Further evidence of biallelic variants in KCNK18 as a cause of intellectual disability and epilepsy with febrile seizure plus

Purvi Majethia; Rhea Harish; Dhanya Lakshmi Narayanan; B. L. Yatheesha; Suvasini Sharma; Anju Shukla

doi:10.1097/MCD.0000000000000463

Further evidence of biallelic variants in KCNK18 as a cause of intellectual disability and epilepsy with febrile seizure plus

Purvi Majethia, Rhea Harish, Dhanya Lakshmi Narayanan, B. L. Yatheesha, Suvasini Sharma, Anju Shukla^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

1 Citation (Scopus)

Abstract

Introduction KCNK18, a potassium channel subfamily K member 18 (MIM∗613655), encodes for TWIK-related spinal cord K+ channel (TRESK) and is important for maintaining neuronal excitability. Monoallelic variants in KCNK18 are known to cause autosomal dominant migraine, with or without aura, susceptibility to, 13 (MIM#613656). Recently, biallelic missense variants in KCNK18 have been reported in three individuals from a non-consanguineous family with intellectual disability, developmental delay, autism spectrum disorder (ASD), and seizure. Methods Singleton exome sequencing was performed for the proband after detailed clinical evaluation to identify the disease-causing variants in concordance with the phenotype. Results We herein report an individual with intellectual disability, developmental delay, ASD, and epilepsy with febrile seizure plus with a novel homozygous stopgain variant, c.499C>T p.(Arg167Ter) in KCNK18. Conclusion This report further validates KCNK18 as a cause of autosomal recessive intellectual disability, epilepsy, and ASD.

Original language	English
Pages (from-to)	147-150
Number of pages	4
Journal	Clinical Dysmorphology
Volume	32
Issue number	4
DOIs	https://doi.org/10.1097/MCD.0000000000000463
Publication status	Published - 01-10-2023

All Science Journal Classification (ASJC) codes

Pediatrics, Perinatology, and Child Health
Anatomy
Pathology and Forensic Medicine
Genetics(clinical)

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title = "Further evidence of biallelic variants in KCNK18 as a cause of intellectual disability and epilepsy with febrile seizure plus",

abstract = "Introduction KCNK18, a potassium channel subfamily K member 18 (MIM∗613655), encodes for TWIK-related spinal cord K+ channel (TRESK) and is important for maintaining neuronal excitability. Monoallelic variants in KCNK18 are known to cause autosomal dominant migraine, with or without aura, susceptibility to, 13 (MIM\#613656). Recently, biallelic missense variants in KCNK18 have been reported in three individuals from a non-consanguineous family with intellectual disability, developmental delay, autism spectrum disorder (ASD), and seizure. Methods Singleton exome sequencing was performed for the proband after detailed clinical evaluation to identify the disease-causing variants in concordance with the phenotype. Results We herein report an individual with intellectual disability, developmental delay, ASD, and epilepsy with febrile seizure plus with a novel homozygous stopgain variant, c.499C>T p.(Arg167Ter) in KCNK18. Conclusion This report further validates KCNK18 as a cause of autosomal recessive intellectual disability, epilepsy, and ASD.",

author = "Purvi Majethia and Rhea Harish and Narayanan, \{Dhanya Lakshmi\} and Yatheesha, \{B. L.\} and Suvasini Sharma and Anju Shukla",

note = "Funding Information: We thank the patient and his family for participating in the study. We also thank the National Institutes of Health, USA, for funding the project titled {\textquoteleft}Genetic Diagnosis of Neurodevelopmental Disorders in India{\textquoteright} (1R01HD093570-01A1). The data can be shared upon a reasonable request to the corresponding author. Publisher Copyright: {\textcopyright} 2023 Lippincott Williams and Wilkins. All rights reserved.",

year = "2023",

month = oct,

day = "1",

doi = "10.1097/MCD.0000000000000463",

language = "English",

volume = "32",

pages = "147--150",

journal = "Clinical Dysmorphology",

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T1 - Further evidence of biallelic variants in KCNK18 as a cause of intellectual disability and epilepsy with febrile seizure plus

AU - Majethia, Purvi

AU - Harish, Rhea

AU - Narayanan, Dhanya Lakshmi

AU - Yatheesha, B. L.

AU - Sharma, Suvasini

AU - Shukla, Anju

N1 - Funding Information: We thank the patient and his family for participating in the study. We also thank the National Institutes of Health, USA, for funding the project titled ‘Genetic Diagnosis of Neurodevelopmental Disorders in India’ (1R01HD093570-01A1). The data can be shared upon a reasonable request to the corresponding author. Publisher Copyright: © 2023 Lippincott Williams and Wilkins. All rights reserved.

PY - 2023/10/1

Y1 - 2023/10/1

N2 - Introduction KCNK18, a potassium channel subfamily K member 18 (MIM∗613655), encodes for TWIK-related spinal cord K+ channel (TRESK) and is important for maintaining neuronal excitability. Monoallelic variants in KCNK18 are known to cause autosomal dominant migraine, with or without aura, susceptibility to, 13 (MIM#613656). Recently, biallelic missense variants in KCNK18 have been reported in three individuals from a non-consanguineous family with intellectual disability, developmental delay, autism spectrum disorder (ASD), and seizure. Methods Singleton exome sequencing was performed for the proband after detailed clinical evaluation to identify the disease-causing variants in concordance with the phenotype. Results We herein report an individual with intellectual disability, developmental delay, ASD, and epilepsy with febrile seizure plus with a novel homozygous stopgain variant, c.499C>T p.(Arg167Ter) in KCNK18. Conclusion This report further validates KCNK18 as a cause of autosomal recessive intellectual disability, epilepsy, and ASD.

AB - Introduction KCNK18, a potassium channel subfamily K member 18 (MIM∗613655), encodes for TWIK-related spinal cord K+ channel (TRESK) and is important for maintaining neuronal excitability. Monoallelic variants in KCNK18 are known to cause autosomal dominant migraine, with or without aura, susceptibility to, 13 (MIM#613656). Recently, biallelic missense variants in KCNK18 have been reported in three individuals from a non-consanguineous family with intellectual disability, developmental delay, autism spectrum disorder (ASD), and seizure. Methods Singleton exome sequencing was performed for the proband after detailed clinical evaluation to identify the disease-causing variants in concordance with the phenotype. Results We herein report an individual with intellectual disability, developmental delay, ASD, and epilepsy with febrile seizure plus with a novel homozygous stopgain variant, c.499C>T p.(Arg167Ter) in KCNK18. Conclusion This report further validates KCNK18 as a cause of autosomal recessive intellectual disability, epilepsy, and ASD.

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Further evidence of biallelic variants in KCNK18 as a cause of intellectual disability and epilepsy with febrile seizure plus

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