Ting-Kai Li, Robert L. Hewitt, Jackie J. Mellor-Burke, Terri L. Greene, Harry L. June, and Lawrence Lumeng

Subjects

Male, medicine.medical_specialty, Receptor complex, Time Factors, FG-7142, Partial agonist, chemistry.chemical_compound, DMCM, Internal medicine, medicine, Inverse agonist, Animals, Dose Reduced, Glucans, Pharmacology, Analysis of Variance, Ethanol, Dose-Response Relationship, Drug, Bretazenil, Azepines, Receptors, GABA-A, Rats, Psychiatry and Mental health, Endocrinology, chemistry, Anesthesia, medicine.drug

Abstract

Benzodiazepine (BDZ) receptor ligands with varying intrinsic efficacies [RO19-4603, 0.02-0.15 mg/kg; FG 7142 1-16 mg/kg; DMCM, 1-8 mg/kg; RO16-6028 (bretazenil), 8-32 mg/kg] in modulating GABAergic activity were examined for the ability to alter palatability-induced ethanol (EtOH) intake in the alcohol-nonpreferring (NP) line of rats. NP rats on a 22-hour fluid-deprivation schedule were given 2-hour daily access to a 10% (v/v) EtOH/3% (g/v) polycose solution and water. Average EtOH intake was 2.1 +/- 0.2 g/kg/2 hours, and water intake was 17.1 +/- 0.9 ml/2 hours. During the initial 15 minutes of the 2-hour session, RO19-4603, the imidazothienodiazepine partial inverse agonist reduced EtOH intake to 19% of control values at 0.04 mg/kg and completely suppressed drinking of the EtOH solution at 0.15 mg/kg. Twenty-four-hour postdrug administration, the 0.08-mg/kg dose of RO19-4603 completely suppressed drinking of the EtOH solution at the 60-minute interval, and the 0.15-mg/kg dose reduced intake to 20% of control levels at the 15-minute interval. FG 7142, the partial beta-carboline inverse agonist reduced EtOH drinking at the 60-minute interval with the 1-mg/kg dose, and the 16-mg/kg dose reduced water intake at the 15-minute interval. DMCM, the full beta-carboline inverse agonist, significantly reduced water intake at 15 minutes (4 and 8 mg/kg), and the same doses caused a substantial increase in EtOH drinking at the 120-minute interval. The anxiolytic agent bretazenil (16 and 32 mg/kg) increased EtOH consumption during the initial 15 minutes to 270% to 425% of control levels, and water intake increased by the end of the 2-hour session to as much as 210% of control following administration of the 32-mg/kg dose. These findings support existing evidence suggesting that BDZ receptor ligands may modify neuronal processes that mediate some reinforcing and/or aversive properties of alcohol. They further demonstrate a potential importance of the GABAA-BDZ receptor complex in mediating palatability- (environmentally) induced EtOH drinking even in rats selectively bred for low alcohol preference.

Published

1996

33. The benzodiazepine inverse agonist RO19-4603 exerts prolonged and selective suppression of ethanol intake in alcohol-preferring (P) rats

Author

Lawrence Lumeng, James M. Murphy, Harry L. June, Ting-Kai Li, and Jackie J. Mellor-Burke

Subjects

medicine.medical_specialty, Receptor complex, Alcohol Drinking, medicine.drug_class, Drinking, chemistry.chemical_compound, Reward, Internal medicine, mental disorders, medicine, Inverse agonist, Animals, GABA-A Receptor Agonists, Pharmacology, Benzodiazepine, Ethanol, Dose-Response Relationship, Drug, Chemistry, Azepines, Alcohol preferring, Effective dose (pharmacology), Rats, Dose–response relationship, Endocrinology, Female, Ethanol intake, Alcohol Deterrents

Abstract

The time course of the benzodiazepine (BDZ) inverse agonist RO19-4603 in antagonizing ethanol (EtOH) intake was investigated in alcohol-preferring (P) rats (n=7) maintained on 24-h continuous free-choice access to EtOH (10% v/v), water, and food. After fluid intakes had stabilized over several weeks, animals were injected with Tween-80 vehicle solution or RO19-4603 (0.075, 0.150, and 0.30 mg/kg). EtOH and water intakes were determined at 8- and 24-h intervals. RO19-4603 caused a marked attenuation of EtOH drinking with each of the doses tested. EtOH intake during the 8-h following 0.075, 0.150, and 0.30 mg/kg RO19-4603 was decreased by approximately 36, 74, and 57%, respectively. Intakes during the 24-h interval were similar to the vehicle control condition. However, 32 h post-drug administration, EtOH intakes were reduced to approximately 27, 31, and 29% following the 0.075, 0.150 and 0.30 mg/kg doses, respectively. To further confirm the reliability of the RO19-4603 dose-response effect, and its selectivity for EtOH, the highest dose condition (0.30 mg/kg) was tested twice. The second 0.30 mg/kg dose condition exerted a profile of effects similar to the initial treatment; 8 h following administration, intake was decreased to 60% of the control level, and 32 h post-drug administration intake was decreased to approximately 46% of the controls. These decreases were evidently selective in comparison with water, since water drinking showed compensatory increases which paralleled the decreased EtOH consumption. Dose-response comparisons indicated that 0.150 mg/kg approaches the maximum effective dose, since the 0.30 mg/kg dose of RO19-4603 did not produce an additional decrease in EtOH intake. Furthermore, unlike the lower doses, the 0.30 mg/kg dose failed to yield reliable compensatory increases in water drinking. The results demonstrated that a single acute administration of RO19-4603 produces prolonged and selective suppression of EtOH intake in P rats maintained on 24-h continuous free access to EtOH. While it is not clear at present what properties of the ligand might explain the observed effects on EtOH intake, these findings along with our previous work, clearly suggest that RO19-4603 may modify neuronal processes that promote EtOH self-administration. Neural transmission at the GABAA-BDZ receptor complex may play an important role in mediating EtOH reinforcement.

Published

1994

34. Ethanol self-administration in freely feeding and drinking rats: effects of Ro15-4513 alone, and in combination with Ro15-1788 (flumazenil)

Author

Roger W. Hughes, Harry L. June, Michael J. Lewis, and Holly L. Spurlock

Subjects

Agonist, Flumazenil, Male, Azides, Alcohol Drinking, medicine.drug_class, Pharmacology, Rats, Sprague-Dawley, Benzodiazepines, medicine, Animals, Drug Interactions, GABA-A Receptor Agonists, Ro15-4513, Benzodiazepine, Dose-Response Relationship, Drug, Ethanol, GABAA receptor, Chemistry, Receptor antagonist, Rats, Conditioning, Operant, Antagonism, Self-administration, Reinforcement, Psychology, medicine.drug

Abstract

Recent work in our laboratory demonstrated that Ro15-4513, a partial inverse benzodiazepine (BDZ) agonist, decreases ethanol (ETOH) self-administration in rodents under fluid deprivation conditions. The present study further examined the effects of Ro15-4513 (2.5 and 5.0 mg/kg) alone and in combination with Ro15-1788, (flumazenil) (8.0 and 16.0 mg/kg), a BDZ receptor antagonist on ETOH self-administration in freely feeding and drinking rats. Animals were trained to consume ETOH (11% v/v) using a limited access procedure. Measurements were taken at 10- and 60-min intervals. Ro15-4513 (2.5 and 5.0 mg/kg) markedly attenuated ETOH consumption at both intervals. The antagonistic actions of Ro15-4513 were completely blocked by the higher dose of flumazenil at both intervals; the lower dose failed to antagonize the Ro15-4513-induced reduction of ETOH intake. When flumazenil was given alone, both doses reduced ETOH self-administration at 60 min; although the magnitude of the antagonism was comparable to that of Ro15-4513 only with the highest does of flumazenil (16.0 mg/kg). Neither Ro15-4513 nor flumazenil alone or in combination significantly altered water intake at any of the tested doses. Rats pretreated with Ro15-4513 showed a substantial reduction in blood ethanol concentration (BEC) compared with the Tween-80 vehicle condition at the 10-min interval. However, the BEC of animals given Ro15-4513 in combination with flumazenil were similar to rats given Tween-80 vehicle. The present study extends our previous research by demonstrating that Ro15-4513 and flumazenil attenuate ETOH self-administration in non-food or water deprived rats. These studies suggest that the suppressant effects of Ro15-4513 and flumazenil on ETOH self-administration are associated with actions at the BDZ site of the GABAA receptor complex. These data are discussed in relation to the possible mechanism(s) by which Ro-15-4513 and flumazenil exert their antagonism on ETOH self-administration.

Published

1994

35. Ro15-4513 enhances and attenuates motor stimulant effects of ethanol in rats

Author

Michael J. Lewis and Harry L. June

Subjects

Male, Azides, medicine.medical_specialty, Health (social science), medicine.medical_treatment, Stimulation, Motor Activity, Toxicology, Biochemistry, Open field, Benzodiazepines, Behavioral Neuroscience, chemistry.chemical_compound, Neurochemical, Internal medicine, medicine, Animals, Drug Interactions, Ro15-4513, Ethanol, Chemistry, Low activity, Rats, Inbred Strains, Long-term potentiation, General Medicine, Receptors, GABA-A, Rats, Stimulant, Endocrinology, Neurology, Anesthesia, medicine.drug

Abstract

The actions of the imidazobenzodiazepine, Ro15-4513 (2.5 mg/kg IP), ethanol (0.50 g/kg, 0.75 g/kg, 1.25 g/kg), and Ro15-4513 in combination with ethanol were assessed using low activity male Charles River (CD) rats. Horizontal (ambulatory) and nonhorizontal (rearing, grooming, etc.) activity were measured in the open field with a Digiscan activity system. When Ro15-4513 was given alone, animals responded in a manner similar to that of the control animals. Ethanol alone, however, resulted in a significant enhancement of activity, with the effect being most pronounced at 0.50 g/kg for horizontal activity and 1.25 g/kg for nonhorizontal activity. A potentiation of the ethanol-induced stimulant effect was observed following pretreatment with Ro15-4513 on the horizontal activity measure for the 1.25 g/kg ethanol group. An attenuation of activity was observed for this group on the nonhorizontal activity measure. Ro15-4513, however, did not affect the stimulation produced by the other doses of ethanol on the nonhorizontal measure. The results suggest that possibility of distinct neurochemical mechanisms in the mediation of horizontal and nonhorizontal activity and that, perhaps, GABA-benzodiazepine mechanisms may play different roles in mediating their ETOH-induced stimulant effect.

Published

1989

36. Ro15-4513 antagonizes depression of open-field horizontal activity by ethanol in rats

Author

Harry L. June, Michael J. Lewis, and Lynelle T. Johnson

Subjects

Male, endocrine system, medicine.medical_specialty, Azides, Health (social science), Motor Activity, Toxicology, Biochemistry, Open field, Behavioral Neuroscience, chemistry.chemical_compound, Benzodiazepines, Internal medicine, mental disorders, medicine, Animals, Ro15-4513, reproductive and urinary physiology, Depression (differential diagnoses), Ethanol, Rats, Inbred Strains, General Medicine, Rats, Endocrinology, Neurology, chemistry, Anesthesia, Psychology, medicine.drug

Abstract

The imidazobenzodiazepine, Ro15-4513, has been shown to antagonize some of the behavioral effects of ethanol (ETOH). In rats having relatively little experience in the open field, the actions of ETOH (0.75 g/kg IP), Ro15-4513 (1.25 mg/kg and 2.5 mg/kg, IP), and Ro15-4513 in combination with ETOH were measured on horizontal activity. Rats receiving ETOH showed a significant depression in horizontal activity. Doses of Ro15-4513 given alone produced no significant differences in activity from baseline levels. Rats pretreated with Ro15-4513 prior to receiving ETOH, however, showed a significant attenuation of the ETOH induced depression of activity. These results indicate that Ro15-4513 is effective in attenuating the depressive effects of ETOH in the open field in rats having little experience in the apparatus.

Published

1989