Developmental and Epileptic Encephalopathy 76: Case Report and Review of Literature

复合杂合度 表型 癫痫 遗传学 生酮饮食 全球发育迟缓 智力残疾 基因型-表型区分 基因 生物 医学 神经科学
作者
Xiaodi Han,Jie Deng,Chunhong Chen,Xiaohui Wang,Fang Fang,Hua Li,Jie Luo,Jie Wu
出处
期刊:Children (Basel) [Multidisciplinary Digital Publishing Institute]
卷期号:9 (12): 1967-1967
标识
DOI:10.3390/children9121967
摘要

Previous studies have suggested that the ACTL6B monoallelic variant is responsible for an autosomal dominant inherited intellectual developmental disorder with severe speech and ambulation deficits. The clinical phenotype of developmental and epileptic encephalopathy type 76 (DEE76) due to ACTL6B biallelic variants was first reported in 2019, with an autosomal recessive mode of inheritance. In this paper, we report on a child in China with DEE76 caused by a compound heterozygous variant of the ACTL6B gene, and we review the literature on ACTL6B gene variants causing DEE76 with complete clinical information. Including our case 1, the genotype and phenotypic characteristics of 18 children from 14 families are summarized. All 18 cases are autosomal recessive, including 12 with homozygous variants and six with compound heterozygous variants. A total of 17 variants have been reported so far, including 14 variants of the loss function. We summarize the clinical features using Human Phenotype Ontology (HPO) terms. We find that DEE76, caused by the ACTL6B biallelic variant, is an early-onset drug-refractory epilepsy with global developmental delayHP:0001263, hypertoniaHP:0001276, and microcephalyHP:0000252, and imaging is characterized by brain delayed myelinationHP:0012448. Our case of DEE76 had not been reported when the patient underwent genetic testing in 2018, and the diagnosis was clarified by the reanalysis of the data 2 years later, being the first reported Chinese patient and the only one in which the application of a ketogenic diet for antiepileptic treatment may have been effective.
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