Mono-allelic KCNB2 variants lead to a neurodevelopmental syndrome caused by altered channel inactivation.

Creator(s)

Shreyas Bhat
Justine Rousseau
Coralie Michaud
Charles Marques Lourenço
Joan M. Stoler
Raymond J. Louie
Lola K. Clarkson
Angie Lichty
Daniel C. Koboldt
Shalini C. Reshmi
Sanjay M. Sisodiya
Eva M M Hoytema van Konijnenburg
Klaas Koop
Peter M. van Hasselt
Florence Démurger
Christèle Dubourg
Bonnie Sullivan, Children's Mercy HospitalFollow
Susan S. Hughes
Isabelle Thiffault, Children's Mercy HospitalFollow
Elisabeth Simard Tremblay
Andrea Accogli
Myriam Srour
Rikard Blunck
Philippe M. Campeau

Document Type

Article

Publication Date

4-4-2024

Identifier

DOI: 10.1016/j.ajhg.2024.02.014

Abstract

Ion channels mediate voltage fluxes or action potentials that are central to the functioning of excitable cells such as neurons. The KCNB family of voltage-gated potassium channels (Kv) consists of two members (KCNB1 and KCNB2) encoded by KCNB1 and KCNB2, respectively. These channels are major contributors to delayed rectifier potassium currents arising from the neuronal soma which modulate overall excitability of neurons. In this study, we identified several mono-allelic pathogenic missense variants in KCNB2, in individuals with a neurodevelopmental syndrome with epilepsy and autism in some individuals. Recurrent dysmorphisms included a broad forehead, synophrys, and digital anomalies. Additionally, we selected three variants where genetic transmission has not been assessed, from two epilepsy studies, for inclusion in our experiments. We characterized channel properties of these variants by expressing them in oocytes of Xenopus laevis and conducting cut-open oocyte voltage clamp electrophysiology. Our datasets indicate no significant change in absolute conductance and conductance-voltage relationships of most disease variants as compared to wild type (WT), when expressed either alone or co-expressed with WT-KCNB2. However, variants c.1141A>G (p.Thr381Ala) and c.641C>T (p.Thr214Met) show complete abrogation of currents when expressed alone with the former exhibiting a left shift in activation midpoint when expressed alone or with WT-KCNB2. The variants we studied, nevertheless, show collective features of increased inactivation shifted to hyperpolarized potentials. We suggest that the effects of the variants on channel inactivation result in hyper-excitability of neurons, which contributes to disease manifestations.

Journal Title

American journal of human genetics

Volume

111

Issue

4

First Page

761

Last Page

777

MeSH Keywords

Animals; Humans; Action Potentials; Epilepsy; Mutation, Missense; Neurons; Oocytes; Xenopus laevis; Shab Potassium Channels; Neurodevelopmental Disorders

Keywords

KCNB2; channel inactivation, neurodevelopmental disorders, voltage-gated potassium channels; dysmorphism; epilepsy; global developmental delay

Recommended Citation

Bhat S, Rousseau J, Michaud C, et al. Mono-allelic KCNB2 variants lead to a neurodevelopmental syndrome caused by altered channel inactivation. Am J Hum Genet. 2024;111(4):761-777. doi:10.1016/j.ajhg.2024.02.014