Antagonists of Ionotropic Receptors for the Inhibitory Neurotransmitter GABA: Therapeutic Indications

Hinton, Tina; Johnston, Graham A.R.

doi:10.5772/intechopen.72678

Cited by 3 publications

(3 citation statements)

References 77 publications

(88 reference statements)

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“…Previous studies have shown that pharmacological targeting of GABA A Rs can alleviate neuropathic pain in a peripheral nerve injury model 19 , yet no evidence has been provided regarding the role of any GABA A R subunit on hindlimb functional recovery in SCI rats. We first applied sustained administration of bicuculline, a competitive antagonist of GABA A Rs 20 , either with or without hUC-MSC transplantation to assess the effects of GABA A Rs on hUC-MSC-mediated SCI repair. IF staining showed that the general expression levels and/or distributions of different GABA A R subunits were not obviously affected by bicuculline treatment at the epicenter (Figure 3 A).…”

Section: Resultsmentioning

confidence: 99%

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABA_A receptor

Cao¹,

Chen²,

Huang³

et al. 2022

Theranostics

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Rationale: Spinal cord injury (SCI) remains an incurable neurological disorder leading to permanent and profound neurologic deficits and disabilities. Human umbilical cord-derived mesenchymal stem cells (hUC-MSCs) are particularly appealing in SCI treatment to curtail damage, restore homeostasis and possible neural relay. However, the detailed mechanisms underlying hUC-MSC-mediated functional recovery of SCI have not been fully elucidated. The purpose of our current study is to identify novel therapeutic targets and depict the molecular mechanisms underlying the hUC-MSC-mediated recovery of subacute SCI. Methods: Adult female rats suffering from subacute incomplete thoracic SCI were treated with intrathecal transplantation of hUC-MSCs. The beneficial effects of hUC-MSCs on SCI repair were evaluated by a series of behavioral analyses, motor evoked potentials (MEPs) recording of hindlimb and immunohistochemistry. We carried out extensive transcriptome comparative analyses of spinal cord tissues at the lesion site from the subacute phase of SCI (sub-SCI) either treated without (+PBS) or with hUC-MSCs (+MSC) at 0 (sub-SCI), 1, 2, and 4 weeks post-transplantation (wpt), as well as normal spinal cord segments of intact/sham rats (Intact). Adeno-associated virus (AAV)-mediated neuron-specific expression system was employed to functionally screen specific γ-aminobutyric acid type A receptor (GABA A R) subunits promoting the functional recovery of SCI in vivo . The mature cortical axon scrape assay and transplantation of genetically modified MSCs with either overexpression or knockdown of brain-derived neurotrophic factor (BDNF) were employed to demonstrate that hUC-MSCs ameliorated the reduction of GABA A R subunits in the injured spinal cord via BDNF secretion in vitro and in vivo , respectively. Results: Comparative transcriptome analysis revealed the GABAergic synapse pathway is significantly enriched as a main target of hUC-MSC-activated genes in the injured spinal cord. Functional screening of the primary GABA A R subunits uncovered that Gabrb3 and Garbg2 harbored the motor and electrophysiological recovery-promoting competence. Moreover, targeting either of the two pivotal subunits β3 or γ2 in combination with/without the K + /Cl - cotransporter 2 (KCC2) reinforced the therapeutic effects. Mechanistically, BDNF secreted by hUC-MSCs contributed to the upregulation of GABA A R subunits (β3 & γ2) and KCC2 in the injured neurons. Conclusions: Our study identifies a novel mode for hUC-MSC-mediated locomotor recovery of SCI through synergistic upregulation of GABA A R β3 and γ2 along with KCC2 by BDNF secretion, indicating the significance of restoring the excitation/inhibition balan...

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Section: Resultsmentioning

confidence: 99%

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABA_A receptor

Cao¹,

Chen²,

Huang³

et al. 2022

Theranostics

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“…The effects of both gabazine and picrotoxin treatment at ambient CO 2 on specific behavioural traits in the current study suggests that receptors in I. pygmaeus are sensitive to gabazine and picrotoxin. Furthermore, the concentrations used did not cause any obvious convulsions, which can be produced by the excitotoxic effects of GABA A R antagonists when administered systemically (Hinton and Johnston, 2018). The concentrations used are based on previous in vivo studies showing behavioural change with no convulsant effects reported (Biscocho et al, 2018;Chivers et al, 2014;Hamilton et al, 2013;Nilsson et al, 2012;Rittschof et al, 1986;Watson et al, 2014).…”

Section: Behavioural Effects Of Gabazine and Picrotoxinmentioning

confidence: 99%

The role of ligand-gated chloride channels in behavioural alterations at elevated CO2 in a cephalopod

Thomas

Spady

Munday

et al. 2021

Journal of Experimental Biology

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Projected future carbon dioxide (CO2) levels in the ocean can alter marine animal behaviours. Disrupted functioning of γ-aminobutyric acid type A (GABAA) receptors (ligand-gated chloride channels) is suggested to underlie CO2-induced behavioural changes in fish. However, the mechanisms underlying behavioural changes in marine invertebrates are poorly understood. We pharmacologically tested the role of GABA-, glutamate-, acetylcholine- and dopamine-gated chloride channels in CO2-induced behavioural changes in a cephalopod, the two-toned pygmy squid (Idiosepius pygmaeus). We exposed squid to ambient (∼450 µatm) or elevated (∼1,000 µatm) CO2 for seven days. Squid were treated with sham, the GABAA receptor antagonist gabazine, or the non-specific GABAA receptor antagonist picrotoxin, before measurement of conspecific-directed behaviours and activity levels upon mirror exposure. Elevated CO2 increased conspecific-directed attraction and aggression, as well as activity levels. For some CO2-affected behaviours, both gabazine and picrotoxin had a different effect at elevated compared to ambient CO2, providing robust support for the GABA hypothesis within cephalopods. In another behavioural trait, picrotoxin but not gabazine had a different effect in elevated compared to ambient CO2, providing the first pharmacological evidence, in fish and marine invertebrates, for altered functioning of ligand-gated chloride channels, other than the GABAA R, underlying CO2-induced behavioural changes. For some other behaviours, both gabazine and picrotoxin had a similar effect in elevated and ambient CO2, suggesting altered function of ligand-gated chloride channels was not responsible for these CO2-induced changes. Multiple mechanisms may be involved, which could explain the variability in the CO2 and drug treatment effects across behaviours.

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“…19 Since systemic administration of brain-permeant unspecific or subtype-unselective GABA A R antagonists (i.e., PTX or BCC) causes profound convulsant effects, they have been used as powerful tools to elucidate the physiological importance of the receptors without any therapeutic potential. 20 Indeed, although a number of GABA A R agonists or PAMs are approved for clinical use, the silent allosteric modulator flumazenil is the only GABA A R antagonist currently used in medical practice. 21 Due to the low number of GABA A R subtype-specific antagonists, the potential of such compounds as CNS targeting therapeutics has only been sparingly studied.…”

Section: ■ Introductionmentioning

confidence: 99%

Structure–Activity Studies of 3,9-Diazaspiro[5.5]undecane-Based γ-Aminobutyric Acid Type A Receptor Antagonists with Immunomodulatory Effect

et al. 2021

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The 3,9-diazaspiro[5.5]undecane-based compounds 2027 and 018 have previously been reported to be potent competitive γ-aminobutyric acid type A receptor (GABAAR) antagonists showing low cellular membrane permeability. Given the emerging peripheral application of GABAAR ligands, we hypothesize 2027 analogs as promising lead structures for peripheral GABAAR inhibition. We herein report a study on the structural determinants of 2027 in order to suggest a potential binding mode as a basis for rational design. The study identified the importance of the spirocyclic benzamide, compensating for the conventional acidic moiety, for GABAAR ligands. The structurally simplified m-methylphenyl analog 1e displayed binding affinity in the high-nanomolar range (K i = 180 nM) and was superior to 2027 and 018 regarding selectivity for the extrasynaptic α4βδ subtype versus the α1- and α2- containing subtypes. Importantly, 1e was shown to efficiently rescue inhibition of T cell proliferation, providing a platform to explore the immunomodulatory potential for this class of compounds.

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Antagonists of Ionotropic Receptors for the Inhibitory Neurotransmitter GABA: Therapeutic Indications

Cited by 3 publications

References 77 publications

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABA_A receptor

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABA_A receptor

The role of ligand-gated chloride channels in behavioural alterations at elevated CO2 in a cephalopod

Structure–Activity Studies of 3,9-Diazaspiro[5.5]undecane-Based γ-Aminobutyric Acid Type A Receptor Antagonists with Immunomodulatory Effect

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Antagonists of Ionotropic Receptors for the Inhibitory Neurotransmitter GABA: Therapeutic Indications

Cited by 3 publications

References 77 publications

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABAA receptor

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABAA receptor

The role of ligand-gated chloride channels in behavioural alterations at elevated CO2 in a cephalopod

Structure–Activity Studies of 3,9-Diazaspiro[5.5]undecane-Based γ-Aminobutyric Acid Type A Receptor Antagonists with Immunomodulatory Effect

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Product

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hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABA_A receptor

hUC-MSC-mediated recovery of subacute spinal cord injury through enhancing the pivotal subunits β3 and γ2 of the GABA_A receptor