Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), Illkirch 67400, France; INSERM U964, Illkirch 67400, France; CNRS UMR7104, Illkirch 67400, France; Strasbourg University, Illkirch 67400, France.
INSERM U964, Illkirch 67400, France; CNRS UMR7104, Illkirch 67400, France; Strasbourg University, Illkirch 67400, France.
Mol Ther. 2018 Apr 4;26(4):1082-1092. doi: 10.1016/j.ymthe.2018.02.008. Epub 2018 Feb 14.
Myotubular myopathy, or X-linked centronuclear myopathy, is a severe muscle disorder representing a significant burden for patients and their families. It is clinically characterized by neonatal and severe muscle weakness and atrophy. Mutations in the myotubularin (MTM1) gene cause myotubular myopathy, and no specific curative treatment is available. We previously found that dynamin 2 (DNM2) is upregulated in both Mtm1 knockout and patient muscle samples, whereas its reduction through antisense oligonucleotides rescues the clinical and histopathological features of this myopathy in mice. Here, we propose a novel approach targeting Dnm2 mRNA. We screened and validated in vitro and in vivo several short hairpin RNA (shRNA) sequences that efficiently target Dnm2 mRNA. A single intramuscular injection of AAV-shDnm2 resulted in long-term reduction of DNM2 protein level and restored muscle force, mass, histology, and myofiber ultrastructure and prevented molecular defects linked to the disease. Our results demonstrate a robust DNM2 knockdown and provide an alternative strategy based on reduction of DNM2 to treat myotubular myopathy.
肌管性肌病,或 X 连锁中轴核肌病,是一种严重的肌肉疾病,给患者及其家庭带来了巨大的负担。其临床特征为新生儿期出现严重的肌肉无力和萎缩。肌小管素 1 (MTM1)基因突变会导致肌管性肌病,目前尚无特效治疗方法。我们之前发现 dynamin 2 (DNM2)在 Mtm1 敲除和患者肌肉样本中均上调,而通过反义寡核苷酸降低其水平可挽救该肌病在小鼠中的临床和组织病理学特征。在这里,我们提出了一种针对 Dnm2 mRNA 的新方法。我们在体外和体内筛选和验证了几种有效靶向 Dnm2 mRNA 的短发夹 RNA (shRNA)序列。单次肌肉内注射 AAV-shDnm2 可长期降低 DNM2 蛋白水平,并恢复肌肉力量、质量、组织学以及肌纤维超微结构,防止与疾病相关的分子缺陷。我们的结果证明了 DNM2 的有效敲低,并提供了一种基于降低 DNM2 水平来治疗肌管性肌病的替代策略。
