动力蛋白 2 为中心核肌病带来新希望。
Dynamin 2 the rescue for centronuclear myopathy.
出版信息
J Clin Invest. 2014 Mar;124(3):976-8. doi: 10.1172/JCI74434. Epub 2014 Feb 24.
Abstract
Centronuclear myopathy is a lethal muscle disease. The most severe form of the disease, X-linked centronuclear myopathy, is due to mutations in the gene encoding myotubularin (MTM1), while mutations in dynamin 2 (DNM2) and amphiphysin 2/BIN1 (AMPH2) cause milder forms of myopathy. MTM1 is a lipid phosphatase, and mutations that disrupt this activity cause severe muscle wasting. In this issue of the JCI, Cowling and colleagues report on their finding of increased DNM2 levels in human and mouse muscle with MTM1 mutations. Partial reduction of Dnm2 in mice harboring Mtm1 mutations remarkably rescued muscle wasting and lethality, and this effect was muscle specific. DNM2 regulates membrane trafficking through vesicular scission, and it is presumed that reducing this activity accounts for improved outcome in X-linked centronuclear myopathy.
摘要
中心核肌病是一种致命的肌肉疾病。该病最严重的形式,X 连锁中心核肌病,是由于编码肌小管素(MTM1)的基因突变所致,而 dynamin 2(DNM2)和 amphiphysin 2/BIN1(AMPH2)的突变则导致更为轻微的肌病形式。MTM1 是一种脂质磷酸酶,破坏其活性的突变会导致严重的肌肉消耗。在本期 JCI 中,Cowling 及其同事报告了他们在携带 MTM1 突变的人类和小鼠肌肉中发现 DNM2 水平升高的发现。在携带 Mtm1 突变的小鼠中,DNm2 的部分减少显著挽救了肌肉消耗和致死性,并且这种作用是肌肉特异性的。DNM2 通过囊泡分裂调节膜运输,据推测,降低这种活性解释了 X 连锁中心核肌病的改善结果。
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