Urtasun M, Sáenz A, Roudaut C, Poza J J, Urtizberea J A, Cobo A M, Richard I, García Bragado F, Leturcq F, Kaplan J C, Martí Massó J F, Beckmann J S, López de Munain A
Department of Neurology, Hospital Ntra. Sra. Aránzazu, San Sebastián, Basque Country, Spain.
Brain. 1998 Sep;121 ( Pt 9):1735-47. doi: 10.1093/brain/121.9.1735.
The concept of limb-girdle muscular dystrophy (LGMD) is changing rapidly due to the advances in molecular genetics. Recently, seven different gene loci have been described, demonstrating that limb-girdle muscular dystrophy is a heterogeneous syndrome, which includes different diseases with a similar phenotype. In isolated populations which have little genetic exchange with neighbouring populations, an accumulation of cases may be found. We carried out an epidemiological study in Guipúzcoa, a small mountainous Basque province in northern Spain, and found the highest prevalence rate of LGMD described so far: 69 per million. Genetic studies demonstrated that 38 cases corresponded to the LGMD2A type, due to calpain-3 gene mutations. Only one patient with alpha-sarcoglycanopathy was found, and in 12 patients the genetic defect was not identified. Moreover, the particular calpain-3 mutation predominant in Basque chromosomes (exon 22, 2362AG-->TCATCT), has only been rarely found in the rest of the world. This observation strongly suggests a founder effect in the indigenous population of Guipúzcoa. The clinical characteristics of the patients with calpain-3 gene mutations were quite homogeneous and different from the other groups (sarcoglycanopathy and unknown gene defect), allowing for a precise clinical diagnostic. The disease onset was between the ages of 8 and 15 years, in most cases in the pelvic girdle, and the patients became wheelchair-bound between 11 and 28 years after onset. No pseudohypertrophy of calves or contractures were observed. No clear correlations were found between the nature and site of the mutation and the resulting phenotype.
由于分子遗传学的进展,肢带型肌营养不良(LGMD)的概念正在迅速变化。最近,已经描述了七个不同的基因位点,这表明肢带型肌营养不良是一种异质性综合征,其中包括具有相似表型的不同疾病。在与邻近人群几乎没有基因交流的孤立人群中,可能会发现病例的聚集。我们在西班牙北部一个多山的小巴斯克省吉普斯夸进行了一项流行病学研究,发现了迄今为止所描述的LGMD的最高患病率:每百万人口中有69例。基因研究表明,38例病例对应于LGMD2A型,是由钙蛋白酶-3基因突变引起的。仅发现一名α-肌聚糖病患者,在12名患者中未鉴定出基因缺陷。此外,在巴斯克染色体中占主导地位的特定钙蛋白酶-3突变(外显子22,2362AG→TCATCT)在世界其他地区很少见。这一观察结果强烈表明在吉普斯夸的原住民中存在奠基者效应。钙蛋白酶-3基因突变患者的临床特征相当一致,并且与其他组(肌聚糖病和未知基因缺陷)不同,从而实现了精确的临床诊断。疾病发病年龄在8至15岁之间,大多数情况下累及骨盆带,患者在发病后11至28年之间需要依靠轮椅行动。未观察到小腿假肥大或挛缩。在突变的性质和位点与所产生的表型之间未发现明确的相关性。
