Your search keyword '"Marcia J. Ramaker"' showing total 14 results

1. Examining the effects of the histone methyltransferase inhibitor BIX-01294 on histone modifications and gene expression in both a clinical population and mouse models.

Author

Kayla A Chase, Benjamin Feiner, Marcia J Ramaker, Edward Hu, Cherise Rosen, and Rajiv P Sharma

Subjects

Medicine, Science

Abstract

Schizophrenia has been consistently characterized by abnormal patterns of gene down-regulation, increased restrictive chromatin assemblies, and reduced transcriptional activity. Histone methyltransferase (HMT) mRNA and H3K9me2 levels are elevated in postmortem brain and peripheral blood cells of persons with schizophrenia. Moreover, this epigenomic state likely contributes to the disease, as HMT levels correlate with clinical symptomatology. This manuscript sought to establish the potential therapeutic value of the HMT inhibitor BIX-01294 (BIX). Human peripheral mononuclear cells (PBMC) from 24 individuals with schizophrenia and 24 healthy individuals were cultured in the presence of BIX (5uM or 10uM). Mice were given once daily intraperitoneal injections of BIX (0.5 or 1mg/kg) for one week. Cultured cells, mouse cortex, or striatum was harvested, RNA extracted and RT-PCR conducted for several schizophrenia candidate genes: IL-6, Gad1, Nanog, KLF4, Reln, and Bdnf9a. Total H3K9me2 levels were measured using western blot while H3K9me2 binding to selected genes of interest was conducted using chromatin immunoprecipitation (ChIP). Neuronal subtype-specific BDNF conditional knockdown was conducted using the cre/lox system of mutant animals. Treatment with BIX decreased H3K9me2 and increased selected mRNA levels in cultured PBMCs from both normal controls and participants with schizophrenia. In mice, peripheral administration of BIX decreased cortical H3K9me2 levels and increased schizophrenia candidate gene expression. In BDNF conditional knockdown animals, BIX administration was able to significantly rescue Bdnf9a mRNA levels in ChAT and D1 Bdnf conditional knockdown mice. The results presented in this manuscript demonstrate a potential for further research into the clinical effectiveness of histone modifying pharmacology in the treatment of schizophrenia.

Published

2019

2. Identification of a novel, fast-acting GABAergic antidepressant

Author

Amanda M. Barkley-Levenson, Marcia J. Ramaker, Leggy A. Arnold, Margaret L. Guthrie, Katherine M.J. McMurray, Abraham A. Palmer, M K Reddy, James M. Cook, Viresh H. Rawal, Preetpal S. Sidhu, P K Elkin, and Stephanie C. Dulawa

Subjects

Male, 0301 basic medicine, GABA Agents, Serotonin reuptake inhibitor, Prefrontal Cortex, Pharmacology, CREB, Hippocampus, Partial agonist, Article, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, medicine, Animals, Molecular Biology, Swimming, Depressive Disorder, Mice, Inbred BALB C, Fluoxetine, biology, Depression, Chemistry, Lactoylglutathione Lyase, Pyruvaldehyde, Antidepressive Agents, Tail suspension test, 3. Good health, Mice, Inbred C57BL, Psychiatry and Mental health, 030104 developmental biology, Hindlimb Suspension, biology.protein, Antidepressant, Female, Psychopharmacology, 030217 neurology & neurosurgery, Behavioural despair test, medicine.drug

Abstract

Current pharmacotherapies for depression exhibit slow onset, side effects and limited efficacy. Therefore, identification of novel fast-onset antidepressants is desirable. GLO1 is a ubiquitous cellular enzyme responsible for the detoxification of the glycolytic byproduct methylglyoxal (MG). We have previously shown that MG is a competitive partial agonist at GABA-A receptors. We examined the effects of genetic and pharmacological inhibition of GLO1 in two antidepressant assay models: the tail suspension test (TST) and the forced swim test (FST). We also examined the effects of GLO1 inhibition in three models of antidepressant onset: the chronic FST (cFST), chronic mild stress (CMS) paradigm, and olfactory bulbectomy (OBX). Genetic knockdown of Glo1 or pharmacological inhibition using two structurally distinct GLO1 inhibitors (S-bromobenzylglutathione cyclopentyl diester (pBBG) or methyl gerfelin (MeGFN)) reduced immobility in the TST and acute FST. Both GLO1 inhibitors also reduced immobility in the cFST after 5 days of treatment. In contrast, the serotonin reuptake inhibitor fluoxetine (FLX) reduced immobility after 14, but not 5 days of treatment. Furthermore, 5 days of treatment with either GLO1 inhibitor blocked the depression-like effects induced by CMS on the FST and coat state, and attenuated OBX-induced locomotor hyperactivity. Finally, 5 days of treatment with a GLO1 inhibitor (pBBG), but not FLX, induced molecular markers of the antidepressant response including brain-derived neurotrophic factor (BDNF) induction and increased phosphorylated cyclic-AMP response binding protein (pCREB) to CREB ratio in the hippocampus and medial prefrontal cortex (mPFC). Our findings indicate that GLO1 inhibitors may provide a novel and fast-acting pharmacotherapy for depression.

Published

2017

3. Examining the effects of the histone methyltransferase inhibitor BIX-01294 on histone modifications and gene expression in both a clinical population and mouse models

Author

Edward Hu, Cherise Rosen, Kayla A. Chase, Rajiv P. Sharma, Benjamin Feiner, and Marcia J. Ramaker

Subjects

0301 basic medicine, Male, Gene Expression, Biochemistry, Histones, Mice, 0302 clinical medicine, Mathematical and Statistical Techniques, Gene expression, Medicine and Health Sciences, Enzyme Inhibitors, Epigenomics, Cerebral Cortex, Gene knockdown, education.field_of_study, Multidisciplinary, biology, Statistics, Brain, Azepines, Animal Models, Histone Code, Histone, Experimental Organism Systems, Histone methyltransferase, Physical Sciences, Histone Methyltransferases, Medicine, Female, Epigenetics, Anatomy, Research Article, medicine.medical_specialty, Science, Population, Mouse Models, Research and Analysis Methods, 03 medical and health sciences, Kruppel-Like Factor 4, Model Organisms, Extraction techniques, Internal medicine, Mental Health and Psychiatry, DNA-binding proteins, medicine, Genetics, Animals, Humans, RNA, Messenger, Statistical Methods, education, Analysis of Variance, Biology and life sciences, Brain-Derived Neurotrophic Factor, Proteins, RNA extraction, Neostriatum, Reelin Protein, 030104 developmental biology, Endocrinology, Gene Expression Regulation, Mutation, biology.protein, Leukocytes, Mononuclear, Quinazolines, Schizophrenia, Animal Studies, Chromatin immunoprecipitation, 030217 neurology & neurosurgery, Mathematics

Abstract

Schizophrenia has been consistently characterized by abnormal patterns of gene down-regulation, increased restrictive chromatin assemblies, and reduced transcriptional activity. Histone methyltransferase (HMT) mRNA and H3K9me2 levels are elevated in postmortem brain and peripheral blood cells of persons with schizophrenia. Moreover, this epigenomic state likely contributes to the disease, as HMT levels correlate with clinical symptomatology. This manuscript sought to establish the potential therapeutic value of the HMT inhibitor BIX-01294 (BIX). Human peripheral mononuclear cells (PBMC) from 24 individuals with schizophrenia and 24 healthy individuals were cultured in the presence of BIX (5uM or 10uM). Mice were given once daily intraperitoneal injections of BIX (0.5 or 1mg/kg) for one week. Cultured cells, mouse cortex, or striatum was harvested, RNA extracted and RT-PCR conducted for several schizophrenia candidate genes: IL-6, Gad1, Nanog, KLF4, Reln, and Bdnf9a. Total H3K9me2 levels were measured using western blot while H3K9me2 binding to selected genes of interest was conducted using chromatin immunoprecipitation (ChIP). Neuronal subtype-specific BDNF conditional knockdown was conducted using the cre/lox system of mutant animals. Treatment with BIX decreased H3K9me2 and increased selected mRNA levels in cultured PBMCs from both normal controls and participants with schizophrenia. In mice, peripheral administration of BIX decreased cortical H3K9me2 levels and increased schizophrenia candidate gene expression. In BDNF conditional knockdown animals, BIX administration was able to significantly rescue Bdnf9a mRNA levels in ChAT and D1 Bdnf conditional knockdown mice. The results presented in this manuscript demonstrate a potential for further research into the clinical effectiveness of histone modifying pharmacology in the treatment of schizophrenia.

Published

2018

4. Dlgap1 knockout mice exhibit alterations of the postsynaptic density and selective reductions in sociability

Author

Noboru H. Komiyama, Seth G. N. Grant, Marcia J. Ramaker, Marcelo P. Coba, James A. Knowles, Stephanie C. Dulawa, Summer L. Thompson, and Emily V. Ho

Subjects

Male, 0301 basic medicine, Scaffold protein, Autism, lcsh:Medicine, Open field, Mice, 0302 clinical medicine, 2.1 Biological and endogenous factors, Aetiology, lcsh:Science, Prepulse inhibition, Mice, Knockout, Neurons, Pediatric, Multidisciplinary, Behavior, Animal, Mental Health, Schizophrenia, Knockout mouse, Female, Protein Binding, Knockout, Intellectual and Developmental Disabilities (IDD), Biology, Article, 03 medical and health sciences, Glutamatergic, Behavioral and Social Science, mental disorders, Genetics, medicine, Animals, Social Behavior, Behavior, Animal, lcsh:R, Neurosciences, Wild type, Post-Synaptic Density, medicine.disease, SAP90-PSD95 Associated Proteins, Brain Disorders, 030104 developmental biology, lcsh:Q, Neuroscience, Postsynaptic density, 030217 neurology & neurosurgery

Abstract

The scaffold protein DLGAP1 is localized at the post-synaptic density (PSD) of glutamatergic neurons and is a component of supramolecular protein complexes organized by PSD95. Gain-of-function variants of DLGAP1 have been associated with obsessive-compulsive disorder (OCD), while haploinsufficient variants have been linked to autism spectrum disorder (ASD) and schizophrenia in human genetic studies. We tested male and female Dlgap1 wild type (WT), heterozygous (HT), and knockout (KO) mice in a battery of behavioral tests: open field, dig, splash, prepulse inhibition, forced swim, nest building, social approach, and sucrose preference. We also used biochemical approaches to examine the role of DLGAP1 in the organization of PSD protein complexes. Dlgap1 KO mice were most notable for disruption of protein interactions in the PSD, and deficits in sociability. Other behavioral measures were largely unaffected. Our data suggest that Dlgap1 knockout leads to PSD disruption and reduced sociability, consistent with reports of DLGAP1 haploinsufficient variants in schizophrenia and ASD.

Published

2018

5. Differences in the reinstatement of ethanol seeking with ganaxolone and gaboxadol

Author

Tamara J. Phillips, Matthew M. Ford, Deborah A. Finn, and Marcia J. Ramaker

Subjects

Male, Agonist, Ganaxolone, Neuroactive steroid, medicine.drug_class, Population, Pregnanolone, Pharmacology, Article, Extinction, Psychological, chemistry.chemical_compound, medicine, Animals, education, GABA Agonists, education.field_of_study, Behavior, Animal, Ethanol, GABAA receptor, General Neuroscience, Allopregnanolone, Isoxazoles, Receptors, GABA-A, Mice, Inbred C57BL, chemistry, Psychology, Gaboxadol, medicine.drug

Abstract

The endogenous neuroactive steroid allopregnanolone (ALLO) has previously been shown to induce reinstatement of ethanol seeking in rodents. ALLO is a positive allosteric modulator at both synaptic and extrasynaptic GABA A receptors. The contribution of each class of GABA A receptors in mediating reinstatement of ethanol seeking is unknown. The first aim of the present study was to determine whether ganaxolone (GAN), a longer-acting synthetic analog of ALLO, also promotes reinstatement of ethanol seeking. The second aim was to examine whether preferentially activating extrasynaptic GABA A receptors with the selective agonist gaboxadol (THIP) was sufficient to reinstate responding for ethanol in mice. Male C57BL/6J mice were trained to lever press for access to a 10% ethanol (v/v) solution (10E), using a sucrose-fading procedure. Following extinction of the lever-pressing behavior, systemic THIP (0, 4 and 6 mg/kg) and GAN (0, 10, and 15 mg/kg) were tested for their ability to reinstate ethanol-appropriate responding in the absence of 10E access. GAN significantly increased lever pressing on the previously active lever, while THIP did not alter lever-pressing behavior. The results of this study suggest that direct activation of extrasynaptic GABA A receptors at the GABA site is not sufficient to induce ethanol seeking in the reinstatement procedure. Future studies are necessary to elucidate the mechanisms and brain areas by which differences in the pharmacological activity of GAN and THIP at the GABA A receptor contribute to the dissimilarity in their effect on the reinstatement of ethanol seeking. Nonetheless, based on the increased use of these drugs in clinical trials across multiple disease states, the effects of GAN or THIP on alcohol seeking may be an important consideration if these drugs are to be used clinically in a population with a co-occurring alcohol use disorder.

Published

2014

6. Effect of ganaxolone and THIP on operant and limited-access ethanol self-administration

Author

Deborah A. Finn, Moriah N. Strong, Matthew M. Ford, and Marcia J. Ramaker

Subjects

Male, Agonist, Ganaxolone, Time Factors, Neuroactive steroid, Alcohol Drinking, medicine.drug_class, Self Administration, Pregnanolone, Pharmacology, Article, Mice, Cellular and Molecular Neuroscience, chemistry.chemical_compound, medicine, Animals, GABA-A Receptor Agonists, Molecular Targeted Therapy, Nootropic Agents, Dose-Response Relationship, Drug, Ethanol, Chemistry, GABAA receptor, Allopregnanolone, Drugs, Investigational, Isoxazoles, Receptors, GABA-A, Mice, Inbred C57BL, Protein Subunits, Conditioning, Operant, Self-administration, Reinforcement, Psychology, Gaboxadol, Alcohol Deterrents, medicine.drug

Abstract

Recent evidence suggests that GABAA receptor ligands may regulate ethanol intake via effects at both synaptic and extrasynaptic receptors. For example, the endogenous neurosteroid, allopregnanolone (ALLO) has a similar pharmacological profile as ethanol, and it alters ethanol intake in rodent models. Additionally, recent evidence suggests that δ-subunit containing extrasynaptic GABAA receptors may confer high sensitivity to both ethanol and neurosteroids. The purpose of the present study was to determine the effects of ganaxolone (GAN; an ALLO analogue) and gaboxadol (THIP; a GABAA receptor agonist with selectivity for the extrasynaptic δ-subunit) on ethanol intake, drinking patterns, and bout characteristics in operant and limited access self-administration procedures. In separate studies, the effects of GAN (0 – 10 mg/kg) and THIP (2 – 16 mg/kg) were tested in C57BL/6J male mice provided with two-hour access to a two-bottle choice of water or 10% ethanol or trained to respond for 30 minutes of access to 10% ethanol. GAN had no overall significant effect on operant ethanol self-administration, but tended to decrease the latency to consume the first bout. In the limited-access procedure, GAN dose-dependently decreased ethanol intake. THIP dose-dependently decreased ethanol intake in both paradigms, altering both the consummatory and appetitive processes of operant self-administration as well as shifting the drinking patterns in both procedures. These results add to literature suggesting time-dependent effects of neurosteroids to promote the onset, and to subsequently decrease, ethanol drinking behavior, and they support a role for extrasynaptic GABAA receptor activation in ethanol reinforcement.

Published

2012

7. Ivermectin reduces alcohol intake and preference in mice

Author

Ronald L. Alkana, Nhat Huynh, Sheraz Khoja, Megan M. Yardley, Nicos A. Petasis, Letisha R. Wyatt, Stan G. Louie, Deborah A. Finn, Marco Bortolato, Liana Asatryan, Daryl L. Davies, and Marcia J. Ramaker

Subjects

Male, Alcohol Drinking, Drinking Behavior, Binge drinking, Self Administration, Alcohol, Pharmacology, Choice Behavior, Article, Mice, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Sex Factors, Ivermectin, medicine, Animals, Saccharin, Ethanol, Antiparasitic Agents, Dose-Response Relationship, Drug, urogenital system, Antiparasitic agent, Mice, Inbred C57BL, Tolerability, chemistry, embryonic structures, Conditioning, Operant, Female, Self-administration, Psychology, medicine.drug

Abstract

The high rate of therapeutic failure in the management of alcohol use disorders (AUDs) underscores the urgent need for novel and effective strategies that can deter ethanol consumption. Recent findings from our group showed that ivermectin (IVM), a broad-spectrum anthelmintic with high tolerability and optimal safety profile in humans and animals, antagonized ethanol-mediated inhibition of P2X4 receptors (P2X4Rs) expressed in Xenopus oocytes. This finding prompted us to hypothesize that IVM may reduce alcohol consumption; thus, in the present study we investigated the effects of this agent on several models of alcohol self-administration in male and female C57BL/6 mice. Overall, IVM (1.25-10 mg/kg, intraperitoneal) significantly reduced 24-h alcohol consumption and intermittent limited access (4-h) binge drinking, and operant alcohol self-administration (1-h). The effects on alcohol intake were dose-dependent with the significant reduction in intake at 9 h after administration corresponding to peak IVM concentrations (C(max)) in the brain. IVM also produced a significant reduction in 24-h saccharin consumption, but did not alter operant sucrose self-administration. Taken together, the findings indicate that IVM reduces alcohol intake across several different models of self-administration and suggest that IVM may be useful in the treatment of AUDs.

Published

2012

8. Alteration of Ethanol Drinking in Mice via Modulation of the GABAA Receptor with Ganaxolone, Finasteride, and Gaboxadol

Author

Matthew M. Ford, Deborah A. Finn, Andrea M. Fretwell, and Marcia J. Ramaker

Subjects

Agonist, Pregnanolone, medicine.medical_specialty, Ganaxolone, Ethanol, Neuroactive steroid, medicine.drug_class, Chemistry, GABAA receptor, Allopregnanolone, Medicine (miscellaneous), Pharmacology, Toxicology, Psychiatry and Mental health, chemistry.chemical_compound, Endocrinology, Internal medicine, medicine, Gaboxadol, medicine.drug

Abstract

Background: Neurosteroids and other γ-aminobutyric acidA (GABAA) receptor–modulating compounds have been shown to affect ethanol intake, although their mechanism remains unclear. This study examined how patterns of 24-hour ethanol drinking in mice were altered with the synthetic GABAergic neurosteroid ganaxolone (GAN), with an inhibitor of neurosteroid synthesis (finasteride [FIN]), or a GABAA receptor agonist with some selectivity at extrasynaptic receptors (gaboxadol HCL [THIP]). Methods: Male C57BL/6J mice had continuous access to a 10% v/v ethanol solution (10E) or water. Using lickometer chambers, drinking patterns were analyzed among mice treated in succession to GAN (0, 5, and 10 mg/kg), FIN (0 or 100 mg/kg), and THIP (0, 2, 4, 8, and 16 mg/kg). Results: GAN shifted drinking in a similar but extended manner to previous reports using low doses of the neurosteroid allopregnanolone (ALLO); drinking was increased in hour 1, decreased in hours 2 and 3, and increased in hours 4 and 5 postinjection. THIP (8 mg/kg) and FIN both decreased 10E drinking during the first 5 hours postinjection by 30 and 53%, respectively, while having no effect on or increasing water drinking, respectively. All 3 drugs altered the initiation of drinking sessions in a dose-dependent fashion. FIN increased and GAN decreased time to first lick and first bout. THIP (8 mg/kg) decreased time to first lick but increased time to first bout and attenuated first bout size. Conclusions: The present findings support a role for the modulation of ethanol intake by neurosteroids and GABAA receptor–acting compounds and provide hints as to how drinking patterns are shifted. The ability of THIP to alter 10E drinking suggests that extrasynaptic GABAA receptors may be involved in the modulation of ethanol intake. Further, the consistent results with THIP to that seen previously with high doses of ALLO suggest that future studies should further examine the relationship between neurosteroids and extrasynaptic GABAA receptors, which could provide a better understanding of the mechanism by which neurosteroids influence ethanol intake.

Published

2011

9. 799. Behavioral and Molecular Effects of Putative OCD Risk Gene BTBD3

Author

James A. Knowles, Marcia J. Ramaker, Madeline Klinger, Nuno Sousa, João Bessa, Summer L. Thompson, Jared W. Young, Emily V. Ho, M. Morais, Amanda C Welch, and Stephanie C. Dulawa

Subjects

Genetics, 0303 health sciences, 03 medical and health sciences, 0302 clinical medicine, Risk gene, Biology, 030217 neurology & neurosurgery, Biological Psychiatry, 030304 developmental biology

Published

2017

10. Effect of nucleus accumbens shell infusions of ganaxolone or gaboxadol on ethanol consumption in mice

Author

Matthew M. Ford, Marcia J. Ramaker, Tamara J. Phillips, Moriah N. Strong-Kaufman, and Deborah A. Finn

Subjects

Agonist, Male, Ganaxolone, medicine.medical_specialty, Neuroactive steroid, Alcohol Drinking, medicine.drug_class, Pregnanolone, Pharmacology, Nucleus accumbens, Article, Nucleus Accumbens, chemistry.chemical_compound, Mice, Internal medicine, medicine, Animals, GABA-A Receptor Agonists, Ethanol, Chemistry, GABAA receptor, Allopregnanolone, Isoxazoles, Receptors, GABA-A, Mice, Inbred C57BL, Endocrinology, Infusions, Intraventricular, Treatment Outcome, Gaboxadol, medicine.drug

Abstract

Allopregnanolone (ALLO) is an endogenous neuroactive steroid thought to alter the reinforcement value of alcohol (ethanol) due to its actions as a positive modulator of the GABAA receptor (GABAAR). Extrasynaptic GABAARs may be a particularly sensitive target of ethanol and neuroactive steroids. Previous work showed that systemic injections of an ALLO analog, ganaxolone (GAN), or an extrasynaptic GABAAR agonist (gaboxadol; THIP) decreased ethanol intake in male mice with limited access to ethanol. The present studies tested whether activation of GABAARs in the nucleus accumbens (NAc) shell by GAN or THIP was sufficient to reduce ethanol intake. C57BL/6J male mice had 2-h access to 10 % ethanol (10E) and water, and 10E intake was measured following site-specific infusions of GAN or THIP. Decreases in limited-access 10E consumption were observed following site-specific bilateral infusions of either drug into the NAc shell. Significant changes in intake were absent when the drugs were infused in a region dorsal to the target site (GAN) or into the lateral ventricle (THIP). Locomotor data confirmed that the decreases in intake were not due to a sedative effect of the drugs. These data demonstrate the sufficiency of GABAAR activation by a positive allosteric modulator or an agonist with selectivity for extrasynaptic GABAARs to decrease ethanol consumption in mice. Importantly, more refined GABAAR-active targets that decrease ethanol intake may enhance our understanding and ability to treat alcohol use disorders.

Published

2014

11. Quantification of ten neuroactive steroids in plasma in Withdrawal Seizure-Prone and -Resistant mice during chronic ethanol withdrawal

Author

Jeremiah P. Jensen, David J. Rossi, Melinda L. Helms, John C. Crabbe, Michelle A. Tanchuck-Nipper, Christopher Snelling, Matthew M. Ford, Marcia J. Ramaker, Debra K. Cozzoli, and Deborah A. Finn

Subjects

Male, medicine.medical_specialty, Neuroactive steroid, Endogeny, Pregnanolone, Pharmacology, Article, chemistry.chemical_compound, Mice, Neurochemical, Seizures, Internal medicine, medicine, Animals, Receptor, Neurotransmitter Agents, Ethanol, Chemistry, Allopregnanolone, Central Nervous System Depressants, Reproducibility of Results, Receptors, GABA-A, Tetrahydrodeoxycorticosterone, Substance Withdrawal Syndrome, Endocrinology, Chronic Disease, Pregnenolone, medicine.drug

Abstract

Rationale The rapid membrane actions of neuroactive steroids, particularly via an enhancement of γ-aminobutyric acidA receptors (GABAARs), participate in the regulation of central nervous systemexcitability. Priorevidencesuggestsan inverse relationship between endogenous GABAergic neuroactive steroid levels and behavioral changes in excitability during ethanol withdrawal. Objectives Previously, we found that ethanol withdrawal significantly decreased plasma allopregnanolone (ALLO) levels, a potent GABAergic neuroactive steroid, and decreased GABAAR sensitivity to ALLO in Withdrawal Seizure-Prone (WSP) but not in Withdrawal Seizure-Resistant (WSR) mice. However, the effect of ethanol withdrawal on levels of other endogenous GABAAR-active steroids is not known. Methods After validation of a gas chromatography-mass spectrometry method for the simultaneous quantification of ten neuroactive steroids, we analyzed plasma from control male WSP-1 and WSR-1 mice and during ethanol withdrawal. Results We quantified levels of nine neuroactive steroids in WSP-1 and WSR-1 plasma; levels of pregnanolone were not detectable. Basal levels of five neuroactive steroids were higher in WSR-1 versus WSP-1 mice. Ethanol withdrawal significantly suppressed five neuroactive steroids in WSP-1 and WSR-1 mice, including ALLO. Conclusions Due to lower basal levels of some GABAARactivesteroidsinWSP-1mice, awithdrawal-induceddecrease inWSP-1micemay havea greater physiologicalconsequence than a similar decrease in WSR-1 mice. Because WSP-1 mice alsoexhibit a reduction inGABAAR sensitivity to neuroactive steroids during withdrawal, it is possible that the combined decrease in neuroactive steroids and GABAAR sensitivity during ethanol withdrawal in WSP-1 mice represents a neurochemical substrate for severe ethanol withdrawal.

Published

2013

12. Recent advances in the discovery and preclinical testing of novel compounds for the prevention and/or treatment of alcohol use disorders

Author

Segev Barak, Marco Bortolato, Dorit Ron, Jing Liang, Richard W. Olsen, Deborah A. Finn, Daryl L. Davies, and Marcia J. Ramaker

Subjects

Drug Evaluation, Preclinical, Medicine (miscellaneous), Alcohol abuse, Craving, Alcohol, Purinergic Receptors, Pharmacology, Toxicology, chemistry.chemical_compound, Substance Misuse, Alcohol Use and Health, GABAA Receptors, Psychology, Molecular Targeted Therapy, High rate, Antiparasitic Agents, Dihydromyricetin, Substance Abuse, Preclinical, Alcohol-Induced Disorders, Psychiatry and Mental health, Alcoholism, Preclinical testing, 5.1 Pharmaceuticals, Alcohol intake, Mental health, medicine.symptom, Development of treatments and therapeutic interventions, medicine.medical_specialty, Herbal Medicine, Clinical Sciences, Article, Behavioral and Social Science, medicine, Effective treatment, Animals, Humans, Glial Cell Line-Derived Neurotrophic Factor, GABA-A Receptor Agonists, Intensive care medicine, Ivermectin, business.industry, Prevention, Neurosciences, Ligand-Gated Ion Channels, medicine.disease, Antiparasitic agent, Brain Disorders, Good Health and Well Being, chemistry, Drug Evaluation, Plant Preparations, business, Ganaxolone, Central Nervous System Agents

Abstract

Alcohol abuse and dependence have a staggering socio-economic impact, yet current therapeutic strategies are largely inadequate to treat these disorders. Thus, the development of new strategies that can effectively prevent alcohol use disorders is of paramount importance. Currently approved medications attempt to deter alcohol intake by blocking EtOH metabolism or by targeting the neurochemical systems downstream of the cascades leading to craving and dependence. Unfortunately, these medications have provided only limited success as indicated by the continued high rates of alcohol abuse and alcoholism. The lack of currently available effective treatment strategies is highlighted by the urgent call by the NIAAA to find new and paradigm-changing therapeutics to either prevent or treat alcohol-related problems. The present mini-review highlights recent findings from four laboratories with a focus on compounds that have the potential to be novel therapeutic agents that can be developed for the prevention and/or treatment of alcohol use disorders.

Published

2013

13. Alteration of ethanol drinking in mice via modulation of the GABA(A) receptor with ganaxolone, finasteride, and gaboxadol

Author

Marcia J, Ramaker, Matthew M, Ford, Andrea M, Fretwell, and Deborah A, Finn

Subjects

Male, Alcohol Drinking, Behavior, Animal, Dose-Response Relationship, Drug, Finasteride, Drinking Behavior, Isoxazoles, Pregnanolone, Receptors, GABA-A, Article, Mice, Inbred C57BL, Mice, Models, Animal, Animals, GABA-A Receptor Agonists

Abstract

Neurosteroids and other γ-aminobutyric acid(A) (GABA(A) ) receptor-modulating compounds have been shown to affect ethanol intake, although their mechanism remains unclear. This study examined how patterns of 24-hour ethanol drinking in mice were altered with the synthetic GABAergic neurosteroid ganaxolone (GAN), with an inhibitor of neurosteroid synthesis (finasteride [FIN]), or a GABA(A) receptor agonist with some selectivity at extrasynaptic receptors (gaboxadol HCL [THIP]).Male C57BL/6J mice had continuous access to a 10% v/v ethanol solution (10E) or water. Using lickometer chambers, drinking patterns were analyzed among mice treated in succession to GAN (0, 5, and 10 mg/kg), FIN (0 or 100 mg/kg), and THIP (0, 2, 4, 8, and 16 mg/kg).GAN shifted drinking in a similar but extended manner to previous reports using low doses of the neurosteroid allopregnanolone (ALLO); drinking was increased in hour 1, decreased in hours 2 and 3, and increased in hours 4 and 5 postinjection. THIP (8 mg/kg) and FIN both decreased 10E drinking during the first 5 hours postinjection by 30 and 53%, respectively, while having no effect on or increasing water drinking, respectively. All 3 drugs altered the initiation of drinking sessions in a dose-dependent fashion. FIN increased and GAN decreased time to first lick and first bout. THIP (8 mg/kg) decreased time to first lick but increased time to first bout and attenuated first bout size.The present findings support a role for the modulation of ethanol intake by neurosteroids and GABA(A) receptor-acting compounds and provide hints as to how drinking patterns are shifted. The ability of THIP to alter 10E drinking suggests that extrasynaptic GABA(A) receptors may be involved in the modulation of ethanol intake. Further, the consistent results with THIP to that seen previously with high doses of ALLO suggest that future studies should further examine the relationship between neurosteroids and extrasynaptic GABA(A) receptors, which could provide a better understanding of the mechanism by which neurosteroids influence ethanol intake.

Published

2011

14. Discrete Forebrain Neuronal Networks Supporting Noradrenergic Regulation of Sensorimotor Gating

Author

Abha K. Rajbhandari, Karen M Alsene, Marcia J. Ramaker, and Vaishali P. Bakshi

Subjects

Agonist, Male, Reflex, Startle, Quinpirole, medicine.drug_class, Nucleus accumbens, Biology, Hippocampus, Rats, Sprague-Dawley, Norepinephrine, Adrenergic Agents, Prosencephalon, Extended amygdala, Neural Pathways, medicine, Animals, Drug Interactions, Prepulse inhibition, Pharmacology, Brain Mapping, Dose-Response Relationship, Drug, Neural Inhibition, Sensory Gating, Amygdala, Rats, Psychiatry and Mental health, Stria terminalis, Drug Combinations, medicine.anatomical_structure, nervous system, Acoustic Stimulation, Forebrain, Dopamine Agonists, Original Article, Neuroscience, medicine.drug, Basolateral amygdala, Psychoacoustics

Abstract

Prepulse inhibition (PPI) refers to the reduction in the startle response when a startling stimulus is preceded by a weak prestimulus, and is an endophenotype of deficient sensorimotor gating in several neuropsychiatric disorders. Emerging evidence suggests that norepinephrine (NE) regulates PPI, however, the circuitry involved is unknown. We found recently that stimulation of the locus coeruleus (LC), the primary source of NE to the forebrain, induces a PPI deficit that is a result of downstream NE release. Hence, this study sought to identify LC-innervated forebrain regions that mediate this effect. Separate groups of male Sprague–Dawley rats received a cocktail solution of the α1-NE receptor agonist phenylephrine plus the β-receptor agonist isoproterenol (equal parts of each; 0, 3, 10, and 30 μg) into subregions of the medial prefrontal cortex (mPFC), nucleus accumbens (NAcc), extended amygdala, mediodorsal thalamus (MD-thalamus), or the dorsal hippocampus (DH) before PPI testing. NE agonist infusion into the posterior mPFC, NAcc shell, bed nucleus of the stria terminalis, basolateral amygdala, and the MD-thalamus disrupted PPI, with particularly strong effects in MD-thalamus. Sites in which NE receptor stimulation did not disrupt PPI (anterior mPFC, NAcc core, central amygdala, and DH) did support PPI disruptions with the dopamine D2 receptor agonist quinpirole (0, 10 μg). This pattern reveals new pathways in the regulation of PPI, and suggests that NE transmission within distinct thalamocortical and ventral forebrain networks may subserve the sensorimotor gating deficits that are seen in disorders such as schizophrenia, Tourette syndrome, and post-traumatic stress disorder.

Published

2011