Literature DB >> 35819138

BK channel properties correlate with neurobehavioral severity in three KCNMA1-linked channelopathy mouse models.

Su Mi Park1, Cooper E Roache1, Philip H Iffland2, Hans J Moldenhauer1, Katia K Matychak1, Amber E Plante1, Abby G Lieberman3, Peter B Crino2, Andrea Meredith1.   

Abstract

KCNMA1 forms the pore of BK K+ channels, which regulate neuronal and muscle excitability. Recently, genetic screening identified heterozygous KCNMA1 variants in a subset of patients with debilitating paroxysmal non-kinesigenic dyskinesia, presenting with or without epilepsy (PNKD3). However, the relevance of KCNMA1 mutations and the basis for clinical heterogeneity in PNKD3 has not been established. Here, we evaluate the relative severity of three KCNMA1 patient variants in BK channels, neurons, and mice. In heterologous cells, BKN999S and BKD434G channels displayed gain-of-function (GOF) properties, whereas BKH444Q channels showed loss-of-function (LOF) properties. The relative degree of channel activity was BKN999S > BKD434G>WT > BKH444Q. BK currents and action potential firing were increased, and seizure thresholds decreased, in Kcnma1N999S/WT and Kcnma1D434G/WT transgenic mice but not Kcnma1H444Q/WT mice. In a novel behavioral test for paroxysmal dyskinesia, the more severely affected Kcnma1N999S/WT mice became immobile after stress. This was abrogated by acute dextroamphetamine treatment, consistent with PNKD3-affected individuals. Homozygous Kcnma1D434G/D434G mice showed similar immobility, but in contrast, homozygous Kcnma1H444Q/H444Q mice displayed hyperkinetic behavior. These data establish the relative pathogenic potential of patient alleles as N999S>D434G>H444Q and validate Kcnma1N999S/WT mice as a model for PNKD3 with increased seizure propensity.
© 2022, Park et al.

Entities:  

Keywords:  BK channel; KCNMA1; calcium-activated potassium channel; dentate gyrus; epilepsy; mouse; neuroscience; paroxysmal non-kinesigenic dyskinesia

Mesh:

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Year:  2022        PMID: 35819138      PMCID: PMC9275823          DOI: 10.7554/eLife.77953

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.713


  116 in total

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  1 in total

1.  Effect of an autism-associated KCNMB2 variant, G124R, on BK channel properties.

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  1 in total

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