Drug-Resistant Epilepsy in Tuberous Sclerosis Complex Is Associated With TSC2 Genotype: More Findings From the Preventing Epilepsy Using Vigatrin (PREVeNT) Trial

IF 3.2 3区 医学 Q2 CLINICAL NEUROLOGY
Laura S. Farach MD , Melissa A. Richard PhD , Aynara C. Wulsin MD, PhD , Elizabeth M. Bebin MD , Darcy A. Krueger MD, PhD , Mustafa Sahin MD, PhD , Brenda E. Porter MD, PhD , Tarrant O. McPherson PhD , Jurriaan M. Peters MD, PhD , Sarah O'Kelley PhD , Katherine S. Taub MD , Rajsekar Rajaraman MD , Stephanie C. Randle MD , William M. McClintock MD , Mary Kay Koenig MD , Michael D. Frost MD , Klaus Werner MD, PhD , Danielle A. Nolan MD , Michael Wong MD, PhD , Gary Cutter PhD , Elida Salazar
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引用次数: 0

Abstract

Background

Children with tuberous sclerosis complex (TSC) are at high risk for drug-resistant epilepsy (DRE). The ability to stratify those at highest risk for DRE is important for counseling and prompt, aggressive management, necessary to optimize neurocognitive outcomes. Using the extensively phenotyped PREVeNT cohort, we aimed to characterize whether the TSC genotype was associated with DRE.

Methods

The study group (N = 70) comprised participants with TSC enrolled at age less than or equal to six months with detailed epilepsy and other phenotypic and genotypic data, prospectively collected as part of the PREVeNT trial. Genotype-phenotype correlations of DRE, time to first abnormal electroencephalography, and time to epilepsy onset were compared using Fisher exact test and regression models.

Results

Presence of a TSC2 pathogenic variant was significantly associated with DRE, compared with TSC1 and participants with no pathogenic mutation identified. In fact, all participants with DRE had a TSC2 pathogenic variant. Furthermore, TSC2 variants expected to result in no protein product were associated with higher risk for DRE. Finally, TSC1 pathogenic variants were associated with later-onset epilepsy, on average 21.2 months later than those with other genotypes.

Conclusions

Using a comprehensively phenotyped cohort followed from infancy, this study is the first to delineate genotype-phenotype correlations for epilepsy severity and onset in children with TSC. Patients with TSC2 pathogenic variants, especially TSC2 pathogenic variants predicted to result in lack of TSC2 protein, are at highest risk for DRE, and are likely to have earlier epilepsy onset than those with TSC1. Clinically, these insights can inform counseling, surveillance, and management.

结节性硬化症复合体的耐药性癫痫与 TSC2 基因型有关:PREVeNT 试验的更多发现
背景患有结节性硬化综合征(TSC)的儿童是耐药性癫痫(DRE)的高危人群。对抗药性癫痫高危人群进行分层的能力对于咨询和及时、积极的管理非常重要,而这是优化神经认知结果所必需的。方法研究组(N = 70)由在 PREVeNT 试验中前瞻性收集的年龄小于或等于 6 个月的 TSC 患者组成,他们拥有详细的癫痫及其他表型和基因型数据。结果与TSC1和未发现致病基因突变的参与者相比,TSC2致病基因变异的存在与DRE显著相关。事实上,所有罹患DRE的参与者都有TSC2致病变体。此外,预计不会产生蛋白质产物的 TSC2 变异与 DRE 风险较高有关。最后,TSC1致病变体与晚发性癫痫有关,比其他基因型的患者平均晚21.2个月。结论本研究利用一个从婴儿期就开始跟踪的全面表型队列,首次描述了TSC儿童癫痫严重程度和发病的基因型-表型相关性。TSC2致病变异患者,尤其是TSC2致病变异导致TSC2蛋白缺乏的患者,罹患DRE的风险最高,其癫痫发病时间也可能早于TSC1患者。在临床上,这些见解可以为咨询、监测和管理提供参考。
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来源期刊
Pediatric neurology
Pediatric neurology 医学-临床神经学
CiteScore
4.80
自引率
2.60%
发文量
176
审稿时长
78 days
期刊介绍: Pediatric Neurology publishes timely peer-reviewed clinical and research articles covering all aspects of the developing nervous system. Pediatric Neurology features up-to-the-minute publication of the latest advances in the diagnosis, management, and treatment of pediatric neurologic disorders. The journal''s editor, E. Steve Roach, in conjunction with the team of Associate Editors, heads an internationally recognized editorial board, ensuring the most authoritative and extensive coverage of the field. Among the topics covered are: epilepsy, mitochondrial diseases, congenital malformations, chromosomopathies, peripheral neuropathies, perinatal and childhood stroke, cerebral palsy, as well as other diseases affecting the developing nervous system.
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