Your search keyword '"Hogenkamp DJ"' showing total 5 results

1. Positive allosteric modulators of nonbenzodiazepine γ-aminobutyric acidA receptor subtypes for the treatment of chronic pain.

Author

Johnstone TBC, Xie JY, Qu C, Wasiak DJ, Hogenkamp DJ, Porreca F, and Gee KW

Subjects

Allosteric Regulation drug effects, Animals, Chronic Pain etiology, Conditioning, Operant, Disease Models, Animal, Dose-Response Relationship, Drug, GABA Modulators chemistry, HIV Infections complications, Hyperalgesia physiopathology, Male, Nucleus Accumbens drug effects, Nucleus Accumbens pathology, Pain Measurement, Pain Threshold drug effects, Patch-Clamp Techniques, Peripheral Nerve Injuries complications, Physical Endurance drug effects, RNA, Messenger metabolism, RNA, Messenger pharmacology, Rats, Rats, Sprague-Dawley, Receptors, GABA genetics, Chronic Pain drug therapy, Chronic Pain metabolism, GABA Modulators therapeutic use, Receptors, GABA metabolism

Abstract

Chronic neuropathic pain may be caused, in part, by loss of inhibition in spinal pain processing pathways due to attenuation of local GABAergic tone. Nociception and nocifensive behaviors are reduced after enhancement of tonically activated extrasynaptic GABAAR-mediated currents by agonist ligands for δ subunit-containing GABAARs. However, typical ligands that target δ subunit-containing GABAARs are limited due to sedative effects at higher doses. We used the spinal nerve ligation (SNL) and gp120 models of experimental neuropathic pain to evaluate compound 2-261, a nonbenzodiazepine site positive allosteric modulator of α4β3δ GABAARs optimized to be nonsedative by selective activation of β2/3-subunit-containing GABAARs over receptor subtypes incorporating β1 subunits. Similar levels of 2-261 were detected in the brain and plasma after intraperitoneal administration. Although systemic 2-261 did not alter sensory thresholds in sham-operated animals, it significantly reversed SNL-induced thermal and tactile hypersensitivity in a GABAAR-dependent fashion. Intrathecal 2-261 produced conditioned place preference and elevated dopamine levels in the nucleus accumbens of nerve-injured, but not sham-operated, rats. In addition, systemic pretreatment with 2-261 blocked conditioned place preference from spinal clonidine in SNL rats. Moreover, 2-261 reversed thermal hyperalgesia and partially reversed tactile allodynia in the gp120 model of HIV-related neuropathic pain. The effects of 2-261 likely required interaction with the α4β3δ GABAAR because 2-301, a close structural analog of 2-261 with limited extrasynaptic receptor efficacy, was not active. Thus, 2-261 may produce pain relief with diminished side effects through selective modulation of β2/3-subunit-containing extrasynaptic GABAARs.

Published

2019

2. Role of β 2/3 -specific GABA-A receptor isoforms in the development of hippocampus kindling epileptogenesis.

Author

Reddy DS, Yoshimura RF, Ramanathan G, Carver C, Johnstone TB, Hogenkamp DJ, and Gee KW

Subjects

Allosteric Regulation drug effects, Allosteric Regulation physiology, Animals, GABA Modulators pharmacology, Hippocampus drug effects, Kindling, Neurologic drug effects, Male, Mice, Mice, 129 Strain, Mice, Inbred C57BL, Protein Isoforms, Seizures physiopathology, Temporal Lobe drug effects, Temporal Lobe physiopathology, Epilepsy drug therapy, Epilepsy physiopathology, GABA Modulators therapeutic use, Hippocampus physiopathology, Kindling, Neurologic physiology, Receptors, GABA-A physiology

Abstract

Objective: Subunit-specific positive allosteric modulators (PAMs) of gamma-aminobutyric acid-A (GABA-A) receptors are commonly used to uncover the role of GABA-A receptor isoforms in brain function. Recently, we have designed novel PAMs selective for β 2/3 -subunit containing GABA-A receptors (β 2/3 -selective PAMs) that are nonbenzodiazepine site-mediated and do not show an α-subunit isoform selectivity, yet exhibit anxiolytic efficacy with reduced potential for sedation, cognitive impairment, and tolerance. In this study, we used three novel β 2/3 -selective PAMs (2-261, 2-262, and 10029) with differential β 2/3 -subunit potency to identify the role of β 2/3 -selective receptor isoforms in limbic epileptogenesis., Methods: Experimental epileptogenesis was induced in mice by daily hippocampus stimulations until each mouse showed generalized (stage 5) seizures. Patch-clamp electrophysiology was used to record GABA-gated currents. Brain levels of β 2/3 -selective PAMs were determined for mechanistic correlations., Results: Treatment with the β 2/3 -selective PAMs 2-261 (30mg/kg), 2-262 (10mg/kg), and 10029 (30mg/kg), 30min prior to stimulations, significantly suppressed the rate of development of kindled seizure activity without affecting the afterdischarge (AD) signal, indicating their disease-modifying activity. The β 2/3 -selective agents suppressed chemical epileptogenesis in the pentylenetetrazol model. Test doses of these agents were devoid of acute antiseizure activity in the kindling model., Conclusion: These findings demonstrate that β 2/3 -selective PAMs can moderately retard experimental epileptogenesis, indicating the protective role of β 2/3 -subunit GABA-A receptor isoforms in the development of epilepsy., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

3. Limiting activity at beta1-subunit-containing GABAA receptor subtypes reduces ataxia.

Author

Gee KW, Tran MB, Hogenkamp DJ, Johnstone TB, Bagnera RE, Yoshimura RF, Huang JC, Belluzzi JD, and Whittemore ER

Subjects

Allosteric Regulation, Amides chemistry, Amides pharmacokinetics, Amides pharmacology, Animals, Anti-Anxiety Agents chemistry, Anti-Anxiety Agents pharmacokinetics, Ataxia physiopathology, Ataxia psychology, Behavior, Animal drug effects, Dose-Response Relationship, Drug, GABA Modulators chemistry, GABA Modulators pharmacokinetics, Humans, Male, Mice, Oocytes drug effects, Oocytes physiology, Patch-Clamp Techniques, Protein Isoforms physiology, Rats, Rats, Sprague-Dawley, Stereoisomerism, Structure-Activity Relationship, Xenopus laevis, Anti-Anxiety Agents pharmacology, Ataxia prevention & control, GABA Modulators pharmacology, Receptors, GABA-A physiology

Abstract

GABA(A) receptor (R) positive allosteric modulators that selectively modulate GABA(A)Rs containing beta(2)- and/or beta(3)- over beta(1)-subunits have been reported across diverse chemotypes. Examples include loreclezole, mefenamic acid, tracazolate, and etifoxine. In general,"beta(2/3)-selective" GABA(A)R positive allosteric modulators are nonbenzodiazepines (nonBZs), do not show alpha-subunit isoform selectivity, yet have anxiolytic efficacy with reduced ataxic/sedative effects in animal models and humans. Here, we report on an enantiomeric pair of nonBZ GABA(A)R positive allosteric modulators that demonstrate differential beta-subunit isoform selectivity. We have tested this enantiomeric pair along with a series of other beta(2/3)-subunit selective, alpha-subunit isoform-selective, BZ and nonBZ GABA(A) positive allosteric modulators using electrophysiological, pharmacokinetic, and behavioral assays to test the hypothesis that ataxia may be correlated with the extent of modulation at beta(1)-subunit-containing GABA(A)Rs. Our findings provide an alternative strategy for designing anxioselective allosteric modulators of the GABA(A)R with BZ-like anxiolytic efficacy by reducing or eliminating activity at beta(1)-subunit-containing GABA(A)Rs.

Published

2010

4. Nootropic alpha7 nicotinic receptor allosteric modulator derived from GABAA receptor modulators.

Author

Ng HJ, Whittemore ER, Tran MB, Hogenkamp DJ, Broide RS, Johnstone TB, Zheng L, Stevens KE, and Gee KW

Subjects

Animals, Brain metabolism, Cell Survival drug effects, Cognition drug effects, Dizocilpine Maleate pharmacology, Humans, Male, Mice, Mice, Inbred DBA, Rats, Rats, Sprague-Dawley, Xenopus laevis, alpha7 Nicotinic Acetylcholine Receptor, GABA Modulators pharmacology, Nootropic Agents pharmacology, Receptors, GABA-A drug effects, Receptors, Nicotinic drug effects

Abstract

Activation of brain alpha7 nicotinic acetylcholine receptors (alpha7 nAChRs) has broad therapeutic potential in CNS diseases related to cognitive dysfunction, including Alzheimer's disease and schizophrenia. In contrast to direct agonist activation, positive allosteric modulation of alpha7 nAChRs would deliver the clinically validated benefits of allosterism to these indications. We have generated a selective alpha7 nAChR-positive allosteric modulator (PAM) from a library of GABAA receptor PAMs. Compound 6 (N-(4-chlorophenyl)-alpha-[[(4-chloro-phenyl)amino]methylene]-3-methyl-5-isoxazoleacet-amide) evokes robust positive modulation of agonist-induced currents at alpha7 nAChRs, while preserving the rapid native characteristics of desensitization, and has little to no efficacy at other ligand-gated ion channels. In rodent models, it corrects sensory-gating deficits and improves working memory, effects consistent with cognitive enhancement. Compound 6 represents a chemotype for allosteric activation of alpha7 nAChRs, with therapeutic potential in CNS diseases with cognitive dysfunction.

Published

2007

5. Substituted 3beta-phenylethynyl derivatives of 3alpha-hydroxy-5alpha-pregnan-20-one: remarkably potent neuroactive steroid modulators of gamma-aminobutyric acidA receptors.

Author

Hawkinson JE, Acosta-Burruel M, Yang KC, Hogenkamp DJ, Chen JS, Lan NC, Drewe JA, Whittemore ER, Woodward RM, Carter RB, and Upasani RB

Subjects

Animals, Bridged Bicyclo Compounds, Heterocyclic metabolism, Flunitrazepam metabolism, Humans, Male, Mice, Muscimol metabolism, Rats, Recombinant Proteins metabolism, Structure-Activity Relationship, Xenopus, GABA Modulators pharmacology, Pregnanolone pharmacology, Receptors, GABA-A drug effects

Abstract

Neuroactive steroids are positive allosteric modulators of gamma-aminobutyric acidA (GABAA) receptor complexes. Synthetic modification generally does not increase neuroactive steroid potency beyond that of the naturally occurring progesterone metabolite, 3alpha-hydroxy-5alpha-pregnan-20-one (3alpha,5alpha-P). Recently, it has been shown that introduction of appropriately para-substituted phenylethynyl groups at the 3beta-position of 5beta steroids increases receptor potency. The present report presents the synthesis and pharmacological profile of an analogous series of 5alpha steroids. The most striking feature of this series is the further enhancement of in vitro and in vivo potency obtained. In particular, 3beta-(p-acetylphenylethynyl)-3alpha-hydroxy-5alpha-pr egnan-20-one (Co 152791) was 11-, 16- and 49-fold more potent than 3alpha, 5alpha-P in modulating the binding of [35S]TBPS, [3H]flunitrazepam and [3H]muscimol, respectively, in rat brain membranes (Co 152791 IC50 or EC50 = 2-7.5 nM). Similarly, Co 152791 was 3- to 20-fold more potent than 3alpha,5alpha-P as an inhibitor of [35S]TBPS binding in human recombinant receptor combinations containing alpha1, alpha2, alpha3 or alpha5 and beta2gamma2L subunits (Co 152791 IC50 1.4-5.7 nM). Co 152791 displayed low efficacy and 3alpha,5alpha-P had low potency at alpha4/6beta3gamma2L GABAA receptor complexes. Interestingly, Co 152791 demonstrated remarkable potency as a potentiator of GABA-evoked currents in Xenopus oocytes expressing alpha1beta2gamma2L receptors (EC50 0.87 nM), being 184-fold more potent than 3alpha,5alpha-P. High in vitro potency was also reflected in enhanced in vivo activity in that Co 152791 exhibited exceptional anticonvulsant potency, protecting mice from pentylenetetrazol-induced seizures at a approximately 5-fold lower dose than 3alpha,5alpha-P after i.p. administration (Co 152791 ED50 0.6 mg/kg). Moreover, Co 152791 was orally active (ED50 1.1 mg/kg) and exhibited a therapeutic index of 7 relative to rotorod impairment. The remarkable potency of Co 152791 as a positive allosteric modulator of GABAA receptors may be explained by its interaction with an auxiliary binding pocket in the neuroactive steroid binding site. In addition, modification at the 3beta-position probably hinders metabolism of the 3alpha-hydroxy group contributing to the exceptional anticonvulsant potency of this compound relative to other neuroactive steroids.

Published

1998