Carvalho Andreia, Costa Carmen, Pinto Miguel, Taipa Ricardo, Gonçalves Ana, Oliveira Márcia E, Ferreira Sofia, Ribeiro Joana Afonso
Neurology Department, Centro Hospitalar de Vila Nova de Gaia-Espinho, Portugal.
Pediatric Neurology Department, Centro de Desenvolvimento da Criança, Hospital Pediátrico de Coimbra - Centro Hospitalar e Universitário de Coimbra, Coimbra, Portugal.
J Pediatr Genet. 2021 Jun 1;12(3):258-262. doi: 10.1055/s-0041-1728745. eCollection 2023 Sep.
X-linked myotubular myopathy (XLMTM), a centronuclear congenital myopathy secondary to pathogenic variants in the gene encoding myotubularin, is typically recognized for its classic and severe phenotype which includes neonatal hypotonia, severe muscle weakness, long-term ventilator dependence, markedly delayed gross motor milestones with inability to independently ambulate, and a high neonatal and childhood mortality. However, milder congenital forms of the condition and other phenotypes are recognized. We describe a 6-year-old boy with a mild XLMTM phenotype with independent gait and no respiratory insufficiency even in the neonatal period. The child has a hemizygous novel splice site variant in the gene (c.232-25A > T) whose pathogenicity was confirmed by cDNA studies (exon 5 skipping) and muscle biopsy findings. We also compared the phenotype of our patient with the few reported cases that presented a mild XLMTM phenotype and no respiratory distress at birth, and discussed the potential mechanisms underlying this phenotype such as the presence of residual expression of the normal myotubularin transcript.
X连锁性肌管性肌病(XLMTM)是一种继发于编码肌管素基因致病性变异的中央核性先天性肌病,其典型的严重表型包括新生儿肌张力减退、严重肌肉无力、长期依赖呼吸机、粗大运动里程碑明显延迟且无法独立行走,以及新生儿期和儿童期的高死亡率。然而,也认识到该疾病存在较轻的先天性形式和其他表型。我们描述了一名6岁男孩,具有轻度XLMTM表型,即使在新生儿期也有独立步态且无呼吸功能不全。该患儿在该基因中有一个半合子新型剪接位点变异(c.232-25A>T),其致病性通过cDNA研究(外显子5跳跃)和肌肉活检结果得以证实。我们还将我们患者的表型与少数报道的出生时表现为轻度XLMTM表型且无呼吸窘迫的病例进行了比较,并讨论了这种表型潜在的机制,如正常肌管素转录本残留表达的存在。
