Neuropharmacology

, volume 136 , issue Pt A , pages 10-22

GABAA receptor: Positive and negative allosteric modulators

Richard W. Olsen ¹

Hide authors affiliations Show authors affiliations: 1 affiliation

Department of Molecular and Medical Pharmacology David Geffen School of Medicine at UCLA Los Angeles CA USA |

Publication type: Journal Article

Publication date: 2018-07-01

Elsevier

Neuropharmacology

scimago Q1

wos Q1

SJR: 1.589

CiteScore: 9.4

Impact factor: 4.6

ISSN: 00283908, 18737064

DOI: 10.1016/j.neuropharm.2018.01.036

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PubMed ID: 29407219

Pharmacology

Cellular and Molecular Neuroscience

Abstract

gamma-Aminobutyric acid (GABA)-mediated inhibitory neurotransmission and the gene products involved were discovered during the mid-twentieth century. Historically, myriad existing nervous system drugs act as positive and negative allosteric modulators of these proteins, making GABA a major component of modern neuropharmacology, and suggesting that many potential drugs will be found that share these targets. Although some of these drugs act on proteins involved in synthesis, degradation, and membrane transport of GABA, the GABA receptors Type A (GABAAR) and Type B (GABABR) are the targets of the great majority of GABAergic drugs. This discovery is due in no small part to Professor Norman Bowery. Whereas the topic of GABABR is appropriately emphasized in this special issue, Norman Bowery also made many insights into GABAAR pharmacology, the topic of this article. GABAAR are members of the ligand-gated ion channel receptor superfamily, a chloride channel family of a dozen or more heteropentameric subtypes containing 19 possible different subunits. These subtypes show different brain regional and subcellular localization, age-dependent expression, and potential for plastic changes with experience including drug exposure. Not only are GABAAR the targets of agonist depressants and antagonist convulsants, but most GABAAR drugs act at other (allosteric) binding sites on the GABAAR proteins. Some anxiolytic and sedative drugs, like benzodiazepine and related drugs, act on GABAAR subtype-dependent extracellular domain sites. General anesthetics including alcohols and neurosteroids act at GABAAR subunit-interface trans-membrane sites. Ethanol at high anesthetic doses acts on GABAAR subtype-dependent trans-membrane domain sites. Ethanol at low intoxicating doses acts at GABAAR subtype-dependent extracellular domain sites. Thus GABAAR subtypes possess pharmacologically specific receptor binding sites for a large group of different chemical classes of clinically important neuropharmacological agents. This article is part of the "Special Issue Dedicated to Norman G. Bowery".

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GOST |

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GOST Copy

Olsen R. W. GABAA receptor: Positive and negative allosteric modulators // Neuropharmacology. 2018. Vol. 136. No. Pt A. pp. 10-22.

GOST all authors (up to 50) Copy

Olsen R. W. GABAA receptor: Positive and negative allosteric modulators // Neuropharmacology. 2018. Vol. 136. No. Pt A. pp. 10-22.

RIS |

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RIS Copy

TY - JOUR

DO - 10.1016/j.neuropharm.2018.01.036

UR - https://doi.org/10.1016/j.neuropharm.2018.01.036

TI - GABAA receptor: Positive and negative allosteric modulators

T2 - Neuropharmacology

AU - Olsen, Richard W.

PY - 2018

DA - 2018/07/01

PB - Elsevier

SP - 10-22

IS - Pt A

VL - 136

PMID - 29407219

SN - 0028-3908

SN - 1873-7064

ER -

BibTex |

Cite this

BibTex (up to 50 authors) Copy

@article{2018_Olsen,

author = {Richard W. Olsen},

title = {GABAA receptor: Positive and negative allosteric modulators},

journal = {Neuropharmacology},

year = {2018},

volume = {136},

publisher = {Elsevier},

month = {jul},

url = {https://doi.org/10.1016/j.neuropharm.2018.01.036},

number = {Pt A},

pages = {10--22},

doi = {10.1016/j.neuropharm.2018.01.036}

}

MLA

Cite this

MLA Copy

Olsen, Richard W.. “GABAA receptor: Positive and negative allosteric modulators.” Neuropharmacology, vol. 136, no. Pt A, Jul. 2018, pp. 10-22. https://doi.org/10.1016/j.neuropharm.2018.01.036.

Publisher

Elsevier

Journal

Neuropharmacology

scimago Q1

wos Q1

SJR

1.589

CiteScore

9.4

Impact factor

4.6

ISSN

00283908 (Print)

18737064 (Electronic)