Literature DB >> 31783100

Screening for Efficacious Anticonvulsants and Neuroprotectants in Delayed Treatment Models of Organophosphate-induced Status Epilepticus.

Bryan S Barker1, Jay Spampanato2, Hilary S McCarren3, Melissa Smolik2, Cecelia E Jackson3, Eden N Hornung3, David T Yeung4, F Edward Dudek2, John H McDonough3.   

Abstract

Organophosphorus (OP) compounds are deadly chemicals that exert their intoxicating effects through the irreversible inhibition of acetylcholinesterase (AChE). In addition to an excess of peripheral ailments, OP intoxication induces status epilepticus (SE) which if left untreated may lead to permanent brain damage or death. Benzodiazepines are typically the primary therapies for OP-induced SE, but these drugs lose efficacy as treatment time is delayed. The CounterACT Neurotherapeutic Screening (CNS) Program was therefore established by the National Institutes of Health (NIH) to discover novel treatments that may be administered adjunctively with the currently approved medical countermeasures for OP-induced SE in a delayed treatment scenario. The CNS program utilizes in vivo EEG recordings and Fluoro-JadeB (FJB) histopathology in two established rat models of OP-induced SE, soman (GD) and diisopropylfluorophosphate (DFP), to evaluate the anticonvulsant and neuroprotectant efficacy of novel adjunct therapies when administered at 20 or 60 min after the induction of OP-induced SE. Here we report the results of multiple compounds that have previously shown anticonvulsant or neuroprotectant efficacy in other models of epilepsy or trauma. Drugs tested were ganaxolone, diazoxide, bumetanide, propylparaben, citicoline, MDL-28170, and chloroquine. EEG analysis revealed that ganaxolone demonstrated the most robust anticonvulsant activity, whereas all other drugs failed to attenuate ictal activity in both models of OP-induced SE. FJB staining demonstrated that none of the tested drugs had widespread neuroprotective abilities. Overall these data suggest that neurosteroids may represent the most promising anticonvulsant option for OP-induced SE out of the seven unique mechanisms tested here. Additionally, these results suggest that drugs that provide significant neuroprotection from OP-induced SE without some degree of anticonvulsant activity are elusive, which further highlights the necessity to continue screening novel adjunct treatments through the CNS program.
Copyright © 2019 IBRO. All rights reserved.

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Keywords:  anticonvulsant; diisopropylfluorophosphate; nerve agent; neuroprotectant; organophosphorus; status epilepticus

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Year:  2019        PMID: 31783100      PMCID: PMC6935402          DOI: 10.1016/j.neuroscience.2019.11.020

Source DB:  PubMed          Journal:  Neuroscience        ISSN: 0306-4522            Impact factor:   3.708


  70 in total

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Journal:  Neurotoxicology       Date:  2010-06-08       Impact factor: 4.294

Review 5.  Neuroactive steroids for the treatment of status epilepticus.

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Review 8.  Possible alterations in GABAA receptor signaling that underlie benzodiazepine-resistant seizures.

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Review 9.  Development of neuropathology following soman poisoning and medical countermeasures.

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10.  Antiseizure and neuroprotective effects of delayed treatment with midazolam in a rodent model of organophosphate exposure.

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2.  The Kv7 Modulator, Retigabine, is an Efficacious Antiseizure Drug for Delayed Treatment of Organophosphate-induced Status Epilepticus.

Authors:  Bryan S Barker; Jay Spampanato; Hilary S McCarren; Kyle Berger; Cecelia E Jackson; David T Yeung; F Edward Dudek; John H McDonough
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3.  Comparative profile of refractory status epilepticus models following exposure of cholinergic agents pilocarpine, DFP, and soman.

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4.  Allopregnanolone and perampanel as adjuncts to midazolam for treating diisopropylfluorophosphate-induced status epilepticus in rats.

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  4 in total

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