Journal
BRITISH JOURNAL OF PHARMACOLOGY
Volume 168, Issue 5, Pages 1088-1100Publisher
WILEY
DOI: 10.1111/j.1476-5381.2012.02132.x
Keywords
anticonvulsant; antiepileptic drug; ONO-2506; microdialysis; astrocyte; kynurenic acid
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Funding
- Japanese Ministry of Education, Science and Culture [23659564, 22390224]
- Mitsubishi Pharma Research Foundation
- Japan Epilepsy Research Foundation
- Grants-in-Aid for Scientific Research [23659564, 22390224] Funding Source: KAKEN
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Background and Purpose Anticonvulsants have been developed according to the traditional neurotransmission imbalance hypothesis. However, the anticonvulsive pharmacotherapy currently available remains unsatisfactory. To develop new antiepileptic drugs with novel antiepileptic mechanisms, we have tested the antiepileptic actions of ONO-2506, a glial modulating agent, and its effects on tripartite synaptic transmission. Experimental Approach Dose-dependent effects of ONO-2506 on maximal-electroshock seizure (MES), pentylenetetrazol-induced seizure (PTZ) and epileptic discharge were determined in a genetic model of absence epilepsy in mice (Cacna1atm2Nobs/tm2Nobs strain). Antiepileptic mechanisms of ONO-2506 were analysed by examining the interaction between ONO-2506 and transmission-modulating toxins (tetanus toxin, fluorocitrate, tetrodotoxin) on release of l-glutamate, d-serine, GABA and kynurenic acid in the medial-prefrontal cortex (mPFC) of freely moving rats using microdialysis and primary cultured rat astrocytes. Key Results ONO-2506 inhibited spontaneous epileptic discharges in Cacna1atm2Nobs/tm2Nobs mice without affecting MES or PTZ. Given systemically, ONO-2506 increased basal release of GABA and kynurenic acid in the mPFC through activation of both neuronal and glial exocytosis, but inhibited depolarization-induced releases of all transmitters. ONO-2506 increased basal glial release of kynurenic acid without affecting those of l-glutamate, d-serine or GABA. However, ONO-2506 inhibited AMPA-induced releases of l-glutamate, d-serine, GABA and kynurenic acid. Conclusions and Implications ONO-2506 did not affect traditional convulsive tests but markedly inhibited epileptic phenomena in the genetic epilepsy mouse model. ONO-2506 enhanced release of inhibitory neuro- and gliotransmitters during the resting stage and inhibited tripartite transmission during the hyperactive stage. The results suggest that ONO-2506 is a novel potential glial-targeting antiepileptic drug. Linked Article This article is commented on by Onat, pp. 10861087 of this issue. To view this commentary visit http://dx.doi.org/10.1111/bph.12050
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