Assessment of a Targeted Gene Panel for Identification of Genes Associated With Movement Disorders

运动障碍 舞蹈病 帕金森病 肌张力障碍 外显子组测序 肌阵挛 医学 小脑共济失调 共济失调 原发性震颤 表型 疾病 遗传学 生物 内科学 精神科 基因
作者
Solveig Montaut,Christine Tranchant,Nathalie Drouot,Gabrielle Rudolf,Claire Guissart,Julien Tarabeux,Tristan Stemmelen,Amandine Velt,Cécile Fourrage,Patrick Nitschké,Bénédicte Gérard,Jean‐Louis Mandel,M. Kœnig,Jamel Chelly,Mathieu Anheim
出处
期刊:JAMA Neurology [American Medical Association]
卷期号:75 (10): 1234-1234 被引量:53
标识
DOI:10.1001/jamaneurol.2018.1478
摘要

Movement disorders are characterized by a marked genotypic and phenotypic heterogeneity, complicating diagnostic work in clinical practice and molecular diagnosis.To develop and evaluate a targeted sequencing approach using a customized panel of genes involved in movement disorders.We selected 127 genes associated with movement disorders to create a customized enrichment in solution capture array. Targeted high-coverage sequencing was applied to DNA samples taken from 378 eligible patients at 1 Luxembourgian, 1 Algerian, and 25 French tertiary movement disorder centers between September 2014 and July 2016. Patients were suspected of having inherited movement disorders because of early onset, family history, and/or complex phenotypes. They were divided in 5 main movement disorder groups: parkinsonism, dystonia, chorea, paroxysmal movement disorder, and myoclonus. To compare approaches, 23 additional patients suspected of having inherited cerebellar ataxia were included, on whom whole-exome sequencing (WES) was done. Data analysis occurred from November 2015 to October 2016.Percentages of individuals with positive diagnosis, variants of unknown significance, and negative cases; mutational frequencies and clinical phenotyping of genes associated with movement disorders.Of the 378 patients (of whom 208 were male [55.0%]), and with a median (range) age at disease onset of 31 (0-84) years, probable pathogenic variants were identified in 83 cases (22.0%): 46 patients with parkinsonism (55% of 83 patients), 21 patients (25.3%) with dystonia, 7 patients (8.4%) with chorea, 7 patients (8.4%) with paroxysmal movement disorders, and 2 patients (2.4%) with myoclonus as the predominant phenotype. Some genes were mutated in several cases in the cohort. Patients with pathogenic variants were significantly younger (median age, 27 years; interquartile range [IQR], 5-36 years]) than the patients without diagnosis (median age, 35 years; IQR, 15-46 years; P = .04). Diagnostic yield was significantly lower in patients with dystonia (21 of 135; 15.6%; P = .03) than in the overall cohort. Unexpected genotype-phenotype correlations in patients with pathogenic variants deviating from the classic phenotype were highlighted, and 49 novel probable pathogenic variants were identified. The WES analysis of the cohort of 23 patients with cerebellar ataxia led to an overall diagnostic yield of 26%, similar to panel analysis but at a cost 6 to 7 times greater.High-coverage sequencing panel for the delineation of genes associated with movement disorders was efficient and provided a cost-effective diagnostic alternative to whole-exome and whole-genome sequencing.

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