Looking for Novelty in an “Old” Receptor: Recent Advances Toward Our Understanding of GABAARs and Their Implications in Receptor Pharmacology

Castellano, David; Shepard, Ryan D.; Lü, Wei

doi:10.3389/fnins.2020.616298

Cited by 39 publications

(41 citation statements)

References 224 publications

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“…Sensitivity to the benzodiazepines, chlordiazepoxide and diazepam, is conferred by the presence of the γ2 receptor subunit in the GABA A receptor complex [32,33] whilst sensitivity to the NSAID, mefenamic acid is conferred by the presence of the β2/β3 subunits in the receptor complex [4,34]. We can therefore deduce from our electrophysiological data that the GABA A receptor isoforms expressed by iCells are likely composed of αxβ2/3γ2 subunits (where x is one of several possible α subunits) to enable the rich and complex pharmacological responses observed to these clinically important agents and consistent with native GABA A receptor pharmacology [35]. Measurements of mRNA expression levels of GABA A receptor subunits in iCell neurons are also entirely consistent with our patch-clamp data [7,11].…”

Section: Discussionsupporting

confidence: 61%

An Electrophysiological and Pharmacological Study of the Properties of Human iPSC-Derived Neurons for Drug Discovery

Halliwell

Salmanzadeh

Coyne

et al. 2021

Cells

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Human stem cell-derived neurons are increasingly considered powerful models in drug discovery and disease modeling, despite limited characterization of their molecular properties. Here, we have conducted a detailed study of the properties of a commercial human induced Pluripotent Stem Cell (iPSC)-derived neuron line, iCell [GABA] neurons, maintained for up to 3 months in vitro. We confirmed that iCell neurons display neurite outgrowth within 24 h of plating and label for the pan-neuronal marker, βIII tubulin within the first week. Our multi-electrode array (MEA) recordings clearly showed neurons generated spontaneous, spike-like activity within 2 days of plating, which peaked at one week, and rapidly decreased over the second week to remain at low levels up to one month. Extracellularly recorded spikes were reversibly inhibited by tetrodotoxin. Patch-clamp experiments showed that iCell neurons generated spontaneous action potentials and expressed voltage-gated Na and K channels with membrane capacitances, resistances and membrane potentials that are consistent with native neurons. Our single neuron recordings revealed that reduced spiking observed in the MEA after the first week results from development of a dominant inhibitory tone from GABAergic neuron circuit maturation. GABA evoked concentration-dependent currents that were inhibited by the convulsants, bicuculline and picrotoxin, and potentiated by the positive allosteric modulators, diazepam, chlordiazepoxide, phenobarbital, allopregnanolone and mefenamic acid, consistent with native neuronal GABAA receptors. We also show that glycine evoked robust concentration-dependent currents that were inhibited by the neurotoxin, strychnine. Glutamate, AMPA, Kainate and NMDA each evoked concentration-dependent currents in iCell neurons that were blocked by their selective antagonists, consistent with the expression of ionotropic glutamate receptors. The NMDA currents required the presence of the co-agonist glycine and were blocked in a highly voltage-dependent manner by Mg2+ consistent with the properties of native neuronal NMDA receptors. Together, our data suggest that such human iPSC-derived neurons may have significant value in drug discovery and development and may eventually largely replace the need for animal tissues in human biomedical research.

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Section: Discussionsupporting

confidence: 61%

An Electrophysiological and Pharmacological Study of the Properties of Human iPSC-Derived Neurons for Drug Discovery

Halliwell

Salmanzadeh

Coyne

et al. 2021

Cells

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“…In fact, many receptors can exist in nature as receptor complexes where accessory proteins or auxiliary subunits can impact receptor trafficking, kinetics, and pharmacology (Maher et al, 2017). Already, these accessory proteins have been identified for VGCCs (Campiglio and Flucher, 2015), AMPARs (Kamalova and Nakagawa, 2021), nAChRs (Boulin et al, 2012), and most recently GABA A Rs (Castellano et al, 2020;Han et al, 2020). Indeed, targeting of auxiliary subunits has already succeeded with gabapentin being used for the treatment of epilepsy and pain.…”

Section: Discussionmentioning

confidence: 99%

Targeting Endocannabinoid Signaling in the Lateral Habenula as an Intervention to Prevent Mental Illnesses Following Early Life Stress: A Perspective

Shepard

Nugent

2021

Front. Synaptic Neurosci.

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Adverse events and childhood trauma increase the susceptibility towards developing psychiatric disorders (substance use disorder, anxiety, depression, etc.) in adulthood. Although there are treatment strategies that have utility in combating these psychiatric disorders, little attention is placed on how to therapeutically intervene in children exposed to early life stress (ELS) to prevent the development of later psychopathology. The lateral habenula (LHb) has been a topic of extensive investigation in mental health disorders due to its prominent role in emotion and mood regulation through modulation of brain reward and motivational neural circuits. Importantly, rodent models of ELS have been shown to promote LHb dysfunction. Moreover, one of the potential mechanisms contributing to LHb neuronal and synaptic dysfunction involves endocannabinoid (eCB) signaling, which has been observed to critically regulate emotion/mood and motivation. Many pre-clinical studies targeting eCB signaling suggest that this neuromodulatory system could be exploited as an intervention therapy to halt maladaptive processes that promote dysfunction in reward and motivational neural circuits involving the LHb. In this perspective article, we report what is currently known about the role of eCB signaling in LHb function and discuss our opinions on new research directions to determine whether the eCB system is a potentially attractive therapeutic intervention for the prevention and/or treatment of ELS-associated psychiatric illnesses.

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“…The dysfunction of GABAergic transmission contributes to several neurological conditions, such as depression, anxiety, epilepsy (for a review, see: [78]), SZ [79], and ASD [80,81]. Based on the considerable combinatorial possibilities, a novel and more specific pharmacological intervention has been proposed as a potential advancement for clinical treatment over the use of nonselective GABA A receptor agonists (for a review, see: [78,82]. Furthermore, accessory molecules that interact with GABA A receptors may be new potential targets.…”

Section: Neuroplastin and Gaba A Receptor (Gaba A R)mentioning

confidence: 99%

Neuroplastin in Neuropsychiatric Diseases

Lin

Liang

Herrera-Molina

et al. 2021

Genes

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Molecular mechanisms underlying neuropsychiatric and neurodegenerative diseases are insufficiently elucidated. A detailed understanding of these mechanisms may help to further improve medical intervention. Recently, intellectual abilities, creativity, and amnesia have been associated with neuroplastin, a cell recognition glycoprotein of the immunoglobulin superfamily that participates in synapse formation and function and calcium signaling. Data from animal models suggest a role for neuroplastin in pathways affected in neuropsychiatric and neurodegenerative diseases. Neuroplastin loss or disruption of molecular pathways related to neuronal processes has been linked to various neurological diseases, including dementia, schizophrenia, and Alzheimer’s disease. Here, we review the molecular features of the cell recognition molecule neuroplastin, and its binding partners, which are related to neurological processes and involved in learning and memory. The emerging functions of neuroplastin may have implications for the treatment of diseases, particularly those of the nervous system.

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Looking for Novelty in an “Old” Receptor: Recent Advances Toward Our Understanding of GABAARs and Their Implications in Receptor Pharmacology

Cited by 39 publications

References 224 publications

An Electrophysiological and Pharmacological Study of the Properties of Human iPSC-Derived Neurons for Drug Discovery

An Electrophysiological and Pharmacological Study of the Properties of Human iPSC-Derived Neurons for Drug Discovery

Targeting Endocannabinoid Signaling in the Lateral Habenula as an Intervention to Prevent Mental Illnesses Following Early Life Stress: A Perspective

Neuroplastin in Neuropsychiatric Diseases

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