THAP1（DYT6）基因突变与伴有明显痉挛性发音障碍的全身性肌张力障碍：一项基因筛查研究。

Mutations in THAP1 (DYT6) and generalised dystonia with prominent spasmodic dysphonia: a genetic screening study.

作者信息

Djarmati Ana, Schneider Susanne A, Lohmann Katja, Winkler Susen, Pawlack Heike, Hagenah Johann, Brüggemann Norbert, Zittel Simone, Fuchs Tania, Raković Aleksandar, Schmidt Alexander, Jabusch Hans-Christian, Wilcox Robert, Kostić Vladimir S, Siebner Hartwig, Altenmüller Eckart, Münchau Alexander, Ozelius Laurie J, Klein Christine

机构信息

Schilling Department of Clinical and Molecular Neurogenetics, University of Lübeck, Lübeck, Germany.

出版信息

Lancet Neurol. 2009 May;8(5):447-52. doi: 10.1016/S1474-4422(09)70083-3. Epub 2009 Apr 1.

DOI:10.1016/S1474-4422(09)70083-3

PMID:19345148

Abstract

BACKGROUND

DYT6 is a primary, early-onset torsion dystonia; however, unlike in DYT1 dystonia, the symptoms of DYT6 dystonia frequently involve the craniocervical region. Recently, two mutations in THAP1, the gene that encodes THAP (thanatos-associated protein) domain-containing apoptosis-associated protein 1 (THAP1), have been identified as a cause of DYT6 dystonia.

METHODS

We screened THAP1 by sequence analysis and quantitative real-time polymerase chain reaction (PCR) in 160 white patients of European ancestry who had dystonia with an early age at onset (n=64), generalised dystonia (n=35), a positive family history of dystonia (n=56), or facial or laryngeal dystonia. Another 160 patients with dystonia were screened for reported and novel variants in THAP1. 280 neurologically healthy controls were screened for the newly identified and previously reported changes in THAP1 and these and an additional 75 controls were screened for a rare non-coding mutation.

FINDINGS

We identified two mutations in THAP1 (388_389delTC and 474delA), respectively, in two (1%) German patients from the 160 patients with dystonia. Both mutation carriers had laryngeal dystonia that started in childhood and both went on to develop generalised dystonia. Thus, two of three patients with early-onset generalised dystonia with orobulbar involvement had mutations in THAP1. One of the identified patients with DYT6 dystonia had two family members with subtle motor signs who also carried the same mutation. A rare substitution in the 5'untranslated region (-236_235GA-->TT) was found in 20 of 320 patients and in seven of 355 controls (p=0.0054).

INTERPRETATION

Although mutations in THAP1 might have only a minor role in patients with different, but mainly focal, forms of dystonia, they do seem to be associated with early-onset generalised dystonia with spasmodic dysphonia. This combination of symptoms might be a characteristic feature of DYT6 dystonia and could be useful in the differential diagnosis of DYT1, DYT4, DYT12, and DYT17 dystonia. In addition to the identified mutations, a rare non-coding substitution in THAP1 might increase the risk of dystonia.

FUNDING

Deutsche Forschungsgemeinschaft; Volkswagen Foundation; Dystonia Medical Research Foundation; University of Lübeck.

摘要

背景

DYT6是一种原发性早发性扭转性肌张力障碍；然而，与DYT1肌张力障碍不同，DYT6肌张力障碍的症状常累及颅颈区域。最近，已确定编码含THAP（与死亡相关蛋白）结构域的凋亡相关蛋白1（THAP1）的基因THAP1中的两个突变是DYT6肌张力障碍的病因。

方法

我们对160名具有欧洲血统的白种肌张力障碍患者进行了序列分析和定量实时聚合酶链反应（PCR）筛查THAP1，这些患者有早发肌张力障碍（n = 64）、全身性肌张力障碍（n = 35）、肌张力障碍家族史阳性（n = 56）或面部或喉部肌张力障碍。另外160名肌张力障碍患者被筛查THAP1中的已报道和新的变异。对280名神经学上健康的对照者筛查THAP1中新发现的和先前报道的变化，并且对这些对照者以及另外75名对照者筛查一种罕见的非编码突变。

结果

在160名肌张力障碍患者中的两名（1%）德国患者中，我们分别在THAP1中鉴定出两个突变（388_389delTC和474delA）。两名突变携带者均有始于儿童期的喉部肌张力障碍，并且均继而发展为全身性肌张力障碍。因此，三名有口咽受累的早发性全身性肌张力障碍患者中有两名在THAP1中有突变。一名已鉴定的DYT6肌张力障碍患者有两名有轻微运动体征的家庭成员，他们也携带相同的突变。在320名患者中的20名以及355名对照者中的7名中发现了5'非翻译区的一种罕见替代（-236_235GA-->TT）（p = 0.0054）。

解读

尽管THAP1中的突变在不同但主要为局灶性的肌张力障碍形式的患者中可能仅起次要作用，但它们似乎确实与伴有痉挛性发音障碍的早发性全身性肌张力障碍相关。这种症状组合可能是DYT6肌张力障碍的一个特征性表现，并且可能有助于DYT1、DYT4、DYT12和DYT17肌张力障碍的鉴别诊断。除了已鉴定的突变外，THAP1中的一种罕见非编码替代可能会增加肌张力障碍的风险。