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Diagnostic exome sequencing provides a molecular diagnosis for a significant proportion of patients with epilepsy

癫痫 病因学 外显子组测序 疾病 外显子组 医学 癫痫综合征 儿科 内科学 生物信息学 突变 基因 遗传学 精神科 生物
作者
Katherine L. Helbig,Kelly D. Farwell Hagman,Deepali N. Shinde,Cameron Mroske,Zöe Powis,Shuwei Li,Sha Tang,Ingo Helbig
出处
期刊:Genetics in Medicine [Elsevier BV]
卷期号:18 (9): 898-905 被引量:329
标识
DOI:10.1038/gim.2015.186
摘要

PurposeTo assess the yield of diagnostic exome sequencing (DES) and to characterize the molecular findings in characterized and novel disease genes in patients with epilepsy.MethodsIn an unselected sample of 1,131 patients referred for DES, overall results were compared between patients with and without epilepsy. DES results were examined based on age of onset and epilepsy diagnosis.ResultsPositive/likely positive results were identified in 112/293 (38.2%) epilepsy patients compared with 210/732 (28.7%) patients without epilepsy (P = 0.004). The diagnostic yield in characterized disease genes among patients with epilepsy was 33.4% (105/314). KCNQ2, MECP2, FOXG1, IQSEC2, KMT2A, and STXBP1 were most commonly affected by de novo alterations. Patients with epileptic encephalopathies had the highest rate of positive findings (43.4%). A likely positive novel genetic etiology was proposed in 14/200 (7%) patients with epilepsy; this frequency was highest in patients with epileptic encephalopathies (17%). Three genes (COQ4, DNM1, and PURA) were initially reported as likely positive novel disease genes and were subsequently corroborated in independent peer-reviewed publications.ConclusionDES with analysis and interpretation of both characterized and novel genetic etiologies is a useful diagnostic tool in epilepsy, particularly in severe early-onset epilepsy. The reporting on novel genetic etiologies may further increase the diagnostic yield.Genet Med 18 9, 898–905.
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