4.7 Article

Neuron-Restrictive Silencer Factor-Mediated Hyperpolarization-Activated Cyclic Nucleotide Gated Channelopathy in Experimental Temporal Lobe Epilepsy

ANNALS OF NEUROLOGY (2011)

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Journal

ANNALS OF NEUROLOGY
Volume 70, Issue 3, Pages 454-464

Publisher

WILEY
DOI: 10.1002/ana.22479

Keywords

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Categories

Clinical Neurology Neurosciences

Funding

  1. National Institutes of Neurological Disorders and Stroke [R37 NS35439]
  2. French Institute of Health and Medical Research
  3. Fondation Francaise pour la Recherche sur l'Epilepsie French Foundation for Epilepsy Research''
  4. Fondation pour la Recherche sur le Cerveau Foundation for Brain Research
  5. Agence Nationale pour la Recherche National Research Agency''
  6. Citizens United for Research in Epilepsy
  7. Alberta Heritage Foundation
  8. [NS45540]

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Objective: Enduring, abnormal expression and function of the ion channel hyperpolarization-activated cyclic adenosine monophosphate gated channel type 1 (HCN1) occurs in temporal lobe epilepsy (TLE). We examined the underlying mechanisms, and investigated whether interfering with these mechanisms could modify disease course. Methods: Experimental TLE was provoked by kainic acid-induced status epilepticus (SE). HCN1 channel repression was examined at mRNA, protein, and functional levels. Chromatin immunoprecipitation was employed to identify the transcriptional mechanism of repressed HCN1 expression, and the basis for their endurance. Physical interaction of the repressor, NRSF, was abolished using decoy oligodeoxynucleotides (ODNs). Video/electroencephalographic recordings were performed to assess the onset and initial pattern of spontaneous seizures. Results: Levels of NRSF and its physical binding to the Hcn1 gene were augmented after SE, resulting in repression of HCN1 expression and HCN1-mediated currents (I-h), and reduced I-h-dependent resonance in hippocampal CA1 pyramidal cell dendrites. Chromatin changes typical of enduring, epigenetic gene repression were apparent at the Hcn1 gene within a week after SE. Administration of decoy ODNs comprising the NRSF DNA-binding sequence (neuron restrictive silencer element [NRSE]), in vitro and in vivo, reduced NRSF binding to Hcn1, prevented its repression, and restored I-h function. In vivo, decoy NRSE ODN treatment restored theta rhythm and altered the initial pattern of spontaneous seizures. Interpretation: Acquired HCN1 channelopathy derives from NRSF-mediated transcriptional repression that endures via chromatin modification and may provide insight into the mechanisms of a number of channelopathies that coexist with, and may contribute to, the conversion of a normal brain into an epileptic one. ANN NEUROL 2011;70:454-464

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