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GABAergic

About: GABAergic is a research topic. Over the lifetime, 9595 publications have been published within this topic receiving 473568 citations.


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TL;DR: RO15-4513 reverses both the behavioral and biochemical effects of ethanol, including the action of GABA-induced Cl- fluxes, but its potential clinical application may be restricted due to its inverse agonistic property.
Abstract: The behavioral and biochemical effects of ethanol in man and animals have been investigated for a long time. A role of catecholamines in the central stimulatory action and during withdrawal has been envisaged, but more recent observations have revealed the involvement of inhibitory synaptic transmitter, GABA, in the actions of ethanol. Ethanol-induced motor incoordination, hypnosedation, antianxiety, and anticonvulsant actions are reported to be GABA-mediated. Involvement of the GABA system has been implicated in ethanol withdrawal-induced seizure in animals. More direct evidences using Cl− influx studies in synaptoneurosomes and spinal neuronal culture studies confirm such a mode of action of ethanol, probably influencing the chloride channel modulation at the GABA-benzodiazepine receptor ionophore complex. RO15–4513 ( (ethyl-8-azido-5,6-dihydro-5-methyl-6-Oxo-4H-imidazo [1,5-α], [1,4] benzodiazepine-3-carboxylate), a novel imidazobenzodiazepine, an analogue of the classical benzodiazepine antagonist is reported to possess alcohol antagonistic properties. RO15–4513 reverses both the behavioral and biochemical effects of ethanol, including the action of GABA-induced Cl− fluxes. But its potential clinical application may be restricted due to its inverse agonistic property. The present review focuses on the GABA-linked behavioral and biochemical actions of ethanol and discusses the potential of RO15–4513 as an alcohol antagonist.

135 citations

Journal ArticleDOI
TL;DR: Investigation of frontal cortical tissue taken post mortem from a series of schizophrenic patients and matched control subjects revealed that parvalbumin-, but not calretinin-immunoreactive cells are significantly diminished in schizophrenia, which supports the hypothesis that GABAergic deficits in schizophrenia may stem from toxic events occurring during cortical development which selectively target immature neurons before protection by paravalbumin is conferred.

135 citations

Journal ArticleDOI
TL;DR: The strength of electrical coupling between MCR and MB cells underlies their synchronous activation during carbachol-induced oscillations, and like many other GABAergic interneurons, BCR cells but not MCR cells exhibit restricted cell type-specific gap junction coupling.
Abstract: Calretinin (CR)-positive GABAergic (gamma-aminobutyric acidergic) interneurons have been suggested to target preferentially other GABAergic cells in the neocortex. To systematically study this cell population in the cortex, we generated transgenic mice that express enhanced green fluorescent protein (EGFP) under the control of the CR promoter and characterized EGFP/CR-positive cells at the cellular and network level. Based on anatomical and electrophysiological characteristics, 2 types of EGFP/CR-positive cells could be distinguished that we termed bipolar (BCR) and multipolar (MCR) CR cells. Both cell types share the feature of preferential interneuron targeting but differ in most other characteristics, including firing pattern, biochemical markers, neurite arborization, and synaptic plasticity. Like many other GABAergic interneurons, BCR cells but not MCR cells exhibit restricted cell type-specific gap junction coupling. Notably, MCR cells are electrically coupled in an asymmetric fashion with GABAergic interneurons of another subtype, the parvalbumin-positive multipolar bursting (MB) cells. Most importantly, the strength of electrical coupling between MCR and MB cells underlies their synchronous activation during carbachol-induced oscillations.

135 citations

Journal ArticleDOI
TL;DR: One of the new family of NMDA receptor antagonists, such as DETC-MESO, which regulate the redox site ofNMDA receptors, may prove to be the drug of choice for treating alcoholism as well as many neurological diseases.
Abstract: The pharmacological effects of ethanol are complex and widespread without a well-defined target. Since glutamatergic and GABAergic innervation are both dense and diffuse and account for more than 80% of the neuronal circuitry in the human brain, alterations in glutamatergic and GABAergic function could affect the function of all neurotransmitter systems. Here, we review recent progress in glutamatergic and GABAergic systems with a special focus on their roles in alcohol dependence and alcohol withdrawal-induced seizures. In particular, NMDA-receptors appear to play a central role in alcohol dependence and alcohol-induced neurological disorders. Hence, NMDA receptor antagonists may have multiple functions in treating alcoholism and other addictions and they may become important therapeutics for numerous disorders including epilepsy, Parkinson's disease, amyotrophic lateral sclerosis, Huntington's chorea, anxiety, neurotoxicity, ischemic stroke, and chronic pain. One of the new family of NMDA receptor antagonists, such as DETC-MESO, which regulate the redox site of NMDA receptors, may prove to be the drug of choice for treating alcoholism as well as many neurological diseases.

135 citations

Journal ArticleDOI
TL;DR: Findings emphasize that GABAergic inhibitory interneurons in the PFC undergo a dynamic, cell type-specific remodeling during adolescence and provide a developmental framework for understanding alterations in GABAergic circuits that occur in psychiatric disorders.
Abstract: Determining the normal developmental trajectory of individual GABAergic components in the prefrontal cortex (PFC) during the adolescent transition period is critical because local GABAergic interneurons are thought to play an important role in the functional maturation of cognitive control that occurs in this developmental window. Based on the expression of calcium-binding proteins, three distinctive subtypes of interneurons have been identified in the PFC: parvalbumin (PV)-, calretinin (CR)-, and calbindin (CB)-positive cells. Using biochemical and histochemical measures, we found that the protein level of PV is lowest in juveniles [postnatal days (PD) 25–35] and increases during adolescence (PD 45–55) to levels similar to those observed in adulthood (PD 65–75). In contrast, the protein expression of CR is reduced in adults compared to juvenile and adolescent animals, whereas CB levels remain mostly unchanged across the developmental window studied here. Semi-quantitative immunostaining analyses revealed that the periadolescent upregulation of PV and the loss of the CR signal appear to be attributable to changes in PV- and CR-positive innervation, which are dissociable from the trajectory of PV- and CR-positive cell number. At the synaptic level, our electrophysiological data revealed that a developmental facilitation of spontaneous glutamatergic synaptic inputs onto PV-positive/fast-spiking interneurons parallels the increase in prefrontal PV signal during the periadolescent transition. In contrast, no age-dependent changes in glutamatergic transmission were observed in PV-negative/non fast-spiking interneurons. Together, these findings emphasize that GABAergic inhibitory interneurons in the PFC undergo a dynamic, cell type-specific remodeling during adolescence and provide a developmental framework for understanding alterations in GABAergic circuits that occur in psychiatric disorders.

134 citations


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Performance
Metrics
No. of papers in the topic in previous years
YearPapers
2023371
2022749
2021341
2020320
2019301
2018297