Choi Eunseok, Shin Soyoung, Lee Sangjee, Lee Sook Joung, Park Joonhong
Department of Physical Medicine and Rehabilitation, College of Medicine, The Catholic University of Korea, Seoul, Republic of Korea.
Department of Laboratory Medicine, College of Medicine, The Catholic University of Korea, Seoul, Republic of Korea.
Clin Chim Acta. 2020 Sep;508:28-32. doi: 10.1016/j.cca.2020.05.011. Epub 2020 May 7.
Bethlem myopathy is a kind of collagen VI related myopathy which affects proximal skeletal muscles and leads to gait disturbance and multiple joint contractures with an onset in the first two decades of life. Lung function impairment (respiratory muscle and diaphragmatic weakness, ventilatory restriction, hypoxaemia and hypercapnia) and respiratory failure are part of the clinical spectrum and can occur in ambulatory patients.
We carried out whole exome sequencing (WES) in combination with neuromuscular diseases-associated genes-filtering to detect the possible causative mutation(s) in a Korean family with Bethlem myopathy. An electrodiagnostic study showed myopathic pattern (normal nerve conduction study, and early recruitment and short amplitude muscle unit action potentials) in the proband.
Coexistence of digenic mutations in the collagen VI genes (COL6A1 and COL6A3) was identified by WES in the proband only: heterozygous missense mutations of the COL6A1 (NM_001848.2: c.823G > T, p.Gly275Trp; rs1556425467) and of the COL6A3 genes (NM_004369.3: c.9349G > A, p.Asp3117Asn; rs1226664855). COL6A3 mutation may be candidate as disease-associated variant, as far as it was found only in the proband harboring another heterozygous mutation in COL6A1 gene, previously reported as different pathogenic mutations (p.Gly275Arg and p.Gly275Glu) at the same codon in Bethlem myopathy.
Our findings suggest that the coexistence of these digenic mutations is rare, but it may be used for the risk evaluation of individuals with a possible susceptibility to Bethlem myopathy. Taken together, genetic diagnosis using WES is a useful approach for the identification of pathogenic mutations associated with Bethlem myopathy.
贝斯勒姆肌病是一种与胶原蛋白VI相关的肌病,影响近端骨骼肌,导致步态障碍和多个关节挛缩,发病于生命的前二十年。肺功能损害(呼吸肌无力和膈肌无力、通气受限、低氧血症和高碳酸血症)及呼吸衰竭是临床症状的一部分,可发生于能行走的患者中。
我们对一个患有贝斯勒姆肌病的韩裔家族进行了全外显子组测序(WES),并结合神经肌肉疾病相关基因筛选,以检测可能的致病突变。一项电诊断研究显示先证者存在肌病模式(神经传导研究正常,早期募集和短时限肌肉单位动作电位)。
仅在先证者中通过WES鉴定出胶原蛋白VI基因(COL6A1和COL6A3)双基因突变异质性:COL6A1基因(NM_001848.2:c.823G>T,p.Gly275Trp;rs1556425467)和COL6A3基因(NM_004369.3:c.9349G>A,p.Asp3117Asn;rs1226664855)的杂合错义突变。COL6A3突变可能是疾病相关变异体,因为它仅在先证者中发现,该先证者在COL6A1基因中还存在另一个杂合突变,此前在贝斯勒姆肌病中同一密码子处已报道为不同的致病突变(p.Gly275Arg和p.Gly275Glu)。
我们的研究结果表明,这些双基因突变的共存很罕见,但可用于对可能易患贝斯勒姆肌病的个体进行风险评估。综上所述,使用WES进行基因诊断是鉴定与贝斯勒姆肌病相关致病突变的一种有用方法。
