Dissecting genetic architecture of rare dystonia: genetic, molecular and clinical insights.

IF 3.5 2区 医学 Q2 GENETICS & HEREDITY
Burcu Atasu, Javier Simón-Sánchez, Hasmet Hanagasi, Basar Bilgic, Ann-Kathrin Hauser, Gamze Guven, Peter Heutink, Thomas Gasser, Ebba Lohmann
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引用次数: 0

Abstract

Background: Dystonia is one of the most common movement disorders. To date, the genetic causes of dystonia in populations of European descent have been extensively studied. However, other populations, particularly those from the Middle East, have not been adequately studied. The purpose of this study is to discover the genetic basis of dystonia in a clinically and genetically well-characterised dystonia cohort from Turkey, which harbours poorly studied populations.

Methods: Exome sequencing analysis was performed in 42 Turkish dystonia families. Using co-expression network (CEN) analysis, identified candidate genes were interrogated for the networks including known dystonia-associated genes and genes further associated with the protein-protein interaction, animal model-based characteristics and clinical findings.

Results: We identified potentially disease-causing variants in the established dystonia genes (PRKRA, SGCE, KMT2B, SLC2A1, GCH1, THAP1, HPCA, TSPOAP1, AOPEP; n=11 families (26%)), in the uncommon forms of dystonia-associated genes (PCCB, CACNA1A, ALDH5A1, PRKN; n=4 families (10%)) and in the candidate genes prioritised based on the pathogenicity of the variants and CEN-based analyses (n=11 families (21%)). The diagnostic yield was found to be 36%. Several pathways and gene ontologies implicated in immune system, transcription, metabolic pathways, endosomal-lysosomal and neurodevelopmental mechanisms were over-represented in our CEN analysis.

Conclusions: Here, using a structured approach, we have characterised a clinically and genetically well-defined dystonia cohort from Turkey, where dystonia has not been widely studied, and provided an uncovered genetic basis, which will facilitate diagnostic dystonia research.

剖析罕见肌张力障碍的遗传结构:遗传、分子和临床见解。
背景:肌张力障碍是最常见的运动障碍之一:肌张力障碍是最常见的运动障碍之一。迄今为止,人们已对欧洲后裔肌张力障碍的遗传原因进行了广泛研究。然而,对其他人群,尤其是中东人群的研究还不够充分。本研究的目的是在研究较少的土耳其肌张力障碍人群中发现肌张力障碍的遗传基础:方法:对 42 个土耳其肌张力障碍家庭进行了外显子组测序分析。方法:对 42 个土耳其肌张力障碍家族进行外显子组测序分析,利用共表达网络(CEN)分析对已确定的候选基因进行网络分析,其中包括已知的肌张力障碍相关基因以及与蛋白质相互作用、动物模型特征和临床发现进一步相关的基因:结果:我们在已确定的肌张力障碍基因(PRKRA、SGCE、KMT2B、SLC2A1、GCH1、THAP1、HPCA、TSPOAP1、AOPEP;11个家庭(26%))、不常见的肌张力障碍相关基因(PCCB、CACNA1A、ALDH5A1、PRKN;4个家庭(10%))以及根据变异的致病性和基于CEN的分析优先考虑的候选基因(11个家庭(21%))。诊断率为 36%。在我们的CEN分析中,与免疫系统、转录、代谢途径、内体-溶酶体和神经发育机制有关的一些通路和基因本体所占比例过高:在此,我们采用结构化方法描述了来自土耳其的临床和遗传学定义明确的肌张力障碍队列的特征,该地区的肌张力障碍尚未得到广泛研究,我们还提供了尚未发现的遗传学基础,这将有助于诊断性肌张力障碍的研究。
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来源期刊
Journal of Medical Genetics
Journal of Medical Genetics 医学-遗传学
CiteScore
7.60
自引率
2.50%
发文量
92
审稿时长
4-8 weeks
期刊介绍: Journal of Medical Genetics is a leading international peer-reviewed journal covering original research in human genetics, including reviews of and opinion on the latest developments. Articles cover the molecular basis of human disease including germline cancer genetics, clinical manifestations of genetic disorders, applications of molecular genetics to medical practice and the systematic evaluation of such applications worldwide.
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