Department of Neurology Rui Jin Hospital & Rui Jin Hospital North Shanghai Jiao Tong University School of Medicine Shanghai 200025 China.
Core Facility of Basic Medical Sciences Shanghai Jiao Tong University School of Medicine Shanghai 200025 China.
Ann Clin Transl Neurol. 2019 May 8;6(6):1062-1071. doi: 10.1002/acn3.787. eCollection 2019 Jun.
GDP-mannose pyrophosphorylase B (GMPPB) related phenotype spectrum ranges widely from congenital myasthenic syndrome (CMS), limb-girdle muscular dystrophy type 2T (LGMD 2T) to severe congenital muscle-eye-brain syndrome. Our study investigates the clinicopathologic features of a patient with novel mutations and explores the pathogenetic mechanism.
The patient was a 22-year-old woman with chronic proximal limb weakness for 9 years without cognitive deterioration. Weakness became worse after fatigue. Elevated serum creatine kinase and decrements on repetitive nerve stimulation test were recorded. MRI showed fatty infiltration in muscles of lower limbs and shoulder girdle on T1 sequence. Open muscle biopsy and genetic analysis were performed.
Muscle biopsy showed myogenic changes. Two missense mutations in gene (c.803T>C and c.1060G>A) were identified in the patient. Western blotting and immunostaining showed GMPPB and -dystroglycan deficiency in the patient's muscle. In vitro, mutant GMPPB forming cytoplasmic aggregates completely colocalized with microtubule-associated protein 1 light chain 3-II (LC3-II), a classical marker of autophagosome. Degradation of GMPPB was accompanied by an upregulation of LC3-II, which could be restored by lysosomal inhibitor leupeptin.
We identified two novel mutations causing overlap phenotype between LGMD 2T and CMS. We provided the initial evidence that mutant GMPPB colocalizes with autophagosome at subcellular level. GMPPB mutants degraded by autophagy-lysosome pathway is associated with LGMD 2T. This study shed the light into the enzyme replacement which could become one of the therapeutic targets in the future study.
GDP-甘露糖焦磷酸化酶 B(GMPPB)相关表型谱范围广泛,从先天性肌无力综合征(CMS)、肢带型肌营养不良 2T 型(LGMD 2T)到严重先天性肌-眼-脑综合征。本研究探讨了一位具有新型突变的患者的临床病理特征,并探讨了其发病机制。
患者为 22 岁女性,慢性近端肢体无力 9 年,无认知恶化。疲劳后症状加重。血清肌酸激酶升高,重复神经刺激试验有递减。MRI 在 T1 序列上显示下肢和肩部肌肉脂肪浸润。进行了开放性肌肉活检和基因分析。
肌肉活检显示肌源性改变。在患者的基因中发现了两个错义突变(c.803T>C 和 c.1060G>A)。Western blot 和免疫染色显示患者肌肉中的 GMPPB 和 -dystroglycan 缺乏。在体外,突变的 GMPPB 形成的细胞质聚集体与微管相关蛋白 1 轻链 3-II(LC3-II)完全共定位,LC3-II 是自噬体的经典标志物。GMPPB 的降解伴随着 LC3-II 的上调,这可以通过溶酶体抑制剂亮肽素恢复。
我们鉴定了两个导致 LGMD 2T 和 CMS 重叠表型的新型突变。我们提供了初步证据,表明突变的 GMPPB 在亚细胞水平上与自噬体共定位。通过自噬-溶酶体途径降解的 GMPPB 突变体与 LGMD 2T 相关。本研究为酶替代治疗提供了新的见解,可能成为未来研究的治疗靶点之一。
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