Article ID Journal Published Year Pages File Type
6275830 Neuroscience 2012 10 Pages PDF
Abstract

Our previous work has correlated permanent alterations in the rat neurosecretory machinery with epileptogenesis. Such findings highlighted the need for a greater understanding of the molecular mechanisms underlying epilepsy so that novel therapeutic regimens can be designed. To this end, we examined kindling in transgenic mice with a defined reduction of a key element of the neurosecretory machinery: the v-SNARE (vesicle-bound SNAP [soluble NSF attachment protein] receptor), synaptobrevin/vesicle-associated membrane protein 2 (VAMP2). Initial analysis of biochemical markers, which previously displayed kindling-dependent alterations in rat hippocampal synaptosomes, showed similar trends in both wild-type and VAMP2+/− mice, demonstrating that kindled rat and mouse models are comparable. This report focuses on the effects that a ∼50% reduction of synaptosomal VAMP2 has on the progression of electrical kindling and on glutamate release in hippocampal subregions. Our studies show that epileptogenesis is dramatically attenuated in VAMP2+/− mice, requiring both higher current and more stimulations to reach a fully kindled state (two successive Racine stage 5 seizures). Progression through the five identifiable Racine stages was slower and more variable in the VAMP2+/− animals compared with the almost linear progression seen in wild-type littermates. Consistent with the expected effects of reducing a major neuronal v-SNARE, glutamate-selective, microelectrode array (MEA) measurements in specific hippocampal subregions of VAMP2+/− mice showed significant reductions in potassium-evoked glutamate release. Taken together these studies demonstrate that manipulating the levels of the neurosecretory machinery not only affects neurotransmitter release but also mitigates kindling-induced epileptogenesis.

▶The v-SNARE, VAMP2, was reduced by 60% in hippocampal synaptosomes of VAMP2+/− mice compared with VAMP2+/+littermates. ▶Amygdala kindling was attenuated in VAMP2+/− vs. VAMP2+/+ mice, requiring a higher AD threshold and more stimuli. ▶Progression through kindling stages oscillated in VAMP2+/− vs. an almost linear progression seen in VAMP2+/+ littermates. ▶One month post-kindling there was increased ipsilateral 7SC and bilateral SV2, greater in VAMP2+/+ than VAMP2+/− hippocampus. ▶One month post-kindling there were reductions of KCl-evoked glutamate release in VAMP2+/− compared with VAMP2+/+ DG and CA3.

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