Your search keyword '"Carla Maciag"' showing total 7 results

1. Anticonvulsant profile of the neuroactive steroid, SGE-516, in animal models

Author

Francesco G. Salituro, Gabriel Martinez Botella, James J. Doherty, Rebecca S. Hammond, Alison L. Althaus, Carla Maciag, Albert J. Robichaud, and Michael A. Ackley

Subjects

Male, 0301 basic medicine, Allosteric modulator, Neuroactive steroid, medicine.medical_treatment, Action Potentials, Convulsants, Pregnanolone, Pharmacology, Hippocampus, Rats, Sprague-Dawley, Fragile X Mental Retardation Protein, Mice, 03 medical and health sciences, Epilepsy, chemistry.chemical_compound, 0302 clinical medicine, Piperidines, Seizures, Convulsion, Kindling, Neurologic, Potassium Channel Blockers, medicine, Animals, gamma-Aminobutyric Acid, Mice, Knockout, Electroshock, GABAA receptor, Allopregnanolone, medicine.disease, Rats, Disease Models, Animal, 030104 developmental biology, Anticonvulsant, Neurology, Mechanism of action, chemistry, Pentylenetetrazole, Anticonvulsants, Neurology (clinical), medicine.symptom, 030217 neurology & neurosurgery

Abstract

Despite the availability of multiple antiepileptic drugs (AED), failure to adequately control seizures is a challenge for approximately one third of epilepsy patients, and new therapies with a differentiated mechanism of action are needed. The neuroactive steroid, SGE-516, is a positive allosteric modulator of both gamma- and delta-containing GABAA receptors. This broad GABAA receptor activity differentiates neuroactive steroids like SGE-516 from benzodiazepines, a class of anticonvulsants which have been shown in vitro to selectively target gamma-subunit containing GABAA receptors. As a neuroactive steroid, SGE-516 has pharmacokinetic properties that are intended to allow for chronic oral dosing. We investigated the anticonvulsant activity of SGE-516 across numerous in vitro and in vivo models of seizure activity. SGE-516 dose-dependently reduced neuronal firing rates and epileptiform activity in vitro. In mice, SGE-516 protected against acute seizures in the PTZ-induced chemo-convulsant seizure model and the 6Hz psychomotor seizure model. In addition, SGE-516 demonstrated anticonvulsant activity in the mouse corneal kindling model. These data suggest that SGE-516 may have potential for development as a novel oral AED for the treatment of refractory seizures.

Published

2017

2. Quetiapine and its metabolite norquetiapine: translation fromin vitropharmacology toin vivoefficacy in rodent models

Author

Thomas J. Hudzik, Michael W. Wood, Carla Maciag, Jianwei Liu, S. Nyberg, Alan J. Cross, Dan Widzowski, and Anna Zacco

Subjects

0301 basic medicine, Pharmacology, medicine.drug_class, business.industry, Atypical antipsychotic, Drug action, Anxiolytic, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, In vivo, Quetiapine Fumarate, medicine, Antidepressant, Quetiapine, business, 030217 neurology & neurosurgery, Active metabolite, medicine.drug

Abstract

BACKGROUND AND PURPOSE Quetiapine has a range of clinical activity distinct from other atypical antipsychotic drugs, demonstrating efficacy as monotherapy in bipolar depression, major depressive disorder and generalized anxiety disorder. The neuropharmacological mechanisms underlying this clinical profile are not completely understood; however, the major active metabolite, norquetiapine, has been shown to have a distinct in vitro pharmacological profile consistent with a broad therapeutic range and may contribute to the clinical profile of quetiapine. EXPERIMENTAL APPROACH We evaluated quetiapine and norquetiapine, using in vitro binding and functional assays of targets known to be associated with antidepressant and anxiolytic drug actions and compared these activities with a representative range of established antipsychotics and antidepressants. To determine how the in vitro pharmacological properties translate into in vivo activity, we used preclinical animal models with translational relevance to established antidepressant-like and anxiolytic-like drug action. KEY RESULTS Norquetiapine had equivalent activity to established antidepressants at the noradrenaline transporter (NET), while quetiapine was inactive. Norquetiapine was active in the mouse forced swimming and rat learned helplessness tests. In in vivo receptor occupancy studies, norquetiapine had significant occupancy at NET at behaviourally relevant doses. Both quetiapine and norquetiapine were agonists at 5-HT1A receptors, and the anxiolytic-like activity of norquetiapine in rat punished responding was blocked by the 5-HT1A antagonist, WAY100635. CONCLUSIONS AND IMPLICATIONS Quetiapine and norquetiapine have multiple in vitro pharmacological actions, and results from preclinical studies suggest that activity at NET and 5-HT1A receptors contributes to the antidepressant and anxiolytic effects in patients treated with quetiapine.

Published

2015

3. EEG-β/γ spectral power elevation in rat: a translatable biomarker elicited by GABAAα2/3-positive allosteric modulators at nonsedating anxiolytic doses

Author

Adam Jeston Dudley, Joanne Smolka, Carla Maciag, Chapdelaine Marc, Michael Quirk, Wei Song, Farzin Gharahdaghi, Xiaodong F. Liu, Maria Ribadeneira, Donna L. Maier, Jeffrey L. Arriza, Dean H. Snyder, James J. Doherty, Maninder Chopra, Min Ding, David Gurley, and Edward P. Christian

Subjects

Male, Patch-Clamp Techniques, GABA Agents, Physiology, medicine.drug_class, Allosteric regulation, Anxiety, Pharmacology, Electroencephalography, Anxiolytic, Conflict, Psychological, Rats, Sprague-Dawley, medicine, Animals, Gamma Rhythm, Rats, Long-Evans, Benzodiazepine, Communication, Dose-Response Relationship, Drug, medicine.diagnostic_test, business.industry, Chemistry, General Neuroscience, Brain, Receptors, GABA-A, Electrodes, Implanted, Anti-Anxiety Agents, Cortical network, Auditory Perception, Linear Models, Conditioning, Operant, Biomarker (medicine), Pharmaco eeg, Beta Rhythm, business

Abstract

Benzodiazepine drugs, through interaction with GABAAα1, GABAAα2,3, and GABAAα5 subunits, modulate cortical network oscillations, as reflected by a complex signature in the EEG power spectrum. Recent drug discovery efforts have developed GABAAα2,3-subunit-selective partial modulators in an effort to dissociate the side effect liabilities from the efficacy imparted by benzodiazepines. Here, we evaluated rat EEG and behavioral end points during dosing of nine chemically distinct compounds that we confirmed statistically to selectively to enhance GABAAα2,3-mediated vs. GABAAα1 or GABAAα5 currents in voltage clamped oocytes transfected with those GABAA subunits. These compounds were shown with in vivo receptor occupancy techniques to competitively displace [3H]flumazenil in multiple brain regions following peripheral administration at increasing doses. Over the same dose range, the compounds all produced dose-dependent EEG spectral power increases in the β- and and γ-bands. Finally, the dose range that increased γ-power coincided with that eliciting punished over unpunished responding in a behavioral conflict model of anxiety, indicative of anxiolysis without sedation. EEG γ-band power increases showed a significant positive correlation to in vitro GABAAα2,3 modulatory intrinsic activity across the compound set, further supporting a hypothesis that this EEG signature was linked specifically to pharmacological modulation of GABAAα2,3 signaling. These findings encourage further evaluation of this EEG signature as a noninvasive clinical translational biomarker that could ultimately facilitate development of GABAAα2,3-subtype-selective drugs for anxiety and potentially other indications.

Published

2015

4. Identification of short-acting κ-opioid receptor antagonists with anxiolytic-like activity

Author

Linda C. Litwin, John C. Gordon, Anna Zacco, Carla Maciag, Timothy Piser, Todd Andrew Brugel, Carolann Thompson, Linda A. Sygowski, Matthew F. Peters, and Patricia Schroeder

Subjects

Male, Elevated plus maze, Time Factors, medicine.drug_class, Drug Evaluation, Preclinical, Diuresis, Pharmacology, Rats, Sprague-Dawley, Opioid receptor, medicine, Animals, Maze Learning, Receptor, Behavior, Animal, Receptors, Opioid, kappa, Antagonist, medicine.disease, Rats, Inhibition, Psychological, Anti-Anxiety Agents, Mood disorders, Prenatal stress, Opioid, Psychology, Stress, Psychological, medicine.drug

Abstract

The κ-opioid receptor plays a central role in mediating the response to stressful life events. Inhibiting κ-opioid receptor signaling is proposed as a mechanism for treating stress-related conditions such as depression and anxiety. Preclinical testing consistently confirms that disruption of κ-opioid signaling is efficacious in animal models of mood disorders. However, concerns about the feasibility of developing antagonists into drugs stem from an unusual pharmacodynamic property of prototypic κ-opioid receptor-selective antagonists; they inhibit receptor signaling for weeks to months after a single dose. Several fundamental questions include - is it possible to identify short-acting antagonists; is long-lasting inhibition necessary for efficacy; and is it safe to develop long-acting antagonists in the clinic. Here, we test representative compounds (AZ-ECPC, AZ-MTAB, and LY-DMPF) from three new chemical series of κ-opioid receptor ligands for long-lasting inhibition. Each compound dose-dependently reversed κ-opioid agonist-induced diuresis. However, unlike the prototypic antagonist, nBNI, which fully inhibited evoked diuresis for at least four weeks, the new compounds showed no inhibition after one week. The two compounds with greater potency and selectivity were tested in prenatally-stressed rats on the elevated plus maze, an exploration-based model of anxiety. Spontaneous exploration of open arms in the elevated plus maze was suppressed by prenatal stress and restored with both compounds. These findings indicate that persistent inhibition is not an inherent property of κ-opioid-selective antagonists and that post-stress dosing with transient inhibitors can be effective in a mood disorder model. This further supports κ-opioid receptor as a promising target for developing novel psychiatric medications.

Published

2011

5. 2,6-Disubstituted pyrazines and related analogs as NR2B site antagonists of the NMDA receptor with anti-depressant activity

Author

Michael W. Wood, Dean G. Brown, Shephali Trivedi, Don Mathisen, Mark Sylvester, Xia Wang, John C. Roberts, Zuozhong Peng, Tao Hu, Tiffany N. Hoerter, Magnus Johansson, Donna L. Maier, Tongming Chen, Jennifer R. Krumrine, Ji Jiang, Carla Maciag, Lee T. Hirata, Celina C. Lasota, Anshul Gupta, Deidre E. Wilkins, Frank Liu, Jian Xia, Charles S. Elmore, Evelynjeane J. Sutton, Xiaoping Wang, James B. Campbell, Jerry Cumberledge, Cristobal Alhambra, Dennis J. McCarthy, Elnaz Menhaji-Klotz, Jian Wang, Xiaotian Wen, Paul J. Ciaccio, and Clay W Scott

Subjects

Stereochemistry, Clinical Biochemistry, hERG, Pharmaceutical Science, Motor Activity, Pharmacology, Binding, Competitive, Receptors, N-Methyl-D-Aspartate, Biochemistry, Chemical synthesis, Imipramine, Inhibitory Concentration 50, Mice, chemistry.chemical_compound, Drug Discovery, medicine, Ifenprodil, Animals, Binding site, Molecular Biology, Binding Sites, Dose-Response Relationship, Drug, Molecular Structure, biology, Organic Chemistry, Antagonist, Biological activity, Antidepressive Agents, chemistry, Pyrazines, biology.protein, Molecular Medicine, NMDA receptor, Protein Binding, medicine.drug

Abstract

Herein we describe the discovery of compounds that are competitive antagonists of the CP101-606 binding site within the NR2B subtype of the NMDA receptor. The compounds identified do not possess phenolic functional groups such as those in ifenprodil and related analogs. Initial identification of hits in this series focused on a basic, secondary amine side chain which led to good potency, but also presented a hERG liability. Further modifications led to examples of non-basic replacements which demonstrated much less liability in this regard. Finally, one compound in the series, 6a, was tested in the mouse forced swim depression assay and found to show activity (sc 60 mg/kg).

Published

2011

6. A randomized, placebo-controlled pilot trial of the delta opioid receptor agonist AZD2327 in anxious depression

Author

Erica M. Richards, Mark A. Smith, Carla Maciag, Neal M. Nolan, Carlos A. Zarate, Rodrigo Machado-Vieira, Shuang Li, Jose A. Franco-Chaves, Wallace C. Duncan, Mark J. Niciu, Daniel C. Mathews, Thomas J. Hudzik, David A. Luckenbaugh, Alan J. Cross, and Dawn F. Ionescu

Subjects

Agonist, Adult, Male, Vascular Endothelial Growth Factor A, medicine.medical_specialty, Hamilton Anxiety Rating Scale, Adolescent, medicine.drug_class, Pilot Projects, Anxiety, Placebo, Anxiolytic, Article, Piperazines, Rats, Sprague-Dawley, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Double-Blind Method, Internal medicine, Receptors, Opioid, delta, medicine, Animals, Humans, Endogenous opioid, Aged, Pharmacology, Depressive Disorder, Major, business.industry, Brain, Electroencephalography, Middle Aged, medicine.disease, 030227 psychiatry, Disease Models, Animal, Anti-Anxiety Agents, Anesthesia, Endogenous depression, Benzamides, Major depressive disorder, Antidepressant, Female, business, 030217 neurology & neurosurgery

Abstract

Patients with anxious major depressive disorder (AMDD) have more severe symptoms and poorer treatment response than patients with non-AMDD. Increasing evidence implicates the endogenous opioid system in the pathophysiology of depression. AZD2327 is a selective delta opioid receptor (DOR) agonist with anxiolytic and antidepressant activity in animal models. This double-blind, parallel group design, placebo-controlled pilot study evaluated the safety and efficacy of AZD2327 in a preclinical model and in patients with AMDD. We initially tested the effects of AZD2327 in an animal model of AMDD. Subsequently, 22 subjects with AMDD were randomized to receive AZD2327 (3 mg BID) or placebo for 4 weeks. Primary outcome measures included the Hamilton Depression Rating Scale (HAM-D) and the Hamilton Anxiety Rating Scale (HAM-A). We also evaluated neurobiological markers implicated in mood and anxiety disorders, including vascular endothelial growth factor (VEGF) and electroencephalogram (EEG). Seven (54 %) patients responded to active drug and three (33 %) responded to placebo. No significant main drug effect was found on either the HAM-D (p = 0.39) or the HAM-A (p = 0.15), but the HAM-A had a larger effect size. Levels of AZ12311418, a major metabolite of AZD2327, were higher in patients with an anti-anxiety response to treatment compared to nonresponders (p = 0.03). AZD2327 treatment decreased VEGF levels (p = 0.02). There was a trend (p

Published

2016

7. Selective alpha7 nicotinic receptor activation by AZD0328 enhances cortical dopamine release and improves learning and attentional processes

Author

E.J. Sutton, Dan Widzowski, Ladislav Mrzljak, Carla Maciag, James J. Doherty, Dekun Song, Chaoying Li, Yi Wang, Thomas J. Hudzik, Michael Quirk, Simon Sydserff, David Gurley, Jeffrey S. Smith, John C. Gordon, Gennady N. Smagin, Edwin C. Johnson, Tim Piser, Edward P. Christian, and Gerald Jonak

Subjects

Agonist, Male, medicine.medical_specialty, Quinuclidines, Patch-Clamp Techniques, alpha7 Nicotinic Acetylcholine Receptor, medicine.drug_class, Dopamine, Action Potentials, Receptors, Nicotinic, Biochemistry, Cell Line, Rats, Sprague-Dawley, chemistry.chemical_compound, Radioligand Assay, Xenopus laevis, Neurochemical, Dopamine receptor D1, Internal medicine, medicine, Animals, Humans, Learning, Attention, Nicotinic Agonists, Neurotransmitter, Furans, Pharmacology, Cerebral Cortex, Neurons, Dopaminergic, Ventral Tegmental Area, AZD0328, Recognition, Psychology, Rats, Ventral tegmental area, medicine.anatomical_structure, Endocrinology, nervous system, chemistry, Oocytes, Conditioning, Operant, Female, Reinforcement, Psychology, medicine.drug

Abstract

AZD0328, a novel spirofuropyridine neuronal nicotinic receptor partial agonist, was used to investigate the role of alpha7 neuronal nicotinic receptor (NNR) activation in the modulation of midbrain dopamine neuron function, cortical dopamine release and on two behavioral tasks known to be dependent on optimal levels of cortical dopamine. In vivo recordings from area 10 (ventral tegmental area) in rat brain showed an increased firing of putative dopamine neurons in response to low (0.00138 mg/kg) doses of AZD0328. Bursting patterns of dopamine neuron activity remained largely unchanged by application of AZD0328. In vivo microdialysis in awake rats showed an increase in extracellular prefrontal cortical dopamine in response to low doses of AZD0328. Compound-stimulated dopamine release showed an inverted dose effect relation that was maximal at the lowest dose tested (0.00178 mg/kg). Peak extracellular dopamine levels were reached 2h after dosing with AZD0328. Acquisition of operant responding with delayed reinforcement in rats was dose dependently enhanced by AZD0328 with a plateau effect measured at 0.003 mg/kg. This effect was blocked by pre-treatment of animals with the selective alpha7 antagonist methyllycaconitine. AZD0328 improved novel object recognition in mice over a broad range of doses (0.00178-1.78 mg/kg) and the compound effect was found to be absent in homozygous alpha7 KO animals. Together, these data indicate that selective interaction with alpha7 NNRs by AZD0328 selectively enhances midbrain dopaminergic neuronal activity causing an enhancement of cortical dopamine levels; these neurochemical changes likely, underlie the positive behavioral responses observed in two different animal models. Our results suggest selective alpha7 NNR agonists may have significant therapeutic utility in neurologic and psychiatric indications where cognitive deficits and dopamine neuron dysfunction co-exist.

Published

2009