4.7 Article

Network-Related Changes in Neurotransmitters and Seizure Propagation During Rodent Epileptogenesis

Journal

NEUROLOGY
Volume 96, Issue 18, Pages E2261-E2271

Publisher

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1212/WNL.0000000000011846

Keywords

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Funding

  1. Swebilius Family Trust
  2. NIH [NS058674, NS070824, NS109062, NS109734]
  3. National Center for Advancing Translational Sciences (NCATS, a component of the NIH) [RR024139]
  4. Citizens United for Research in Epilepsy
  5. University of Oslo (Unifor, Forskerlinjen, and SERTA)

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The study found that changes in glutamate and GABA levels may play important roles in the formation of epilepsy networks and the initiation and propagation of spontaneous seizures during epileptogenesis.
Objective To test the hypothesis that glutamate and GABA are linked to the formation of epilepsy networks and the triggering of spontaneous seizures, we examined seizure initiation/propagation characteristics and neurotransmitter levels during epileptogenesis in a translationally relevant rodent model of mesial temporal lobe epilepsy. Methods The glutamine synthetase (GS) inhibitor methionine sulfoximine was infused into one of the hippocampi in laboratory rats to create a seizure focus. Long-term video-intracranial EEG recordings and brain microdialysis combined with mass spectrometry were used to examine seizure initiation, seizure propagation, and extracellular brain levels of glutamate and GABA. Results All seizures (n = 78 seizures, n = 3 rats) appeared first in the GS-inhibited hippocampus of all animals, followed by propagation to the contralateral hippocampus. Propagation time decreased significantly from 11.65 seconds early in epileptogenesis (weeks 1-2) to 6.82 seconds late in epileptogenesis (weeks 3-4, paired t test, p = 0.025). Baseline extracellular glutamate levels were 11.6-fold higher in the hippocampus of seizure propagation (7.3 mu M) vs the hippocampus of seizure onset (0.63 mu M, analysis of variance/Fisher least significant difference, p = 0.01), even though the concentrations of the major glutamate transporter proteins excitatory amino acid transporter subtypes 1 and 2 and xCT were unchanged between the brain regions. Finally, extracellular GABA in the seizure focus decreased significantly from baseline several hours before a spontaneous seizure (paired t test/false discovery rate). Conclusion The changes in glutamate and GABA suggest novel and potentially important roles of the amino acids in epilepsy network formation and in the initiation and propagation of spontaneous seizures.

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