Hippocampal β2-GABAA receptors mediate LTP suppression by etomidate and contribute to long-lasting feedback but not feedforward inhibition of pyramidal neurons

Alexander G Figueroa; Claudia Benkwitz; Gabe Surges; Nicholas Kunz; Gregg E Homanics; Robert A Pearce

doi:10.1152/jn.00303.2021

Hippocampal β2-GABA_A receptors mediate LTP suppression by etomidate and contribute to long-lasting feedback but not feedforward inhibition of pyramidal neurons

J Neurophysiol. 2021 Oct 1;126(4):1090-1100. doi: 10.1152/jn.00303.2021. Epub 2021 Aug 18.

Authors

Alexander G Figueroa¹, Claudia Benkwitz^{1

2}, Gabe Surges¹, Nicholas Kunz², Gregg E Homanics², Robert A Pearce¹

Affiliations

¹ Department of Anesthesiology, University of Wisconsin-Madison, Madison, Wisconsin.
² Department of Anesthesiology and Perioperative Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania.

Abstract

The general anesthetic etomidate, which acts through γ-aminobutyric acid type A (GABA_A) receptors, impairs the formation of new memories under anesthesia. This study addresses the molecular and cellular mechanisms by which this occurs. Here, using a new line of genetically engineered mice carrying the GABA_A receptor (GABA_AR) β2-N265M mutation, we tested the roles of receptors that incorporate GABA_A receptor β2 versus β3 subunits to suppression of long-term potentiation (LTP), a cellular model of learning and memory. We found that brain slices from β2-N265M mice resisted etomidate suppression of LTP, indicating that the β2-GABA_ARs are an essential target in this model. As these receptors are most heavily expressed by interneurons in the hippocampus, this finding supports a role for interneuron modulation in etomidate control of synaptic plasticity. Nevertheless, β2 subunits are also expressed by pyramidal neurons, so they might also contribute. Therefore, using a previously established line of β3-N265M mice, we also examined the contributions of β2- versus β3-GABA_ARs to GABA_A,slow dendritic inhibition, because dendritic inhibition is particularly well suited to controlling synaptic plasticity. We also examined their roles in long-lasting suppression of population activity through feedforward and feedback inhibition. We found that both β2- and β3-GABA_ARs contribute to GABA_A,slow inhibition and that both β2- and β3-GABA_ARs contribute to feedback inhibition, whereas only β3-GABA_ARs contribute to feedforward inhibition. We conclude that modulation of β2-GABA_ARs is essential to etomidate suppression of LTP. Furthermore, to the extent that this occurs through GABA_ARs on pyramidal neurons, it is through modulation of feedback inhibition.NEW & NOTEWORTHY Etomidate exerts its anesthetic actions through GABA_A receptors. However, the mechanism remains unknown. Here, using a hippocampal brain slice model, we show that β2-GABA_ARs are essential to this effect. We also show that these receptors contribute to long-lasting dendritic inhibition in feedback but not feedforward inhibition of pyramidal neurons. These findings hold implications for understanding how anesthetics block memory formation and, more generally, how inhibitory circuits control learning and memory.

Keywords: GABAA receptors; etomidate; general anesthesia; learning and memory.

MeSH terms

Anesthetics, Intravenous / pharmacology*
Animals
Etomidate / pharmacology*
Hippocampus / drug effects*
Long-Term Potentiation / drug effects*
Mice
Mice, Inbred C57BL
Mice, Transgenic
Neural Inhibition / drug effects*
Pyramidal Cells / drug effects*
Receptors, GABA-A / drug effects*

Substances

Anesthetics, Intravenous
Gabrb2 protein, mouse
Gabrb3 protein, mouse
Receptors, GABA-A
Etomidate

Abstract

MeSH terms

Substances

Grants and funding