Ethosuximide reduces epileptogenesis and behavioral comorbidity in the <scp>GAERS</scp> model of genetic generalized epilepsy

Dezsi, Gabi; Öztürk, Ezgi; Stanić, Davor; Powell, Kim L.; Blumenfeld, Hal; O’Brien, Terence J.; Jones, Nigel C.

doi:10.1111/epi.12118

Cited by 104 publications

(91 citation statements)

References 48 publications

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“…In the WAG/Rij rat model of absence epilepsy, early prophylactic treatment with ethosuximide, levetiracetam, or zonisamide (but not carbamazepine) before the onset of spike-wave discharges in the EEG suppressed the development of such absence-like seizures [31][32][33], which was also subsequently observed in the GAERS model of absence epilepsy [34]. These findings suggest that models are available in which epileptogenesis can be controlled and that early treatment during development may provide a strategy for preventing genetic epilepsy in susceptible individuals.…”

Section: Studies With Aedsmentioning

confidence: 65%

Searching for the Ideal Antiepileptogenic Agent in Experimental Models: Single Treatment Versus Combinatorial Treatment Strategies

White

Löscher²

2014

Neurotherapeutics

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A major unmet medical need is the lack of treatments to prevent (or modify) epilepsy in patients at risk, for example, after epileptogenic brain insults such as traumatic brain injury, stroke, or prolonged acute symptomatic seizures like complex febrile seizures or status epilepticus. Typically, following such brain insults there is a seizure-free interval ("latent period"), lasting months to years before the onset of spontaneous recurrent epileptic seizures. The latent period after a brain insult offers a window of opportunity in which an appropriate treatment may prevent or modify the epileptogenic process induced by a brain insult. A similar latent period occurs in patients with epileptogenic gene mutations. Studies using animal models of epilepsy have led to a greater understanding of the factors underlying epileptogenesis and have provided significant insight into potential targets by which the development of epilepsy may be prevented or modified. This review focuses largely on some of the most common animal models of epileptogenesis and their potential utility for evaluating proposed antiepileptogenic therapies and identifying useful biomarkers. The authors also describe some of the limitations of using animal models in the search for therapies that move beyond the symptomatic treatment of epilepsy. Promising results of previous studies designed to evaluate antiepileptogenesis and the role of monotherapy versus polytherapy approaches are also discussed. Recent data from both models of genetic and acquired epilepsies strongly indicate that it is possible to prevent or modify epileptogenesis, and, hopefully, such promising results can ultimately be translated into the clinic.

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Section: Studies With Aedsmentioning

confidence: 65%

Searching for the Ideal Antiepileptogenic Agent in Experimental Models: Single Treatment Versus Combinatorial Treatment Strategies

White

Löscher²

2014

Neurotherapeutics

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“…It is difficult to know at this time whether the striking reduction in the risk of developing GTCs in those assigned to ethosuximide (even many years later when off the medication) represents a disease modification effect, as was suggested by an observational study 12 and by animal data. 13,14 Longer duration of follow-up with focus on remission outcomes is in progress and may provide a more definitive answer. However, the data provide compelling evidence that concern about the occurrence of GTCs should not change the status of ethosuximide as the preferred first-line therapy for CAE.…”

Section: Resultsmentioning

confidence: 99%

Long-term outcomes of generalized tonic-clonic seizures in a childhood absence epilepsy trial

Shinnar

Cnaan²,

Hu³

et al. 2015

Neurology

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Objective: To determine incidence and early predictors of generalized tonic-clonic seizures (GTCs) in children with childhood absence epilepsy (CAE).Methods: Occurrence of GTCs was determined in 446 children with CAE who participated in a randomized clinical trial comparing ethosuximide, lamotrigine, and valproate as initial therapy for CAE.Results: As of June 2014, the cohort had been followed for a median of 7.0 years since enrollment and 12% (53) have experienced at least one GTC. The median time to develop GTCs from initial therapy was 4.7 years. The median age at first GTC was 13.1 years. Fifteen (28%) were not on medications at the time of their first GTC. On univariate analysis, older age at enrollment was associated with a higher risk of GTCs (p 5 20.0009), as was the duration of the shortest burst on the baseline EEG (p 5 0.037). Failure to respond to initial treatment (p , 0.001) but not treatment assignment was associated with a higher rate of GTCs. Among patients initially assigned to ethosuximide, 94% (15/16) with GTCs experienced initial therapy failure (p , 0.0001). A similar but more modest effect was noted in those initially treated with valproate (p 5 0.017) and not seen in those initially treated with lamotrigine. Conclusions:The occurrence of GTCs in a well-characterized cohort of children with CAE appears lower than previously reported. GTCs tend to occur late in the course of the disorder. Children initially treated with ethosuximide who are responders have a particularly low risk of developing subsequent GTCs. Neurology ® 2015;85:1108-1114 GLOSSARY AED 5 antiepileptic drug; CAE 5 childhood absence epilepsy; CI 5 confidence interval; GTC 5 generalized tonic-clonic seizure; HR 5 hazard ratio; IQR 5 interquartile range; JAE 5 juvenile absence epilepsy; RCT 5 randomized controlled trial.Childhood absence epilepsy (CAE) is the most common childhood-onset epilepsy syndrome, accounting for 10%-17% of all childhood-onset epilepsy.1,2 Although the core seizure type in CAE is absence seizures, studies have reported that generalized tonic-clonic seizures (GTCs) occur in 30%-60% of children with CAE.3,4 Lack of clarity about the homogeneity of these reports' study populations means the incidence of GTCs remains unclear. The timing of GTC onset in children with CAE is also imprecise but GTCs tend to occur late in the course of CAE with latencies of 5-10 years after syndrome onset. 3,4 A double-blind randomized controlled trial (RCT) of initial therapy for children with CAE enrolled 446 children with newly diagnosed CAE (without a history of GTCs) and randomized them to ethosuximide, lamotrigine, or valproate. 5,6 This cohort was well-characterized with pretreatment and subsequent prospective longitudinal assessment of seizure status, EEG, cognition, and behavioral status. The RCT identified ethosuximide as the optimal initial therapy due to superior efficacy compared with lamotrigine and similar efficacy but fewer attentional side effects when compared to valproic acid. 5,6 The results of th...

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“…The corollary applies to seizure termination, which may depend on reversal of tonic inhibition through still undefined endogenous mechanisms. A second issue of clinical importance is the recent finding that early treatment with ethosuximide hinders the epileptogenesis of absence epilepsy in both humans (Berg et al, 2014) and rodents (Dezsi et al, 2013). Since drug treatment does not correct the genetic mutation, it must drive altered activity-dependent changes in developmental gene expression that raise the threshold for oscillations, including those that regulate the strength of feedforward inhibition.…”

mentioning

confidence: 99%

Monogenic models of absence epilepsy

Maheshwari

Noebels

2014

Progress in Brain Research

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Ethosuximide reduces epileptogenesis and behavioral comorbidity in the GAERS model of genetic generalized epilepsy

Cited by 104 publications

References 48 publications

Searching for the Ideal Antiepileptogenic Agent in Experimental Models: Single Treatment Versus Combinatorial Treatment Strategies

Searching for the Ideal Antiepileptogenic Agent in Experimental Models: Single Treatment Versus Combinatorial Treatment Strategies

Long-term outcomes of generalized tonic-clonic seizures in a childhood absence epilepsy trial

Monogenic models of absence epilepsy

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