在肌营养不良模型中,心脏的自噬增强且独立于疾病进展

IF 1.4 Q3 CARDIAC & CARDIOVASCULAR SYSTEMS JRSM Cardiovascular Disease Pub Date : 2019-01-01 DOI:10.1177/2048004019879581
H. Spaulding, C. Ballmann, J. Quindry, M. Hudson, J. Selsby
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引用次数: 2

摘要

背景Duchenne肌营养不良是一种肌肉萎缩性疾病,由肌营养不良蛋白基因突变引起肌营养不良蛋白质功能紊乱。自噬是一种蛋白水解过程,在营养不良的骨骼肌中受损,尽管对营养不良蛋白缺乏对心肌自噬的影响知之甚少。我们假设,随着疾病的进展,基于间接自噬标记物,自噬将变得越来越功能障碍。方法采用蛋白质印迹法检测7周龄和17个月龄对照(C57)和营养不良(mdx)心脏的自噬标志物。结果与我们的假设相反,两组之间的自噬标志物相似。鉴于这些令人惊讶的结果,使用14个月大的mdx小鼠或10个月大mdx/Utrn±小鼠进行了两项独立实验,这是一种更严重的杜兴肌营养不良模型。来自这些动物的数据表明自噬体降解增加。结论这些数据表明,自噬在营养不良心肌中没有像在营养不良骨骼肌中那样受损,并且疾病进展和相关损伤与自噬功能障碍无关。
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Autophagy in the heart is enhanced and independent of disease progression in mus musculus dystrophinopathy models
Background Duchenne muscular dystrophy is a muscle wasting disease caused by dystrophin gene mutations resulting in dysfunctional dystrophin protein. Autophagy, a proteolytic process, is impaired in dystrophic skeletal muscle though little is known about the effect of dystrophin deficiency on autophagy in cardiac muscle. We hypothesized that with disease progression autophagy would become increasingly dysfunctional based upon indirect autophagic markers. Methods Markers of autophagy were measured by western blot in 7-week-old and 17-month-old control (C57) and dystrophic (mdx) hearts. Results Counter to our hypothesis, markers of autophagy were similar between groups. Given these surprising results, two independent experiments were conducted using 14-month-old mdx mice or 10-month-old mdx/Utrn± mice, a more severe model of Duchenne muscular dystrophy. Data from these animals suggest increased autophagosome degradation. Conclusion Together these data suggest that autophagy is not impaired in the dystrophic myocardium as it is in dystrophic skeletal muscle and that disease progression and related injury is independent of autophagic dysfunction.
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来源期刊
JRSM Cardiovascular Disease
JRSM Cardiovascular Disease CARDIAC & CARDIOVASCULAR SYSTEMS-
自引率
6.20%
发文量
12
审稿时长
12 weeks
期刊最新文献
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