Previously defined variants of uncertain significance may play an important role in epilepsy and interactions between certain variants may become pathogenic

IF 2.8 3区医学 Q2 CLINICAL NEUROLOGY Epilepsia Open Pub Date : 2024-11-07 DOI:10.1002/epi4.13085

Yara Hussein, Hila Weisblum-Neuman, Bruria Ben Zeev, Shani Stern

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Abstract

Objective

Epilepsy is a chronic neurological disorder related to various etiologies, and the prevalence of active epilepsy is estimated to be between 4 and 10 per 1000 individuals having a significant role in genetic mutations. Next-Generation Sequencing (NGS) panels are utilized for genetic testing, but a substantial proportion of the results remain uncertain and are not considered directly causative of epilepsy. This study aimed to reevaluate pediatric patients diagnosed with epilepsy who underwent genetic investigation using NGS panels, focusing on inconclusive variant findings or multiple variants of uncertain significance (VUSs).

Methods

A subgroup of pediatric patients aged 0–25 years, diagnosed with epilepsy, who underwent genetic investigation with an NGS epilepsy panel at the Child Neurology Unit, The Edmond and Lily Safra Children's Hospital, Sheba Medical Center, between 2018 and 2022 through Invitae, was reevaluated. Patients with inconclusive variant findings or multiple VUSs in their test results were included. Genetic data were analyzed to identify potentially pathogenic variants and frequent genetic combinations.

Results

Two unrelated potentially pathogenic variants were identified in the SCN9A and QARS1 genes. A frequent genetic combination, RANBP2&RYR3, was also observed among other combinations. The RANBP2 gene consistently co-occurred with RYR3 variants in uncertain results, suggesting potential pathogenicity. Analysis of unaffected parents' data revealed certain combinations inherited from different parents, suggesting specific gene combinations as possible risk factors for the disease.

Significance

This study highlights the importance of reevaluating genetic data from pediatric epilepsy patients with inconclusive variant findings or multiple VUSs. Identification of potentially pathogenic variants and frequent genetic combinations, such as RANBP2&RYR3, could aid in understanding the genetic basis of epilepsy and identifying potential hotspots.

Plain Language Summary

We have performed a retrospective analysis on a subpopulation of pediatric patients diagnosed with epilepsy. We found that specific genetic variants were repeatable, indicating their potential pathogenicity to the disease.

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以前定义的意义不明的变异体可能在癫痫中发挥重要作用，某些变异体之间的相互作用可能成为致病因素。

目的：癫痫是一种与各种病因有关的慢性神经系统疾病，活动性癫痫的发病率估计为每 1000 人中有 4 到 10 人，这与基因突变有很大关系。下一代测序（NGS）面板可用于基因检测，但相当一部分结果仍不确定，不被认为是癫痫的直接致病因素。本研究旨在重新评估使用 NGS 面板进行基因检测的被诊断为癫痫的儿科患者，重点关注不确定的变异结果或多个意义不确定的变异（VUS）：对2018年至2022年期间通过Invitae公司在谢巴医疗中心埃德蒙和莉莉-萨夫拉儿童医院儿童神经科接受NGS癫痫面板遗传学调查的0-25岁确诊为癫痫的儿科患者亚组进行了重新评估。检测结果中存在不确定变异结果或多个 VUS 的患者被纳入其中。对基因数据进行了分析，以确定潜在致病变体和常见基因组合：结果：在 SCN9A 和 QARS1 基因中发现了两个不相关的潜在致病变异。在其他基因组合中还发现了一种常见的基因组合，即 RANBP2&RYR3 组合。在不确定的结果中，RANBP2 基因始终与 RYR3 变体同时出现，这表明了潜在的致病性。对未受影响的父母数据进行分析后发现，某些基因组合遗传自不同的父母，这表明特定的基因组合可能是该疾病的风险因素：本研究强调了对变异结果不确定或存在多个 VUS 的小儿癫痫患者的遗传数据进行重新评估的重要性。识别潜在的致病变异和频繁的基因组合（如 RANBP2&RYR3 ）有助于了解癫痫的遗传基础并识别潜在的热点。原文摘要：我们对诊断为癫痫的亚群儿科患者进行了回顾性分析。我们发现特定的遗传变异具有重复性，这表明它们对该疾病具有潜在的致病性。

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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