对大量成年癫痫患者进行多基因检测:诊断率及具有临床可操作性的基因发现
Multigene Panel Testing in a Large Cohort of Adults With Epilepsy: Diagnostic Yield and Clinically Actionable Genetic Findings.
作者信息
McKnight Dianalee, Bristow Sara L, Truty Rebecca M, Morales Ana, Stetler Molly, Westbrook M Jody, Robinson Kristina, Riethmaier Darlene, Borlot Felippe, Kellogg Marissa, Hwang Sean T, Berg Anne, Aradhya Swaroop
机构信息
Invitae (D.M., S.L.B., R.M.T., A.M., M.S., M.J.W., K.R., D.R., S.A.), San Francisco, CA; Alberta Children's Hospital Research Institute, Cumming School of Medicine, (F.B.) University of Calgary, Canada; Oregon Health & Science University Comprehensive Epilepsy Center (M.K.); Department of Neurology, Donald and Barbara Zucker School of Medicine at Hofstra/Northwell (S.T.H); Epilepsy Center, Ann & Robert H. Lurie Children's Hospital of Chicago (A.B.); and Department of Neurology, Northwestern University-Feinberg School of Medicine (A.B.), Chicago, IL.
出版信息
Neurol Genet. 2021 Dec 16;8(1):e650. doi: 10.1212/NXG.0000000000000650. eCollection 2022 Feb.
BACKGROUND AND OBJECTIVES
Although genetic testing among children with epilepsy has demonstrated clinical utility and become a part of routine testing, studies in adults are limited. This study reports the diagnostic yield of genetic testing in adults with epilepsy.
METHODS
Unrelated individuals aged 18 years and older who underwent diagnostic genetic testing for epilepsy using a comprehensive, next-generation sequencing-based, targeted gene panel (range 89-189 genes) were included in this cross-sectional study. Clinical information, provided at the discretion of the ordering clinician, was reviewed and analyzed. Diagnostic yield was calculated for all individuals including by age at seizure onset and comorbidities based on clinician-reported information. The proportion of individuals with clinically actionable genetic findings, including instances when a specific treatment would be indicated or contraindicated due to a diagnostic finding, was calculated.
RESULTS
Among 2,008 individuals, a diagnostic finding was returned for 218 adults (10.9%), with clinically actionable findings in 55.5% of diagnoses. The highest diagnostic yield was in adults with seizure onset during infancy (29.6%, 0-1 year), followed by in early childhood (13.6%, 2-4 years), late childhood (7.0%, 5-10 years), adolescence (2.4%, 11-17 years), and adulthood (3.7%, ≥18 years). Comorbid intellectual disability (ID) or developmental delay resulted in a high diagnostic yield (16.0%), most notably for females (19.6% in females vs 12.3% in males). Among individuals with pharmacoresistant epilepsy, 13.5% had a diagnostic finding, and of these, 57.4% were clinically actionable genetic findings.
DISCUSSION
These data reinforce the utility of genetic testing for adults with epilepsy, particularly for those with childhood-onset seizures, ID, and pharmacoresistance. This is an important consideration due to longer survival and the complexity of the transition from pediatric to adult care. In addition, more than half of diagnostic findings in this study were considered clinically actionable, suggesting that genetic testing could have a direct impact on clinical management and outcomes.
背景与目的
尽管对癫痫患儿进行基因检测已显示出临床实用性并成为常规检测的一部分,但针对成人的研究有限。本研究报告了成人癫痫基因检测的诊断率。
方法
本横断面研究纳入了年龄在18岁及以上、使用基于新一代测序的综合性靶向基因panel(包含89 - 189个基因)进行癫痫诊断性基因检测的无关个体。对由开单临床医生酌情提供的临床信息进行回顾和分析。根据临床医生报告的信息,计算所有个体的诊断率,包括按癫痫发作起始年龄和合并症进行计算。计算具有临床可操作基因发现的个体比例,包括因诊断发现而需进行特定治疗或禁忌特定治疗的情况。
结果
在2008名个体中,218名成人(10.9%)获得了诊断结果,其中55.5%的诊断具有临床可操作结果。诊断率最高的是婴儿期(29.6%,0 - 1岁)癫痫发作的成人,其次是幼儿期(13.6%,2 - 4岁)、儿童晚期(7.0%,5 - 10岁)、青春期(2.4%,11 - 17岁)和成年期(3.7%,≥18岁)。合并智力残疾(ID)或发育迟缓导致诊断率较高(16.0%),女性尤为明显(女性为19.6%,男性为12.3%)。在药物难治性癫痫个体中,13.5%有诊断结果,其中57.4%是临床可操作的基因发现。
讨论
这些数据强化了对成人癫痫进行基因检测的实用性,特别是对于那些有儿童期发作、ID和药物难治性的患者。鉴于成人存活时间更长以及从儿科护理向成人护理过渡的复杂性,这是一个重要的考虑因素。此外,本研究中超过一半的诊断结果被认为具有临床可操作性,这表明基因检测可能会对临床管理和结果产生直接影响。
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