A potassium channel mutation in neonatal human epilepsy
C Biervert, BC Schroeder, C Kubisch, SF Berkovic… - Science, 1998 - science.org
C Biervert, BC Schroeder, C Kubisch, SF Berkovic, P Propping, TJ Jentsch, OK Steinlein
Science, 1998•science.orgBenign familial neonatal convulsions (BFNC) is an autosomal dominant epilepsy of infancy,
with loci mapped to human chromosomes 20q13. 3 and 8q24. By positional cloning, a
potassium channel gene (KCNQ2) located on 20q13. 3 was isolated and found to be
expressed in brain. Expression of KCNQ2 in frog (Xenopus laevis) oocytes led to potassium-
selective currents that activated slowly with depolarization. In a large pedigree with BFNC, a
five–base pair insertion would delete more than 300 amino acids from the KCNQ2 carboxyl …
with loci mapped to human chromosomes 20q13. 3 and 8q24. By positional cloning, a
potassium channel gene (KCNQ2) located on 20q13. 3 was isolated and found to be
expressed in brain. Expression of KCNQ2 in frog (Xenopus laevis) oocytes led to potassium-
selective currents that activated slowly with depolarization. In a large pedigree with BFNC, a
five–base pair insertion would delete more than 300 amino acids from the KCNQ2 carboxyl …
Benign familial neonatal convulsions (BFNC) is an autosomal dominant epilepsy of infancy, with loci mapped to human chromosomes 20q13.3 and 8q24. By positional cloning, a potassium channel gene (KCNQ2) located on 20q13.3 was isolated and found to be expressed in brain. Expression of KCNQ2 in frog (Xenopus laevis) oocytes led to potassium-selective currents that activated slowly with depolarization. In a large pedigree with BFNC, a five–base pair insertion would delete more than 300 amino acids from the KCNQ2 carboxyl terminus. Expression of the mutant channel did not yield measurable currents. Thus, impairment of potassium-dependent repolarization is likely to cause this age-specific epileptic syndrome.
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