Recurrent seizures and brain pathology after inhibition of glutamine synthetase in the hippocampus in rats

doi:10.1093/brain/awn133

Brain Advance Access published online on July 6, 2008
Brain, doi:10.1093/brain/awn133

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Recurrent seizures and brain pathology after inhibition of glutamine synthetase in the hippocampus in rats

Tore Eid¹^,2, Arko Ghosh², Yue Wang², Henning Beckström²^,5, Hitten P. Zaveri³, Tih-Shih W. Lee⁴, James C. K. Lai⁶, Gauri H. Malthankar-Phatak⁶ and Nihal C. de Lanerolle²

¹Department of Laboratory Medicine, ²Department of Neurosurgery, ³Department of Neurology and ⁴Department of Psychiatry, Yale University School of Medicine, New Haven, CT, USA, ⁵Institute for Basic Medical Sciences, University of Oslo, Oslo, Norway and ⁶Department of Biomedical and Pharmaceutical Sciences, College of Pharmacy and Idaho State University Biomedical Research Institute, Idaho State University, Pocatello, ID, USA

Correspondence to: Tore Eid, MD, PhD, Department of Laboratory Medicine, Yale University School of Medicine, 333 Cedar Street, P.O. Box 208035, New Haven, CT 06520-8035, USA E-mail: tore.eid{at}yale.edu

An excess of extracellular glutamate in the hippocampus hasbeen linked to the generation of recurrent seizures and brainpathology in patients with medically intractable mesial temporallobe epilepsy (MTLE). However, the mechanism which results inglutamate excess in MTLE remains unknown. We recently reportedthat the glutamate-metabolizing enzyme glutamine synthetaseis deficient in the hippocampus in patients with MTLE, and wepostulated that this deficiency is critically involved in thepathophysiology of the disease. To further explore the roleof glutamine synthetase in MTLE we created a novel animal modelof hippocampal glutamine synthetase deficiency by continuous( $~$ 28 days) microinfusion of methionine sulfoximine (MSO: 0.625to 2.5 µg/h) unilaterally into the hippocampus in rats.This treatment led to a deficiency in hippocampal glutaminesynthetase activity by 82–97% versus saline. The majority(>95%) of the MSO-treated animals exhibited recurrent seizuresthat continued for several weeks. Some of the MSO-treated animalsexhibited neuropathological features that were similar to mesialtemporal sclerosis, such as hippocampal atrophy and patternedloss of hippocampal neurons. However, many MSO-treated animalsdisplayed only minimal injury to the hippocampus, with no clearevidence of mesial temporal sclerosis. These findings supportthe hypothesis that a deficiency in hippocampal glutamine synthetasecauses recurrent seizures, even in the absence of classicalmesial temporal sclerosis, and that restoration of glutaminesynthetase may represent a novel approach to therapeutic interventionin this disease.

Key Words: astrocyte; epileptiform EEG discharges; animal models; glutamate; temporal lobes

Abbreviations: CA1-3, cornu ammonis subfields 1–3 of the hippocampus; MSO, methionine sulfoximine; MTLE, mesial temporal lobe epilepsy

Received March 10, 2008. Revised May 30, 2008. Accepted June 2, 2008.

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