Analysis of Plasma Multiplex Cytokines for Children With Febrile Seizures and Severe Acute Encephalitis

Hu, Meihua; Huang, Go-Shine; Wu, Chieh‐Tsai; Lin, Jainn-Jim; Hsia, Shao‐Hsuan; Wang, Huei-Shyong; Lin, Kuang-Lin

doi:10.1177/0883073813488829

Cited by 21 publications

(23 citation statements)

References 20 publications

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“…Some related articles were excluded because of unvalued data (Dias De Sousa et al, 2012), lack of specific values (mean ± SD) ( Masuyama et al, 2002;Virta et al, 2002b;Ichiyama et al, 2004Ichiyama et al, , 2008Ichiyama et al, , 2009Stoeck et al, 2006;Yamanaka et al, 2006Yamanaka et al, , 2010Fukumoto et al, 2007;Sinha et al, 2008 Asano et al, 2010;Blyth et al, 2011;Mathieu et al, 2011;Haberlandt et al, 2013), lack of a control group without any neurological complications interfered with immunological response or using baseline references (Billiau et al, 2007;Alapirtti et al, 2009;Bauer et al, 2009;Li et al, 2013;Uludag et al, 2013), concomitant disorders in epileptic cases [e.g., depression (Lehtimäki et al, 2008) and neurocysticercosis (Evans et al, 1998)], concomitant disorders in the control group (e.g., encephalitis) (Ichiyama et al, 1998;Hu et al, 2014), and replicated data (Peltola et al, 2002). Some abstracts seemed to be related, but full-text was not available to make sure if they met the inclusion criteria or not (Ling et al, 1993;Kawakami et al, 1999b;Haspolat et al, 2002;Ganor et al, 2005;Makis et al, 2005;Lehtimäki et al, 2010;Lukaszewicz et al, 2010;Majoie et al, 2010;Mine et al, 2013).…”

Section: Resultsmentioning

confidence: 97%

Proinflammatory and anti-inflammatory cytokines in febrile seizures and epilepsy: systematic review and meta-analysis

Saghazadeh

Gharedaghi

Meysamie

et al. 2014

Reviews in the Neurosciences

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Section: Resultsmentioning

confidence: 97%

Proinflammatory and anti-inflammatory cytokines in febrile seizures and epilepsy: systematic review and meta-analysis

Saghazadeh

Gharedaghi

Meysamie

et al. 2014

Reviews in the Neurosciences

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“…Reductions in seizure threshold in TMEV‐infected mice highlight its potential as a useful, and technically feasible biomarker of epileptogenesis; this would also provide a more cost‐effective surrogate for chronic video‐EEG recordings for moderate‐throughput drug studies. Changes in threshold that lead to symptomatic seizures are often associated with increased expression of inflammatory markers in animal seizure models and human patients . For example, transgenic mice that overexpress TNF‐α and IL‐6 demonstrate neurologic dysfunction including cell loss, decreased seizure threshold, and SRS .…”

Section: Discussionmentioning

confidence: 99%

“…The mechanisms by which viral encephalitis contributes to epilepsy are unclear, but the risk for developing epilepsy after viral encephalitis with seizures increases 22‐fold . It is likely that viral infection of the CNS underlies the development of chronic epilepsy due to increased expression of inflammatory cytokines, lowered seizure threshold, and increased risk of status epilepticus . In both the developed and developing world, infection‐induced encephalitis can promote the onset of temporal lobe epilepsy (TLE).…”

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confidence: 99%

Acute treatment with minocycline, but not valproic acid, improves long‐term behavioral outcomes in the Theiler's virus model of temporal lobe epilepsy

et al. 2016

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Summary Objective Infection with Theiler’s murine encephalomyelitis virus (TMEV) in C57Bl/6J mice induces acute seizures and development of spontaneous recurrent seizures and behavioral comorbidities weeks later. The present studies sought to determine whether acute therapeutic intervention with an anti-inflammatory–based approach could prevent or modify development of TMEV-induced long-term behavioral comorbidities. Valproic acid (VPA), in addition to its prototypical anticonvulsant properties, inhibits histone deacetylase (HDAC) activity, which may alter expression of the inflammasome. Minocycline (MIN) has previously demonstrated an antiseizure effect in the TMEV model via direct anti-inflammatory mechanisms, but the long-term effect of MIN treatment on the development of chronic behavioral comorbidities is unknown. Methods Mice infected with TMEV were acutely administered MIN (50 mg/kg, b.i.d. and q.d.) or VPA (100 mg/kg, q.d.) during the 7-day viral infection period. Animals were evaluated for acute seizure severity and subsequent development of chronic behavioral comorbidities and seizure threshold. Results Administration of VPA reduced the proportion of mice with seizures, delayed onset of symptomatic seizures, and reduced seizure burden during the acute infection. This was in contrast to the effects of administration of once-daily MIN, which did not affect the proportion of mice with seizures nor delay onset of acute symptomatic seizures. However, VPA-treated mice were no different from VEH-treated mice in long-term behavioral outcomes, including open field activity and seizure threshold. Once-daily MIN treatment, despite no effect on the maximum observed Racine stage seizure severity, was associated with improved long-term behavioral outcomes and normalized seizure threshold. Significance Acute seizure control alone is insufficient to modify chronic disease comorbidities in the TMEV model. This work further supports the role of an inflammatory response in the development of chronic behavioral comorbidities and further highlights the utility of this platform for the development of mechanistically-novel pharmacotherapies for epilepsy.

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“…Human patients with viral infection-induced encephalitis who present with seizures during the acute infection period are up to 22 times more likely to develop spontaneous, unprovoked seizures than the general population (Annegers et al, 1988). More importantly, inflammation represents a significant risk factor for seizure induction and maintenance, with proinflammatory cytokines being highly expressed in various animal seizure models (Pernot et al, 2011;Vezzani and Friedman, 2011) and patients with epilepsy (Kan et al, 2012;He et al, 2013;Hu et al, 2014). In fact, some seizure-induced proinflammatory signaling molecules remain upregulated during epileptogenesis (VoutsinosPorche et al, 2004;Ravizza et al, 2008;Maroso et al, 2010) and may be essential to the establishment of spontaneous recurrent seizures associated with temporal lobe epilepsy (TLE) .…”

Section: Introductionmentioning

confidence: 99%

Evaluating an Etiologically Relevant Platform for Therapy Development for Temporal Lobe Epilepsy: Effects of Carbamazepine and Valproic Acid on Acute Seizures and Chronic Behavioral Comorbidities in the Theiler’s Murine Encephalomyelitis Virus Mouse Model

Barker‐Haliski

Dahle

Heck

et al. 2015

J Pharmacol Exp Ther

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Central nervous system infections can underlie the development of epilepsy, and Theiler's murine encephalomyelitis virus (TMEV) infection in C57BL/6J mice provides a novel model of infectioninduced epilepsy. Approximately 50-65% of infected mice develop acute, handling-induced seizures during the infection. Brains display acute neuropathology, and a high number of mice develop spontaneous, recurrent seizures and behavioral comorbidities weeks later. This study characterized the utility of this model for drug testing by assessing whether antiseizure drug treatment during the acute infection period attenuates handlinginduced seizures, and whether such treatment modifies associated comorbidities. Male C57BL/6J mice infected with TMEV received twice-daily valproic acid (VPA; 200 mg/kg), carbamazepine (CBZ; 20 mg/kg), or vehicle during the infection (days 0-7). Mice were assessed twice daily during the infection period for handling-induced seizures. Relative to vehicle-treated mice, more CBZ-treated mice presented with acute seizures; VPA conferred no change. In mice displaying seizures, VPA, but not CBZ, reduced seizure burden. Animals were then randomly assigned to acute and long-term follow-up. VPA was associated with significant elevations in acute (day 8) glial fibrillary acidic protein (astrocytes) immunoreactivity, but did not affect NeuN (neurons) immunoreactivity. Additionally, VPA-treated mice showed improved motor performance 15 days postinfection (DPI). At 36 DPI, CBZ-treated mice traveled significantly less distance through the center of an open field, indicative of anxiety-like behavior. CBZ-treated mice also presented with significant astrogliosis 36 DPI. Neither CBZ nor VPA prevented long-term reductions in NeuN immunoreactivity. The TMEV model thus provides an etiologically relevant platform to evaluate potential treatments for acute seizures and disease modification.

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Analysis of Plasma Multiplex Cytokines for Children With Febrile Seizures and Severe Acute Encephalitis

Cited by 21 publications

References 20 publications

Proinflammatory and anti-inflammatory cytokines in febrile seizures and epilepsy: systematic review and meta-analysis

Proinflammatory and anti-inflammatory cytokines in febrile seizures and epilepsy: systematic review and meta-analysis

Acute treatment with minocycline, but not valproic acid, improves long‐term behavioral outcomes in the Theiler's virus model of temporal lobe epilepsy

Evaluating an Etiologically Relevant Platform for Therapy Development for Temporal Lobe Epilepsy: Effects of Carbamazepine and Valproic Acid on Acute Seizures and Chronic Behavioral Comorbidities in the Theiler’s Murine Encephalomyelitis Virus Mouse Model

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