Low nanomolar GABA effects at extrasynaptic α4β1/β3δ GABAA receptor subtypes indicate a different binding mode for GABA at these receptors

Ionotropic GABAA receptors are a highly heterogenous population of receptors assembled from a combination of multiple subunits. The aims of this study were to characterize the potency of GABA at human recombinant δ-containing extrasynaptic GABAA receptors expressed in Xenopus oocytes using the two-electrode voltage clamp technique, and to investigate, using site-directed mutagenesis, the molecular determinants for GABA potency at α4β3δ GABAA receptors. α4/δ-Containing GABAA receptors displayed high sensitivity to GABA, with mid-nanomolar concentrations activating α4β1δ (EC50 = 24 nM) and α4β3δ (EC50 = 12 nM) receptors. In the majority of oocytes expressing α4β3δ subtypes, GABA produced a biphasic concentration-response curve, and activated the receptor with low and high concentrations (EC50(1) = 16 nM; EC50(2) = 1.2 μM). At α4β2δ, GABA had low micromolar activity (EC50 = 1 μM). An analysis of 10 N-terminal singly mutated α4β3δ receptors shows that GABA interacts with amino acids different to those reported for α1β2γ2 GABAA receptors. Residues Y205 and R207 of the β3-subunit significantly affected GABA potency, while the residue F71 of the α4- and the residue Y97 of the β3-subunit did not significantly affect GABA potency. Mutating the residue R218 of the δ-subunit, equivalent to the GABA binding residue R207 of the β2-subunit, reduced the potency of GABA by 670-fold, suggesting a novel GABA binding site at the δ-subunit interface. Taken together, GABA may have different binding modes for extrasynaptic δ-containing GABAA receptors compared to their synaptic counterparts.

Graphical abstractGABA displays high and low potencies for α4β3δ GABAA receptors. GABA potency is affected by loop C residues β3Y205, β3R207 and δR218.Figure optionsDownload full-size imageDownload as PowerPoint slide