Krahn M, Pécheux C, Chapon F, Béroud C, Drouin-Garraud V, Laforet P, Romero N B, Penisson-Besnier I, Bernard R, Urtizberea J A, Leturcq F, Lévy N
Département de Génétique Médicale, Hôpital d'enfants de la Timone, Marseille, France.
Clin Genet. 2007 Dec;72(6):582-92. doi: 10.1111/j.1399-0004.2007.00906.x. Epub 2007 Nov 1.
Mutations in the gene encoding calpain-3 (CAPN3) cause autosomal recessive limb-girdle muscular dystrophy type 2A (LGMD2A) and idiopathic eosinophilic myositis. Accurate diagnosis and genetic counselling are based on the identification of disease-causing mutations on both alleles of CAPN3 in the patients. In the present study, we used transcriptional analysis as a complementary approach for patients suspected of being affected with LGMD2A, in whom initial denaturing high-performance liquid chromatography genomic mutation screening evidenced no or only one CAPN3 mutation obviously considered as disease causing. This allowed to identify and characterize cDNA deletions. Further genomic analysis allowed to determine the origin of these deletions, either as splicing defects caused by intronic mutations or as an internal multi-exonic deletion. In particular, we report two novel CAPN3 mutations (c.1745 + 4_1745 + 7delAGTG in IVS13 and c.2185-16A>G in IVS20) and a recurrent large-sized genomic deletion including exons 2-8 for which genomic breakpoints have been characterized. In addition, our results indicate nonsense-mediated messenger RNA decay as a mechanism for under-expression of CAPN3 associated to some specific variations.
编码钙蛋白酶-3(CAPN3)的基因突变会导致常染色体隐性遗传的2A型肢带型肌营养不良症(LGMD2A)和特发性嗜酸性粒细胞性肌炎。准确的诊断和遗传咨询基于对患者CAPN3两个等位基因上致病突变的识别。在本研究中,我们将转录分析作为一种补充方法,用于疑似患有LGMD2A的患者,这些患者最初的变性高效液相色谱基因组突变筛查未发现或仅发现一个明显被视为致病的CAPN3突变。这使得我们能够识别和表征cDNA缺失。进一步的基因组分析使我们能够确定这些缺失的起源,它们要么是由内含子突变引起的剪接缺陷,要么是内部多外显子缺失。特别是,我们报告了两个新的CAPN3突变(IVS13中的c.1745 + 4_1745 + 7delAGTG和IVS20中的c.2185-16A>G)以及一个包括外显子2-8的复发性大基因组缺失,其基因组断点已得到表征。此外,我们的结果表明无义介导的信使RNA衰变是与某些特定变异相关的CAPN3表达不足的一种机制。
