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Hyperkalemic periodic paralysis associated with a novel missense variant located in the inner pore of Nav1.4

Brain and Development, ISSN: 0387-7604, Vol: 45, Issue: 4, Page: 205-211
2023
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Reports Outline Hyperkalemic Periodic Paralysis Findings from Osaka University (Hyperkalemic Periodic Paralysis Associated With a Novel Missense Variant Located In the Inner Pore of Nav1.4)

2023 MAY 01 (NewsRx) -- By a News Reporter-Staff News Editor at Japan Daily Report -- Research findings on Nutritional and Metabolic Diseases and Conditions

Article Description

Hyperkalemic periodic paralysis (HyperPP) is an autosomal dominantly inherited disease characterized by episodic paralytic attacks with hyperkalemia, and is caused by mutations of the SCN4A gene encoding the skeletal muscle type voltage-gated sodium channel Nav1.4. The pathological mechanism of HyperPP was suggested to be associated with gain-of-function changes for Nav1.4 gating, some of which are defects of slow inactivation. We identified a HyperPP family consisting of the proband and his mother, who showed a novel heterozygous SCN4A variant, p.V792G, in an inner pore lesion of segment 6 in Domain II of Nav1.4. Clinical and neurophysiological evaluations were conducted for the proband and his mother. We explored the pathogenesis of the variant by whole-cell patch clamp technique using HEK293T cells expressing the mutant Nav1.4 channel. Functional analysis of Nav1.4 with the V792G mutation revealed a hyperpolarized shift of voltage-dependent activation and fast inactivation. Moreover, steady-state slow inactivation in V792G was impaired with larger residual currents in comparison with wild-type Nav1.4. V792G in SCN4A is a pathogenic variant associated with the HyperPP phenotype and the inner pore lesion of Nav1.4 plays a crucial role in slow inactivation.

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