Literature DB >> 19334075

A KCNQ channel opener for experimental neonatal seizures and status epilepticus.

Yogendrasinh H Raol1, David A Lapides, Jeffery G Keating, Amy R Brooks-Kayal, Edward C Cooper.   

Abstract

OBJECTIVE: Neonatal seizures occur frequently, are often refractory to anticonvulsants, and are associated with considerable morbidity and mortality. Genetic and electrophysiological evidence indicates that KCNQ voltage-gated potassium channels are critical regulators of neonatal brain excitability. This study tests the hypothesis that selective openers of KCNQ channels may be effective for treatment of neonatal seizures.
METHODS: We induced seizures in postnatal day 10 rats with either kainic acid or flurothyl. We measured seizure activity using quantified behavioral rating and electrocorticography. We compared the efficacy of flupirtine, a selective KCNQ channel opener, with phenobarbital and diazepam, two drugs in current use for neonatal seizures.
RESULTS: Unlike phenobarbital or diazepam, flupirtine prevented animals from experiencing development of status epilepticus when administered before kainate. In the flurothyl model, phenobarbital and diazepam increased latency to seizure onset, but flupirtine completely prevented seizures throughout the experiment. Flupirtine was also effective in arresting electrographic and behavioral seizures when administered after animals had developed continuous kainate-induced status epilepticus. Flupirtine caused dose-related sedation and suppressed electroencephalographic activity but did not result in respiratory suppression or result in any mortality.
INTERPRETATION: Flupirtine appears more effective than either of two commonly used antiepileptic drugs, phenobarbital and diazepam, in preventing and suppressing seizures in both the kainic acid and flurothyl models of symptomatic neonatal seizures. KCNQ channel openers merit further study as potential treatments for seizures in infants and children.

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Year:  2009        PMID: 19334075      PMCID: PMC2666110          DOI: 10.1002/ana.21593

Source DB:  PubMed          Journal:  Ann Neurol        ISSN: 0364-5134            Impact factor:   10.422


  51 in total

1.  M channel KCNQ2 subunits are localized to key sites for control of neuronal network oscillations and synchronization in mouse brain.

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3.  KCNQ2 is a nodal K+ channel.

Authors:  Jérôme J Devaux; Kleopas A Kleopa; Edward C Cooper; Steven S Scherer
Journal:  J Neurosci       Date:  2004-02-04       Impact factor: 6.167

4.  Age-dependent modulation of hippocampal excitability by KCNQ-channels.

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5.  Antiepileptic drugs and apoptotic neurodegeneration in the developing brain.

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Review 6.  M-channels: neurological diseases, neuromodulation, and drug development.

Authors:  Edward C Cooper; Lily Y Jan
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7.  Epilepsy after early-life seizures can be independent of hippocampal injury.

Authors:  Yogendra Sinh H Raol; Elaine C Budreck; Amy R Brooks-Kayal
Journal:  Ann Neurol       Date:  2003-04       Impact factor: 10.422

8.  Efficacy of flupirtine on cognitive function in patients with CJD: A double-blind study.

Authors:  M Otto; L Cepek; P Ratzka; S Doehlinger; I Boekhoff; J Wiltfang; E Irle; G Pergande; B Ellers-Lenz; O Windl; H A Kretzschmar; S Poser; H Prange
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9.  KCNQ2 and KCNQ3 potassium channel genes in benign familial neonatal convulsions: expansion of the functional and mutation spectrum.

Authors:  Nanda A Singh; Peter Westenskow; Carole Charlier; Chris Pappas; Jonathan Leslie; Jessica Dillon; V Elving Anderson; Michael C Sanguinetti; Mark F Leppert
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10.  M channels containing KCNQ2 subunits modulate norepinephrine, aspartate, and GABA release from hippocampal nerve terminals.

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2.  Status epilepticus: Role for etiology in determining response to benzodiazepines.

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3.  Progressive NKCC1-dependent neuronal chloride accumulation during neonatal seizures.

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Review 4.  Neonatal seizures: controversies and challenges in translating new therapies from the lab to the isolette.

Authors:  Kevin E Chapman; Yogendra H Raol; Amy Brooks-Kayal
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5.  Development of later life spontaneous seizures in a rodent model of hypoxia-induced neonatal seizures.

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6.  Ischemic injury suppresses hypoxia-induced electrographic seizures and the background EEG in a rat model of perinatal hypoxic-ischemic encephalopathy.

Authors:  A Zayachkivsky; M J Lehmkuhle; J J Ekstrand; F E Dudek
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7.  Anticonvulsant effect of flupirtine in an animal model of neonatal hypoxic-ischemic encephalopathy.

Authors:  Dayalan Sampath; Robert Valdez; Andrew M White; Yogendra H Raol
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10.  Neonatal seizures.

Authors:  Hannah C Glass; Joseph E Sullivan
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