School of Kinesiology and Health Science and the Muscle Health Research Centre, York University, Toronto, ON, Canada.
Department of Human Health and Nutritional Sciences and Cardiovascular Research Group, University of Guelph, Guelph, ON, Canada.
J Physiol. 2020 Apr;598(7):1377-1392. doi: 10.1113/JP277306. Epub 2019 Feb 27.
Ninety-eight per cent of patients with Duchenne muscular dystrophy (DMD) develop cardiomyopathy, with 40% developing heart failure. While increased propensity for mitochondrial induction of cell death has been observed in left ventricle, it remains unknown whether this is linked to impaired mitochondrial respiratory control and elevated H O emission prior to the onset of cardiomyopathy. Classic mouse models of DMD demonstrate hyper-regeneration in skeletal muscle which may mask mitochondrial abnormalities. Using a model with less regenerative capacity that is more akin to DMD patients, we observed elevated left ventricular mitochondrial H O and impaired oxidative phosphorylation in the absence of cardiac remodelling or overt cardiac dysfunction at 4 weeks. These impairments were associated with dysfunctions at complex I, governance by ADP and creatine-dependent phosphate shuttling, which results in a less efficient response to energy demands. Mitochondria may be a therapeutic target for the treatment of cardiomyopathy in DMD.
In Duchenne muscular dystrophy (DMD), mitochondrial dysfunction is predicted as a response to numerous cellular stressors, yet the contribution of mitochondria to the onset of cardiomyopathy remains unknown. To resolve this uncertainty, we designed in vitro assessments of mitochondrial bioenergetics to model mitochondrial control parameters that influence cardiac function. Both left ventricular mitochondrial responsiveness to the central bioenergetic controller ADP and the ability of creatine to facilitate mitochondrial-cytoplasmic phosphate shuttling were assessed. These measurements were performed in D2.B10-DMD /2J mice - a model that demonstrates skeletal muscle atrophy and weakness due to limited regenerative capacities and cardiomyopathy more akin to people with DMD than classic models. At 4 weeks of age, there was no evidence of cardiac remodelling or cardiac dysfunction despite impairments in ADP-stimulated respiration and ADP attenuation of H O emission. These impairments were seen at both submaximal and maximal ADP concentrations despite no reductions in mitochondrial content markers. The ability of creatine to enhance ADP's control of mitochondrial bioenergetics was also impaired, suggesting an impairment in mitochondrial creatine kinase-dependent phosphate shuttling. Susceptibly to permeability transition pore opening and the subsequent activation of cell death pathways remained unchanged. Mitochondrial H O emission was elevated despite no change in markers of irreversible oxidative damage, suggesting alternative redox signalling mechanisms should be explored. These findings demonstrate that selective mitochondrial dysfunction precedes the onset of overt cardiomyopathy in D2.mdx mice, suggesting that improving mitochondrial bioenergetics by restoring ADP, creatine-dependent phosphate shuttling and complex I should be considered for treating DMD patients.
98%的杜氏肌营养不良症(DMD)患者会发展为心肌病,其中 40%会发展为心力衰竭。虽然在左心室中观察到线粒体诱导细胞死亡的倾向增加,但尚不清楚这是否与线粒体呼吸控制受损以及在心肌病发生前 H2O 排放增加有关。DMD 的经典小鼠模型显示出骨骼肌的过度再生,这可能掩盖了线粒体异常。我们使用一种再生能力较低且更类似于 DMD 患者的模型,在 4 周时观察到左心室线粒体 H2O 升高和氧化磷酸化受损,而没有心脏重构或明显的心脏功能障碍。这些损伤与复合物 I、ADP 控制和肌酸依赖的磷酸穿梭功能障碍有关,导致对能量需求的反应效率降低。线粒体可能是治疗 DMD 心肌病的一个治疗靶点。
在杜氏肌营养不良症(DMD)中,线粒体功能障碍被预测为对多种细胞应激的反应,但线粒体对心肌病发病的贡献仍不清楚。为了解决这一不确定性,我们设计了体外评估线粒体生物能学的方法来模拟影响心脏功能的线粒体控制参数。我们评估了左心室线粒体对中央生物能控制器 ADP 的反应性以及肌酸促进线粒体-细胞质磷酸穿梭的能力。这些测量是在 D2.B10-DMD/2J 小鼠中进行的,该模型由于再生能力有限且更类似于 DMD 患者的心肌病,而不是经典模型,因此表现出骨骼肌萎缩和无力。在 4 周龄时,尽管 ADP 刺激呼吸和 ADP 抑制 H2O 排放受损,但没有心脏重构或心脏功能障碍的证据。尽管线粒体含量标志物没有减少,但在亚最大和最大 ADP 浓度下都出现了这些损伤。肌酸增强 ADP 对线粒体生物能学控制的能力也受损,表明线粒体肌酸激酶依赖性磷酸穿梭受损。对通透性转换孔开放和随后的细胞死亡途径激活的易感性没有改变。尽管不可逆氧化损伤的标志物没有变化,但线粒体 H2O 排放增加,表明应探索替代的氧化还原信号转导机制。这些发现表明,选择性线粒体功能障碍先于 D2.mdx 小鼠明显的心肌病发作,这表明通过恢复 ADP、肌酸依赖的磷酸穿梭和复合物 I 来改善线粒体生物能学应该被考虑用于治疗 DMD 患者。
