An intersubunit electrostatic interaction in the GABAA receptor facilitates its responses to benzodiazepines

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Abstract

Benzodiazepines are positive allosteric modulators of the GABAA receptor (GABAAR), acting at the – subunit interface to enhance GABAAR function. GABA or benzodiazepine binding induces distinct conformational changes in the GABAAR. The molecular rearrangements in the GABAAR following benzodiazepine binding remain to be fully elucidated. Using two molecular models of the GABAAR, we identified electrostatic interactions between specific amino acids at the – subunit interface that were broken by, or formed after, benzodiazepine binding. Using two-electrode voltage clamp electrophysiology in Xenopus laevis oocytes, we investigated these interactions by substituting one or both amino acids of each potential pair. We found that Lys104 in the 1 subunit forms an electrostatic bond with Asp75 of the 2 subunit after benzodiazepine binding and that this bond stabilizes the positively modified state of the receptor. Substitution of these two residues to cysteine and subsequent covalent linkage between them increased the receptor’s sensitivity to low GABA concentrations and decreased its response to benzodiazepines, producing a GABAAR that resembles a benzodiazepine-bound WT GABAAR. Breaking this bond restored sensitivity to GABA to WT levels and increased the receptor’s response to benzodiazepines. The 1 Lys104 and 2 Asp75 interaction did not play a role in ethanol or neurosteroid modulation of GABAAR, suggesting that different modulators induce different conformational changes in the receptor. These findings may help explain the additive or synergistic effects of modulators acting at the GABAAR.

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Pflanz, N. C., Daszkowski, A. W., Cornelison, G. L., Trudell, J. R., & John Mihic, S. (2018). An intersubunit electrostatic interaction in the GABAA receptor facilitates its responses to benzodiazepines. Journal of Biological Chemistry, 293(21), 8264–8274. https://doi.org/10.1074/jbc.RA118.002128

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