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TitleMechanisms of inhibition and activation of extrasynaptic αβ GABA receptors.
Journal, issue, pagesNature, Vol. 602, Issue 7897, Page 529-533, Year 2022
Publish dateFeb 9, 2022
AuthorsVikram Babu Kasaragod / Martin Mortensen / Steven W Hardwick / Ayla A Wahid / Valentina Dorovykh / Dimitri Y Chirgadze / Trevor G Smart / Paul S Miller /
PubMed AbstractType A GABA (γ-aminobutyric acid) receptors represent a diverse population in the mammalian brain, forming pentamers from combinations of α-, β-, γ-, δ-, ε-, ρ-, θ- and π-subunits. αβ, ...Type A GABA (γ-aminobutyric acid) receptors represent a diverse population in the mammalian brain, forming pentamers from combinations of α-, β-, γ-, δ-, ε-, ρ-, θ- and π-subunits. αβ, α4βδ, α6βδ and α5βγ receptors favour extrasynaptic localization, and mediate an essential persistent (tonic) inhibitory conductance in many regions of the mammalian brain. Mutations of these receptors in humans are linked to epilepsy and insomnia. Altered extrasynaptic receptor function is implicated in insomnia, stroke and Angelman and Fragile X syndromes, and drugs targeting these receptors are used to treat postpartum depression. Tonic GABAergic responses are moderated to avoid excessive suppression of neuronal communication, and can exhibit high sensitivity to Zn blockade, in contrast to synapse-preferring α1βγ, α2βγ and α3βγ receptor responses. Here, to resolve these distinctive features, we determined structures of the predominantly extrasynaptic αβ GABA receptor class. An inhibited state bound by both the lethal paralysing agent α-cobratoxin and Zn was used in comparisons with GABA-Zn and GABA-bound structures. Zn nullifies the GABA response by non-competitively plugging the extracellular end of the pore to block chloride conductance. In the absence of Zn, the GABA signalling response initially follows the canonical route until it reaches the pore. In contrast to synaptic GABA receptors, expansion of the midway pore activation gate is limited and it remains closed, reflecting the intrinsic low efficacy that characterizes the extrasynaptic receptor. Overall, this study explains distinct traits adopted by αβ receptors that adapt them to a role in tonic signalling.
External linksNature / PubMed:35140402 / PubMed Central
MethodsEM (single particle)
Resolution2.79 - 3.04 Å
Structure data

EMDB-13290, PDB-7pbd:
a1b3 GABA-A receptor + GABA
Method: EM (single particle) / Resolution: 3.04 Å

EMDB-13314: a1b3 GABA-A receptor + GABA
PDB-7pbz: a1b3 GABA-A receptor + GABA + Zn2+
Method: EM (single particle) / Resolution: 2.79 Å

EMDB-13315, PDB-7pc0:
GABA-A receptor bound by a-Cobratoxin
Method: EM (single particle) / Resolution: 3.0 Å

Chemicals

ChemComp-ABU:
GAMMA-AMINO-BUTANOIC ACID / neurotransmitter, inhibitor*YM / Γ-Aminobutyric acid

ChemComp-NAG:
2-acetamido-2-deoxy-beta-D-glucopyranose / N-Acetylglucosamine

ChemComp-HSM:
HISTAMINE / neurotransmitter, hormone*YM / Histamine

ChemComp-UND:
UNDECANE / Undecane

ChemComp-OCT:
N-OCTANE / Octane

ChemComp-HEX:
HEXANE / Hexane

ChemComp-ZN:
Unknown entry

ChemComp-D10:
DECANE / Decane

Source
  • homo sapiens (human)
  • lama glama (llama)
  • naja kaouthia (monocled cobra)
  • monocled cobra (monocled cobra)
KeywordsMEMBRANE PROTEIN / pLGIC GABA Neurotransmission / neurotransmission / toxin / GABA

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