Nootropic Agents Enhance the Recruitment of Fast GABAA Inhibition in Rat Neocortex

doi:10.1093/cercor/bhh191

Cerebral Cortex Advance Access published online on September 30, 2004
Cerebral Cortex, doi:10.1093/cercor/bhh191
© 2004 by Oxford University Press

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Article

Nootropic Agents Enhance the Recruitment of Fast GABA_A Inhibition in Rat Neocortex

Douglas S.F. Ling ¹^* and Larry S. Benardo ²

¹ Department of Physiology and Pharmacology, State University of New York Downstate Medical Center, Brooklyn, NY 11203, USA
² Department of Physiology and Pharmacology, State University of New York Downstate Medical Center, Brooklyn, NY 11203, USA; Department of Neurology, State University of New York Downstate Medical Center, Brooklyn, NY 11203, USA

^* To whom correspondence should be addressed. E-mail: dling{at}downstate.edu.

Abstract

It is widely believed that nootropic (cognition-enhancing)agents produce their therapeutic effects by augmenting excitatorysynaptic transmission in cortical circuits, primarily throughpositive modulation of ${alpha}$ -amino-3-hydroxy-5-methyl-4-isoxazole-propionatereceptors (AMPARs). However, GABA-mediated inhibition is alsocritical for cognition, and enhanced GABA function may be likewisetherapeutic for cognitive disorders. Could nootropics act throughsuch a mechanism as well? To address this question, we examinedthe effects of nootropic agents on excitatory and inhibitorypostsynaptic currents (EPSCs and IPSCs) recorded from layerV pyramidal cells in acute slices of somatosensory cortex. Aniracetam,a positive modulator of AMPA/kainate receptors, increased thepeak amplitude of evoked EPSCs and the amplitude and durationof polysynaptic fast IPSCs, manifested as a greater total chargecarried by IPSCs. As a result, the EPSC/IPSC ratio of totalcharge was decreased, representing a shift in the excitation-inhibitionbalance that favors inhibition. Aniracetam did not affect themagnitude of either monosynaptic IPSCs (mono-IPSCs) recordedin the presence of excitatory amino acid receptor antagonists,or miniature IPSCs (mIPSCs) recorded in the presence of tetrodotoxin.However, the duration of both mono-IPSCs and mIPSCs was prolonged,suggesting that aniracetam also directly modulates GABAergictransmission. Cyclothiazide, a preferential modulator of AMPARfunction, enhanced the magnitude and duration of polysynapticIPSCs, similar to aniracetam, but did not affect mono-IPSCs.Concanavalin A, a kainate receptor modulator, had little effecton EPSCs or IPSCs, suggesting there was no contribution fromkainate receptor activity. These findings indicate that AMPARmodulators strengthen inhibition in neocortical pyramidal cells,most likely by altering the kinetics of AMPARs on synapticallyconnected interneurons and possibly by modulating GABA_A receptorresponses in pyramidal cells. This suggests that the therapeuticactions of nootropic agents may be partly mediated through enhancedcortical GABAergic inhibition, and not solely through the directmodification of excitation, as previously thought.

Keywords: aniracetam; cortex; cyclothiazide; EPSC; IPSC; synaptic inhibition.

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