Association between phenotypes and genotype of developmental and epileptic encephalopathy in next-generation sequencing methods in infants: A scoping review.

Q3 Medicine

Medical Journal of Malaysia Pub Date : 2025-07-01

A Triono, E S Herini, K H Mooiindie, K Iskandar, Gunadi

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引用次数: 0

Abstract

Introduction: Developmental and epileptic encephalopathy (DEE) is epilepsy related to developmental impairment that may be caused by both the underlying etiology (developmental encephalopathy) and superimposed epileptic activity (epileptic encephalopathy). The origin of DEE and the causes of its variations remain unknown. Owing the lack of clarity regarding the role of genetic variables in DEE, we conducted a scoping review to qualitatively identify the genes most important in the development of DEE to provide an up-to-date review.

Material and methods: We searched all published studies related to the genetic factors of DEE. The identified publications were screened and selected by the authors on basis of on inclusion and exclusion criteria and assessed for methodological quality. Eighteen articles were included. The extracted data included age of onset, sex, gene mutations and inheritance (e.g. nucleotide change, protein change, and family testing), clinical manifestation, electroencephalogram, imaging, medication, and outcomes.

Result: A total of 18 studies were included in this scoping review. The most frequently reported gene variants were STXBP1 in Ohtahara Syndrome, SLC1A2 in Early Myoclonic Encephalopathy (EME), CDKL5 in West Syndrome, SCN1A in Dravet Syndrome, and KCNT1 in Epilepsy of Infancy with Migrating Focal Seizures (EIMFS). Each gene was associated with distinct electroclinical features, including differences in age of onset, seizure type, EEG patterns, and developmental outcomes. While genotype and phenotype associations were heterogeneous, certain variants showed consistent patterns indicative of more severe disease courses.

Conclusions: This review identified key gene variants commonly associated with early-onset DEE in infants, particularly STXBP1, SLC1A2, CDKL5, SCN1A, and KCNT1, each linked to unique clinical presentations and outcomes. These findings support the clinical utility of next-generation sequencing (NGS) for early diagnosis and tailored treatment planning in DEE. Understanding genotype-phenotype correlations may enhance prognostication and highlight potential avenues for targeted therapy in future research.

本刊更多论文

下一代婴儿测序方法中发育性和癫痫性脑病的表型和基因型之间的关联：一项范围综述。

发展性和癫痫性脑病（DEE）是一种与发育障碍相关的癫痫，可能是由潜在的病因（发展性脑病）和叠加的癫痫活动（癫痫性脑病）引起的。DEE的起源及其变异的原因尚不清楚。由于遗传变量在DEE中的作用尚不明确，我们进行了一项范围综述，以定性地确定在DEE发展中最重要的基因，以提供最新的综述。材料和方法：我们检索了所有已发表的与DEE遗传因素相关的研究。作者根据纳入和排除标准对确定的出版物进行筛选和选择，并对方法学质量进行评估。共纳入18篇文章。提取的数据包括发病年龄、性别、基因突变和遗传（如核苷酸变化、蛋白变化和家族检测）、临床表现、脑电图、影像学、用药和转归。结果：本综述共纳入18项研究。最常见的基因变异是大田原综合征的STXBP1、早期肌阵挛性脑病（EME）的SLC1A2、West综合征的CDKL5、Dravet综合征的SCN1A和婴儿期癫痫伴迁移局灶性发作（EIMFS）的KCNT1。每个基因都与不同的电临床特征相关，包括发病年龄、癫痫类型、脑电图模式和发育结果的差异。虽然基因型和表型关联是异质的，但某些变异显示出一致的模式，表明更严重的疾病过程。结论：本综述确定了与婴儿早发性DEE相关的关键基因变异，特别是STXBP1、SLC1A2、CDKL5、SCN1A和KCNT1，每一个都与独特的临床表现和结果相关。这些发现支持了下一代测序（NGS）在DEE早期诊断和量身定制治疗计划中的临床应用。了解基因型-表型相关性可以增强预后，并在未来的研究中突出靶向治疗的潜在途径。

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

Medical Journal of Malaysia Medicine-Medicine (all)

CiteScore

1.20

自引率

0.00%

发文量

165

期刊介绍： Published since 1890 this journal originated as the Journal of the Straits Medical Association. With the formation of the Malaysian Medical Association (MMA), the Journal became the official organ, supervised by an editorial board. Some of the early Hon. Editors were Mr. H.M. McGladdery (1960 - 1964), Dr. A.A. Sandosham (1965 - 1977), Prof. Paul C.Y. Chen (1977 - 1987). It is a scientific journal, published quarterly and can be found in medical libraries in many parts of the world. The Journal also enjoys the status of being listed in the Index Medicus, the internationally accepted reference index of medical journals. The editorial columns often reflect the Association''s views and attitudes towards medical problems in the country. The MJM aims to be a peer reviewed scientific journal of the highest quality. We want to ensure that whatever data is published is true and any opinion expressed important to medical science. We believe being Malaysian is our unique niche; our priority will be for scientific knowledge about diseases found in Malaysia and for the practice of medicine in Malaysia. The MJM will archive knowledge about the changing pattern of human diseases and our endeavours to overcome them. It will also document how medicine develops as a profession in the nation. We will communicate and co-operate with other scientific journals in Malaysia. We seek articles that are of educational value to doctors. We will consider all unsolicited articles submitted to the journal and will commission distinguished Malaysians to write relevant review articles. We want to help doctors make better decisions and be good at judging the value of scientific data. We want to help doctors write better, to be articulate and precise.