Human Genome and Stem Cell Research Center, University of São Paulo, São Paulo, Brazil.
Depart of Pediatrics, Medical School of Federal University of Minas Gerais, Belo Horizonte, MG, Brazil.
Acta Myol. 2020 Dec 1;39(4):274-282. doi: 10.36185/2532-1900-030. eCollection 2020 Dec.
Central Core Disease (CCD) is an inherited neuromuscular disorder characterized by the presence of cores in muscle biopsy. CCD is caused by mutations in the RYR1 gene. This gene encodes the ryanodine receptor 1, which is an intracellular calcium release channel from the sarcoplasmic reticulum to the cytosol in response to depolarization of the plasma membrane. Mutations in this gene are also associated with susceptibility to Malignant Hyperthermia (MHS). In this study, we evaluated 20 families with clinical and histological characteristics of CCD to identify primary mutations in patients, for diagnosis and genetic counseling of the families. We identified variants in the RYR1 gene in 19/20 families. The molecular pathogenicity was confirmed in 16 of them. Most of these variants (22/23) are missense and unique in the families. Two variants were recurrent in two different families. We identified six families with biallelic mutations, five compound heterozygotes with no consanguinity, and one homozygous, with consanguineous parents, resulting in 30% of cases with possible autosomal recessive inheritance. We identified seven novel variants, four of them classified as pathogenic. In one family, we identified two mutations in exon 102, segregating in cis, suggesting an additive effect of two mutations in the same allele. This work highlights the importance of using Next-Generation Sequencing technology for the molecular diagnosis of genetic diseases when a very large gene is involved, associated to a broad distribution of the mutations along it. These data also influence the prevention through adequate genetic counseling for the families and cautions against malignant hyperthermia susceptibility.
中央核肌病(CCD)是一种遗传性神经肌肉疾病,其特征是肌肉活检中有核心。CCD 是由 RYR1 基因突变引起的。该基因编码肌质网钙释放通道的ryanodine 受体 1,当质膜去极化时,钙离子从肌质网释放到细胞质。该基因的突变也与恶性高热易感性(MHS)有关。在这项研究中,我们评估了 20 个具有 CCD 的临床和组织学特征的家族,以鉴定患者中的主要突变,为家族的诊断和遗传咨询提供依据。我们在 20/20 的家族中发现了 RYR1 基因的变异。其中 16 个变异具有分子致病性。这些变异中的大多数(22/23)是错义的,且在家族中是独特的。两个变异在两个不同的家族中是复发性的。我们确定了 6 个具有双等位基因突变的家族,5 个非近亲结婚的复合杂合子,和 1 个近亲结婚的纯合子,导致 30%的病例可能为常染色体隐性遗传。我们发现了 7 个新的变异,其中 4 个被归类为致病性的。在一个家族中,我们发现了两个位于外显子 102 的突变,在顺式中分离,表明在同一个等位基因中有两个突变的累加效应。这项工作强调了在涉及一个非常大的基因且其突变沿其广泛分布的遗传疾病的分子诊断中使用下一代测序技术的重要性。这些数据也影响了对家族的适当遗传咨询和对恶性高热易感性的警惕,以进行预防。
