Atlastin1突变在早发型常染色体显性遗传性痉挛性截瘫中很常见。

Atlastin1 mutations are frequent in young-onset autosomal dominant spastic paraplegia.

作者信息

Dürr Alexandra, Camuzat Agnès, Colin Emilie, Tallaksen Chantal, Hannequin Didier, Coutinho Paula, Fontaine Bertrand, Rossi Annick, Gil Roger, Rousselle Christophe, Ruberg Merle, Stevanin Giovanni, Brice Alexis

机构信息

Département de Génétique, Cytogénétique et Embryologie, and INSERM U289, Hôpital Salpêtrière AP-HP, Paris, France.

出版信息

Arch Neurol. 2004 Dec;61(12):1867-72. doi: 10.1001/archneur.61.12.1867.

DOI:10.1001/archneur.61.12.1867

PMID:15596607

Abstract

BACKGROUND

Hereditary spastic paraplegias are disorders that are very heterogeneous, both clinically and genetically. The atlastin1 gene has recently been implicated in SPG3A, a form of autosomal dominant pure spastic paraplegia. Atlastin1 mutations have been identified in 8 families so far.

OBJECTIVES

To determine the relative frequency, phenotype, and mutation spectrum of SPG3A in patients with pure autosomal dominant spastic paraplegia and onset before age 20 years.

PATIENTS AND METHODS

We sequenced the atlastin1 gene in a large series of patients (31 families) in which mutations in the spastin gene, corresponding to the frequent SPG4 locus, had previously been excluded. The phenotype was compared with 126 SPG4 patients.

RESULTS

We identified 12 families (39%) including 34 patients with 9 different missense atlastin1 mutations, 7 of which are newly described. The main clinical characteristic of these SPG3A patients was pure spasticity with very young onset of symptoms (mean age, 4.6 +/- 3.9 years) and slow progression. However, additional signs such as decreased vibration sense and wasting in lower limbs, sphincter disturbances, and scoliosis were found in a minority of patients. In addition, several gene carriers were clinically affected but still asymptomatic (n = 5) or had no clinical signs (n = 2), indicating incomplete penetrance. Compared with patients from other families meeting the same diagnostic criteria (43 patients) and families with SPG4 (126 patients), the major form of autosomal dominant spastic paraplegia, SPG3A patients had earlier symptom onset, less frequently increased reflexes in the upper limbs, decreased vibration sense in the lower limbs, and fewer sphincter disturbances, but more frequently observed wasting in the lower limbs and scoliosis. These particularities, as well as frequent abnormal motor evoked potentials, could help identify patients to be screened for atlastin1 gene mutations.

CONCLUSIONS

This study enables us to estimate the frequency of the SPG3A mutations in France at 39% in families with young-onset autosomal dominant spastic paraplegia after exclusion of SPG4 cases. So far, most mutations have been private, although they were all found in exons 7, 8, 12, and 13. These exons should be given priority when performing molecular diagnoses for SPG3A.

摘要

背景

遗传性痉挛性截瘫是一类在临床和遗传方面都具有高度异质性的疾病。atlastin1基因最近被认为与SPG3A相关，SPG3A是常染色体显性遗传性单纯痉挛性截瘫的一种类型。目前已在8个家系中发现了atlastin1基因突变。

目的

确定在20岁前发病的常染色体显性遗传性单纯痉挛性截瘫患者中SPG3A的相对频率、表型及突变谱。

患者和方法

我们对大量患者（31个家系）的atlastin1基因进行了测序，这些家系之前已排除与常见SPG4位点相对应的痉挛蛋白基因突变。将这些患者的表型与126例SPG4患者进行了比较。

结果

我们鉴定出12个家系（39%），包括34例患者，存在9种不同的atlastin1错义突变，其中7种是新发现的。这些SPG3A患者的主要临床特征为单纯性痉挛，症状出现年龄非常小（平均年龄4.6±3.9岁）且进展缓慢。然而，少数患者还出现了其他体征，如下肢振动觉减退、肌肉萎缩、括约肌功能障碍和脊柱侧弯。此外，有几个基因携带者临床上有症状但仍无症状（n = 5）或无临床体征（n = 2），提示存在不完全外显。与其他符合相同诊断标准的家系患者（43例）以及SPG4家系患者（126例）相比，常染色体显性遗传性痉挛性截瘫的主要类型SPG3A患者症状出现更早，上肢反射亢进较少见，下肢振动觉减退，括约肌功能障碍较少，但下肢肌肉萎缩和脊柱侧弯更为常见。这些特点以及频繁出现的异常运动诱发电位有助于识别需要进行atlastin1基因突变筛查的患者。