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

IF 0.4 4区医学 Q4 GENETICS & HEREDITY

Clinical Dysmorphology Pub Date : 2023-10-01 Epub Date: 2023-05-05 DOI:10.1097/MCD.0000000000000463

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

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引用次数: 0

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.

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KCNK18双等位基因变异是智力残疾和伴有热性惊厥的癫痫的原因的进一步证据。

简介：KCNK18是钾通道亚家族K成员18（MIM*613655），编码TWIK相关脊髓K+通道（TRESK），对维持神经元兴奋性很重要。已知KCNK18中的单等位基因变体会导致常染色体显性偏头痛，无论是否有先兆，对13的易感性（MIM#613656）。最近，据报道，KCNK18的双等位基因错义变体发生在三名来自非血缘家庭的智力残疾、发育迟缓、自闭症谱系障碍（ASD）和癫痫患者身上。方法：在详细的临床评估后，对先证者进行Singleton外显子组测序，以确定与表型一致的致病变异。结果：我们在此报告了一名患有智力残疾、发育迟缓、ASD和癫痫伴热性癫痫的患者，并在KCNK18中发现了一种新的纯合stopgain变体c.499C>T.p.（Arg167Ter）。结论：该报告进一步证实了KCNK18是常染色体隐性遗传性智力残疾、癫痫和ASD的病因。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical Dysmorphology 医学-遗传学

CiteScore

1.20

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： Clinical Dysmorphology publishes succinct case reports on the etiology, clinical delineation, genetic mapping, and molecular embryology of birth defects. This journal covers such topics as multiple congenital anomaly syndromes - with particular emphasis on previously undescribed conditions, rare findings, ethnic differences in existing syndromes, fetal abnormalities, and cytogenetic aberrations that might give clues to the localization of developmental genes. Regular features include original, peer-reviewed articles, conference reports, book and software reviews, abstracts and summaries from the UK Dysmorphology Club, and literature summaries. Submitted articles undergo a preliminary review by the editor. Some articles may be returned to authors wihtout further consideration. Those being considered for publication will undergo further assessment and peer-review by the editors and those invited to do so from a reviewer pool.