2017
DOI: 10.1111/epi.13579
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A novel animal model of acquired human temporal lobe epilepsy based on the simultaneous administration of kainic acid and lorazepam

Abstract: We show here that the effects of systemic KA can be limited to the hippocampus simply with coadministration of a benzodiazepine at a low dose. This means that lorazepam can block convulsive seizures without truly stopping seizure activity. This novel, cSE-free animal model reliably mimics the defining characteristics of acquired mesial TLE: hippocampal sclerosis and spontaneous hippocampal-onset seizures after a prolonged seizure-free period, without significant morbidity, mortality, or nonresponders.

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Cited by 22 publications
(26 citation statements)
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“…The KaL model also recapitulates essential characteristics of human TLE, such as hippocampal sclerosis and hippocampal‐onset epilepsy after a discreet seizure‐free period (Kienzler‐Norwood et al, ). Animals received 15 mg/kg kainic acid monohydrate (10 mg/ml in phosphate‐buffered saline, K0250, Sigma‐Aldrich, Germany) and 0.75 mg/kg lorazepam (2 mg/ml, Pfizer, Germany) that was administered subcutaneously, while the control animals received 15 mg/kg kainic acid monohydrate and 3 mg/kg lorazepam.…”
Section: Methodsmentioning
confidence: 99%
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“…The KaL model also recapitulates essential characteristics of human TLE, such as hippocampal sclerosis and hippocampal‐onset epilepsy after a discreet seizure‐free period (Kienzler‐Norwood et al, ). Animals received 15 mg/kg kainic acid monohydrate (10 mg/ml in phosphate‐buffered saline, K0250, Sigma‐Aldrich, Germany) and 0.75 mg/kg lorazepam (2 mg/ml, Pfizer, Germany) that was administered subcutaneously, while the control animals received 15 mg/kg kainic acid monohydrate and 3 mg/kg lorazepam.…”
Section: Methodsmentioning
confidence: 99%
“…The aim of this study was to discover reference genes for two rat models of epilepsy: 8‐hr perforant pathway stimulation (PPS) (Norwood et al, ) and systemic kainate‐lorazepam (KaL) during epileptogenesis and/or chronic epilepsy, and after acute, noninjurious seizures (30‐min PPS) (Norwood et al, ). The mRNA expression levels of 15 (Kienzler‐Norwood et al, ) potential reference genes were determined in hippocampi from treated and control animals. Four different validated and established methods to determine expression stability were used: geNorm (Vandesompele et al, ), NormFinder (Andersen, Jensen, & Ørntoft, ), BestKeeper (Pfaffl, Tichopad, Prgomet, & Neuvians, ), and Delta‐Ct (ΔCt) (Silver, Best, Jiang, & Thein, ).…”
Section: Introductionmentioning
confidence: 99%
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“…Many available animal models of Mesial Temporal lobe epilepsy (mTLE), and in particular systemic KA administration, are induced by acute treatments that often are associated with high mortality and experimental variability rates (Hellier et al, 1998; McLin and Steward, 2006; Kienzler-Norwood et al, 2017). Modeling mTLE using experimental animals comprises, in general, three well-defined stages: First, an initiating insult to the brain, such as febrile seizures, head trauma, stroke, or strong seizures leading to status epilepticus (SE).…”
Section: Introductionmentioning
confidence: 99%
“…Furthermore, several of the above-mentioned models induce varying mortality rates and are accompanied by severe animal welfare issues (Curia et al, 2008; Lévesque and Avoli, 2013; Lidster et al, 2016). Therefore, preclinical epilepsy research would benefit from more detailed and standardized protocols, with lower mortality rates and improved animal welfare, which could increase intra- and inter-laboratory reproducibility (Lidster et al, 2016; Kienzler-Norwood et al, 2017). …”
Section: Introductionmentioning
confidence: 99%