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Novel KCNQ3 muation in a large family with benign familial neonatal epilepsy: a rare cause of neonatal seizures

Benign familial neonatal seizures (BFNS) present a rare familial epilepsy syndrome caused by genetic alterations in the voltage-gated potassium channels Kv7.2 and Kv7.3, encoded by <i>KCNQ2</i> and <i>KCNQ3.</i> While most BFNS families carry alterations in <i>KCNQ2<...

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Main Authors: Maljevic, Snezana (Author) , Vejzovic, Sabina (Author) , Bernhard, Matthias K. (Author) , Bertsche, Astrid (Author) , Weise, Sebastian (Author) , Döcker, Miriam (Author) , Lerche, Holger (Author) , Lemke, Johannes R. (Author) , Merkenschlager, Andreas (Author) , Syrbe, Steffen (Author)
Format: Article (Journal)
Language:English
Published: July 7, 2016
In: Molecular syndromology
Year: 2016, Volume: 7, Issue: 4, Pages: 189-196
ISSN:1661-8777
DOI:10.1159/000447461
Online Access:Verlag, lizenzpflichtig, Volltext: https://doi.org/10.1159/000447461
Verlag, lizenzpflichtig, Volltext: https://www.karger.com/Article/FullText/447461
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Author Notes:Snezana Maljevic, Sabina Vejzovic, Matthias K. Bernhard, Astrid Bertsche, Sebastian Weise, Miriam Döcker, Holger Lerche, Johannes R. Lemke, Andreas Merkenschlager, Steffen Syrbe
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Summary:Benign familial neonatal seizures (BFNS) present a rare familial epilepsy syndrome caused by genetic alterations in the voltage-gated potassium channels Kv7.2 and Kv7.3, encoded by <i>KCNQ2</i> and <i>KCNQ3.</i> While most BFNS families carry alterations in <i>KCNQ2</i>, mutations in <i>KCNQ3</i> appear to be less common. Here, we describe a family with 6 individuals presenting with neonatal focal and generalized seizures. Genetic testing revealed a novel <i>KCNQ3</i> variant, c.835G>T, cosegregating with seizures in 4 tested individuals. This variant results in a substitution of the highly conserved amino acid valine localized within the pore-forming transmembrane segment S5 (p.V279F). Functional investigations in <i>Xenopus laevis</i> oocytes revealed a loss of function, which supports p.V279F as a pathogenic mutation. When p.V279F was coexpressed with the wild-type (WT) Kv7.2 subunits, the resulting potassium currents were about 10-fold reduced compared to the WT Kv7.3 and Kv7.2 coexpression. Genotype-phenotype correlation shows an incomplete penetrance of p.V279F. Response to antiepileptic treatment was variable, but evaluation of treatment response remained challenging due to the self-limiting character of the disease. The identification of the pathogenic variant helped to avoid unnecessary investigations in affected family members and allowed guided therapy.
Item Description:Gesehen am 06.05.2020
Physical Description:Online Resource
ISSN:1661-8777
DOI:10.1159/000447461

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