Insights into clinical phenotypes and treatment responses in a Small cohort of Taiwanese patients with SCN1A variants: A Preliminary study.

IF 2.3 4区 医学 Q2 PEDIATRICS
Yu Min Syu, Inn-Chi Lee, Jyh-Feng Lu, Pi-Lien Hung, Syuan-Yu Hong, Ming-Tao Yang, Jao-Shwann Liang
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引用次数: 0

Abstract

Background: SCN1A channelopathy is the most well-known cause for epileptic encephalopathies and contributes to a wide phenotypic spectrum. The variable expressivity is troublesome for the interpretation of clinical significance and prognoses. To investigate the clinical manifestations, medications and outcomes of patients with SCN1A channelopathies, we conducted this observation retrospective study in Taiwan.

Methods: A cohort consisting of 16 patients (5 males and 11 females) from multiple centers with identified SCN1A variants was investigated and phenotypically relevant factors were recorded. The variants were identified using NGS and confirmed by Sanger sequencing. A panel of 90 epileptic-related genes was used to identify SCN1A variants and to evaluate some of the potential SCN1A modifier genes.

Results: The mean age of seizure onset was 10.4 months. Twelve of the sixteen patients (75%) had different degrees of neurocognitive sequela and psychobehavioral comorbidity in our cohort. Cognitive impairment was noted in all ten patients with Dravet syndrome (DS) and in two of the patients with non-DS phenotypes. A lower response rate to medications was also noted in patients with DS. Notably, a medication-specific tendency towards valproic acid (VPA), clobazam (CLB), and levetiracetam (LEV) was observed, revealing the effective pharmacotherapies for SCN1A-related seizures. An asymptomatic carrier with a reported pathogenic SCN1A variant was reviewed along with her monozygotic twin sister with DS. Nine novel SCN1A mutations are herein reported, eight of which being classified as pathogenic.

Conclusion: Our study revealed unfavorable outcomes for patients with SCN1A variants. Some patients with SCN1A channelopathy showed specific responsiveness to the pharmacotherapies previously either recommended or contraindicated for these patients. Our study also expands the genotype and provides valuable prognostic insights in patients with SCN1A channelopathy.

对一小批台湾 SCN1A 变异患者的临床表型和治疗反应的见解:初步研究。
背景:SCN1A 通道病是癫痫性脑病最著名的病因,其表型范围很广。多变的表现形式给临床意义和预后的解释带来了麻烦。为了研究 SCN1A 通道病患者的临床表现、用药和预后,我们在台湾开展了这项观察性回顾研究:方法:我们调查了来自多个中心的 16 例 SCN1A 变异患者(5 男 11 女),并记录了与表型相关的因素。变异通过 NGS 鉴定,并经 Sanger 测序确认。90 个癫痫相关基因被用于鉴定 SCN1A 变异,并评估一些潜在的 SCN1A 修饰基因:结果:癫痫发作的平均年龄为 10.4 个月。在我们的队列中,16 名患者中有 12 人(75%)有不同程度的神经认知后遗症和心理行为合并症。所有十名德雷维综合征(Dravet Syndrome,DS)患者和两名非DS表型患者都出现了认知障碍。我们还发现,DS 患者对药物的反应率较低。值得注意的是,观察到丙戊酸(VPA)、氯巴赞(CLB)和左乙拉西坦(LEV)的药物特异性倾向,揭示了治疗 SCN1A 相关癫痫发作的有效药物疗法。研究人员对一名无症状的携带者及其患有 DS 的单卵双胞胎姐妹进行了回顾性研究,该携带者被报告为 SCN1A 变异致病体。本文报告了九种新型 SCN1A 变异,其中八种被归类为致病性变异:我们的研究显示,SCN1A 变异患者的预后不佳。一些SCN1A通道病变患者对之前推荐或禁用的药物治疗表现出特殊的反应性。我们的研究还扩展了SCN1A通道病变患者的基因型,并为其预后提供了有价值的见解。
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来源期刊
CiteScore
3.10
自引率
0.00%
发文量
170
审稿时长
48 days
期刊介绍: Pediatrics and Neonatology is the official peer-reviewed publication of the Taiwan Pediatric Association and The Society of Neonatology ROC, and is indexed in EMBASE and SCOPUS. Articles on clinical and laboratory research in pediatrics and related fields are eligible for consideration.
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