Human KCNQ5 de novo mutations underlie epilepsy and intellectual disability

Aguan D Wei; Paul Wakenight; Theresa A Zwingman; Angela M Bard; Nikhil Sahai; Marjolein H Willemsen; Helenius J Schelhaas; Alexander P A Stegmann; Judith S Verhoeven; Stella A de Man; Marja W Wessels; Tjitske Kleefstra; Deepali N Shinde; Katherine L Helbig; Alice Basinger; Victoria F Wagner; David Rodriguez-Buritica; Emily Bryant; John J Millichap; Kathleen J Millen; William B Dobyns; Jan-Marino Ramirez; Franck K Kalume

doi:10.1152/jn.00509.2021

Human KCNQ5 de novo mutations underlie epilepsy and intellectual disability

J Neurophysiol. 2022 Jul 1;128(1):40-61. doi: 10.1152/jn.00509.2021. Epub 2022 May 18.

Authors

Aguan D Wei¹, Paul Wakenight¹, Theresa A Zwingman¹, Angela M Bard¹, Nikhil Sahai¹, Marjolein H Willemsen^{2

3}, Helenius J Schelhaas⁴, Alexander P A Stegmann⁵, Judith S Verhoeven⁴, Stella A de Man^{6

7}, Marja W Wessels⁷, Tjitske Kleefstra², Deepali N Shinde⁸, Katherine L Helbig^{8

9}, Alice Basinger¹⁰, Victoria F Wagner¹¹, David Rodriguez-Buritica¹¹, Emily Bryant¹², John J Millichap^{12

13

14}, Kathleen J Millen^{1

15}, William B Dobyns^{1

15

16}, Jan-Marino Ramirez^{1

17}, Franck K Kalume^{1

17}

Affiliations

¹ Center for Integrative Brain Research, Seattle Children's Research Institute, Seattle, Washington.
² Department of Human Genetics and Donders Institute for Brain, Cognition and Behaviour, Radboud University Medical Center, Nijmegen, The Netherlands.
³ Department of Human Genetics, Maastricht University Medical Centre, Maastricht, The Netherlands.
⁴ Department of Neurology, Academic Centre for Epileptology Kempenhaeghe, Heeze, The Netherlands.
⁵ Department of Clinical Genetics, Maastricht University Medical Centre, Maastricht, The Netherlands.
⁶ Department of Pediatrics, Amphia Hospital, Breda, The Netherlands.
⁷ Department of Human Genetics, Erasmus Medical Centre, Rotterdam, The Netherlands.
⁸ Ambry Genetics, Aliso Viejo, California.
⁹ Division of Neurology, Children's Hospital of Philadelphia, Philadelphia, Pennsylvania.
¹⁰ Medical Genetics, Cook Children's Hospital, Fort Worth, Texas.
¹¹ Department of Pediatrics, University of Texas Health Science Center, Houston, Texas.
¹² Department of Pediatrics, Northwestern University Feinberg School of Medicine, Chicago, Illinois.
¹³ Department of Neurology, Northwestern University Feinberg School of Medicine, Chicago, Illinois.
¹⁴ Epilepsy Center, Ann & Robert H. Lurie Children's Hospital of Chicago, Chicago, Illinois.
¹⁵ Department of Pediatrics, University of Washington School of Medicine, Seattle, Washington.
¹⁶ Department of Neurology, University of Washington School of Medicine, Seattle, Washington.
¹⁷ Department of Neurological Surgery, University of Washington School of Medicine, Seattle, Washington.

Abstract

We identified six novel de novo human KCNQ5 variants in children with motor/language delay, intellectual disability (ID), and/or epilepsy by whole exome sequencing. These variants, comprising two nonsense and four missense alterations, were functionally characterized by electrophysiology in HEK293/CHO cells, together with four previously reported KCNQ5 missense variants (Lehman A, Thouta S, Mancini GM, Naidu S, van Slegtenhorst M, McWalter K, Person R, Mwenifumbo J, Salvarinova R; CAUSES Study; EPGEN Study; Guella I, McKenzie MB, Datta A, Connolly MB, Kalkhoran SM, Poburko D, Friedman JM, Farrer MJ, Demos M, Desai S, Claydon T. Am J Hum Genet 101: 65-74, 2017). Surprisingly, all eight missense variants resulted in gain of function (GOF) due to hyperpolarized voltage dependence of activation or slowed deactivation kinetics, whereas the two nonsense variants were confirmed to be loss of function (LOF). One severe GOF allele (P369T) was tested and found to extend a dominant GOF effect to heteromeric KCNQ5/3 channels. Clinical presentations were associated with altered KCNQ5 channel gating: milder presentations with LOF or smaller GOF shifts in voltage dependence [change in voltage at half-maximal conduction (ΔV₅₀) = ∼-15 mV] and severe presentations with larger GOF shifts in voltage dependence (ΔV₅₀ = ∼-30 mV). To examine LOF pathogenicity, two Kcnq5 LOF mouse lines were created with CRISPR/Cas9. Both lines exhibited handling- and thermal-induced seizures and abnormal cortical EEGs consistent with epileptiform activity. Our study thus provides evidence for in vivo KCNQ5 LOF pathogenicity and strengthens the contribution of both LOF and GOF mutations to global pediatric neurological impairment, including ID/epilepsy.NEW & NOTEWORTHY Six novel de novo human KCNQ5 variants were identified from children with neurodevelopmental delay, intellectual disability, and/or epilepsy. Expression of these variants along with four previously reported KCNQ5 variants from a similar cohort revealed GOF potassium channels, negatively shifted in V₅₀ of activation and/or delayed deactivation kinetics. GOF is extended to KCNQ5/3 heteromeric channels, making these the predominant channels affected in heterozygous de novo patients. Kcnq5 LOF mice exhibited seizures, consistent with in vivo pathogenicity.

Keywords: KCNQ5; M current; channelopathy; epilepsy; intellectual disability.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Child
Cricetinae
Cricetulus
Epilepsy* / genetics
HEK293 Cells
Humans
Intellectual Disability* / genetics
KCNQ Potassium Channels
Mice
Mutation, Missense
Seizures

Substances

KCNQ Potassium Channels
KCNQ5 protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding