A KCNQ2 Splice Site Mutation Causing Benign Neonatal Convulsions in a Scottish Family

W. L. Lee; C. Biervert; K. Hallmann; A. Tay; J. C. S. Dean; O. K. Steinlein

doi:10.1055/s-2000-15290

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Neuropediatrics 2000; 31(1): 9-12
DOI: 10.1055/s-2000-15290

Original Article

Georg Thieme Verlag Stuttgart · New York

A KCNQ2 Splice Site Mutation Causing Benign Neonatal Convulsions in a Scottish Family

W. L. Lee¹ , C. Biervert² , K. Hallmann² , A. Tay¹ , J. C.S. Dean³ , O. K. Steinlein²

¹Department of Pediatrics, National University of Singapore, Singapore
²Institute for Human Genetics, University of Bonn, Bonn, Germany
³Aberdeen Royal Hospital, Department of Medical Genetics, Aberdeen Royal Infirmary, Scotland, UK

Further Information

Publication History

February 12, 1999

August 31, 1999

Publication Date:
31 December 2000 (online)

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Benign familial neonatal convulsions (BFNC) are one of the rare idiopathic epilepsies with autosomal dominant mode of inheritance. Two voltage-gated potassium channels, KCNQ2 on chromosome 20q13.3 and KCNQ3 on 8q24, have been recently identified as the genes responsible for BFNC. Here we describe a large family with BFNC in which we found a previously undescribed mutation in the KCNQ2 gene. A 1187⁺²T/G nucleotide exchange affects the conserved donor splice site motif in intron 9. This mutation can be predicted to give rise to aberrant splicing of the primary transcript. There was a wide range of clinical manifestations in this family. An unusual clinical feature is the occurrence of partial seizures in later life with corresponding focal neurological deficits.

Key words

Epilepsy - Gene mutation - Potassium channel