Lethal digenic mutations in the K+ channels Kir4.1 (KCNJ10) and SLACK (KCNT1) associated with severe-disabling seizures and neurodevelopmental delay

Sonia Hasan; Ameera Balobaid; Alessandro Grottesi; Omar Dabbagh; Marta Cenciarini; Rifaat Rawashdeh; Afaf Al-Sagheir; Cecilia Bove; Lara Macchioni; Mauro Pessia; Mohammed Al-Owain; Maria Cristina D'Adamo

doi:10.1152/jn.00284.2017

Lethal digenic mutations in the K⁺ channels Kir4.1 (KCNJ10) and SLACK (KCNT1) associated with severe-disabling seizures and neurodevelopmental delay

J Neurophysiol. 2017 Oct 1;118(4):2402-2411. doi: 10.1152/jn.00284.2017. Epub 2017 Jul 26.

Authors

Sonia Hasan¹, Ameera Balobaid², Alessandro Grottesi³, Omar Dabbagh⁴, Marta Cenciarini⁵, Rifaat Rawashdeh², Afaf Al-Sagheir⁶, Cecilia Bove⁵, Lara Macchioni⁵, Mauro Pessia^{5

7}, Mohammed Al-Owain^{2

8}, Maria Cristina D'Adamo^{9

10}

Affiliations

¹ Department of Physiology, Faculty of Medicine, Kuwait University, Safat, Kuwait.
² Department of Medical Genetics, King Faisal Specialist Hospital and Research Centre, Riyadh, Saudi Arabia.
³ Super Computing Applications and Innovation-CINECA, Rome, Italy.
⁴ Department of Neurosciences, King Faisal Specialist Hospital and Research Centre, Riyadh, Saudi Arabia.
⁵ Section of Physiology and Biochemistry, Department of Experimental Medicine, School of Medicine, University of Perugia, Perugia, Italy.
⁶ Department of Pediatrics, King Faisal Specialist Hospital and Research Centre, Riyadh, Saudi Arabia.
⁷ Department of Physiology and Biochemistry, Faculty of Medicine and Surgery, University of Malta, Msida, Malta.
⁸ College of Medicine, AlFaisal University, Riyadh, Saudi Arabia; and.
⁹ Department of Physiology and Biochemistry, Faculty of Medicine and Surgery, University of Malta, Msida, Malta; cristina.dadamo@um.edu.mt.
¹⁰ Fondazione Santa Lucia, IRCCS, Rome, Italy.

Abstract

A 2-yr-old boy presented profound developmental delay, failure to thrive, ataxia, hypotonia, and tonic-clonic seizures that caused the death of the patient. Targeted and whole exome sequencing revealed two heterozygous missense variants: a novel mutation in the KCNJ10 gene that encodes for the inward-rectifying K⁺ channel Kir4.1 and another previously characterized mutation in KCNT1 that encodes for the Na⁺-activated K⁺ channel known as Slo2.2 or SLACK. The objectives of this study were to perform the clinical and genetic characterization of the proband and his family and to examine the functional consequence of the Kir4.1 mutation. The mutant and wild-type KCNJ10 constructs were generated and heterologously expressed in Xenopus laevis oocytes, and whole cell K⁺ currents were measured using the two-electrode voltage-clamp technique. The KCNJ10 mutation c.652C>T resulted in a p.L218F substitution at a highly conserved residue site. Wild-type KCNJ10 expression yielded robust Kir current, whereas currents from oocytes expressing the mutation were reduced, remarkably. Western Blot analysis revealed reduced protein expression by the mutation. Kir5.1 subunits display selective heteromultimerization with Kir4.1 constituting channels with unique kinetics. The effect of the mutation on Kir4.1/5.1 channel activity was twofold: a reduction in current amplitudes and an increase in the pH-dependent inhibition. We thus report a novel loss-of-function mutation in Kir4.1 found in a patient with a coexisting mutation in SLACK channels that results in a fatal disease.NEW & NOTEWORTHY We present and characterize a novel mutation in KCNJ10 Unlike previously reported EAST/SeSAME patients, our patient was heterozygous, and contrary to previous studies, mimicking the heterozygous state by coexpression resulted in loss of channel function. We report in the same patient co-occurrence of a KCNT1 mutation resulting in a more severe phenotype. This study provides new insights into the phenotypic spectrum and to the genotype-phenotype correlations associated with EAST/SeSAME and MMFSI.

Keywords: KCNJ10; Kir4.1; genetics; mutation; seizures.

Publication types

Case Reports

MeSH terms

Animals
Developmental Disabilities / genetics*
Developmental Disabilities / pathology
Heterozygote
Humans
Infant
Loss of Function Mutation*
Male
Mutation, Missense*
Nerve Tissue Proteins / genetics*
Nerve Tissue Proteins / metabolism
Potassium Channels / genetics*
Potassium Channels / metabolism
Potassium Channels, Inwardly Rectifying / genetics*
Potassium Channels, Inwardly Rectifying / metabolism
Potassium Channels, Sodium-Activated
Seizures / genetics*
Seizures / pathology
Syndrome
Xenopus

Substances

KCNT1 protein, human
Kcnj10 (channel)
Nerve Tissue Proteins
Potassium Channels
Potassium Channels, Inwardly Rectifying
Potassium Channels, Sodium-Activated