The role of GABA sub(A) beta 2 subunit-containing receptors in mediating the anticonvulsant and sedative effects of loreclezole

The majority of inhibitory neurotransmission in the brain is mediated by the gamma -aminobutyric acid (GABA) type A (GABA sub(A)) receptor. The anticonvulsant loreclezole largely acts by potentiating GABA sub(A) receptors containing beta 2 and beta 3 subunits. We used a genetically modified mouse co...

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Bibliographic Details
Published in:The European journal of neuroscience 2006-07, Vol.24 (1), p.167-174
Main Authors: Groves, James O, Guscott, Martin R, Hallett, David J, Rosahl, Thomas W, Pike, Andrew, Davies, Amy, Wafford, Keith A, Reynolds, David S
Format: Article
Language:English
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Summary:The majority of inhibitory neurotransmission in the brain is mediated by the gamma -aminobutyric acid (GABA) type A (GABA sub(A)) receptor. The anticonvulsant loreclezole largely acts by potentiating GABA sub(A) receptors containing beta 2 and beta 3 subunits. We used a genetically modified mouse containing a loreclezole-insensitive beta 2 subunit ( beta 2N265S) to determine the role of this subunit in mediating the sedative and anticonvulsive effects of loreclezole. Sedation was assessed by measuring spontaneous locomotor activity and beam walking performance, and anticonvulsant efficacy was determined by pentylenetetrazole (PTZ) and amygdala kindling-induced seizures. The beta 2N265S mice did not exhibit loreclezole-mediated sedation as shown by normal locomotor activity and beam walking performance. However, loreclezole also failed to provide significant protection against PTZ-induced seizures in the beta 2N265S mice. Reduced efficacy against amygdala-kindled seizures, both acutely and over a 13-day chronic dosing study, was also observed in beta 2N265S mice. These results suggest that the majority of the sedative effects and a significant proportion of the anticonvulsant efficacy of loreclezole are mediated via beta 2-containing GABA sub(A) receptors.
ISSN:0953-816X
1460-9568
DOI:10.1111/j.1460-9568.2006.04890.x