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肌营养不良症导致心脏中心血管祖细胞进行性耗竭。

Dystrophin Deficiency Causes Progressive Depletion of Cardiovascular Progenitor Cells in the Heart.

机构信息

Department of Biology, Faculty of Medicine, Masaryk University, Kamenice 5/A3, 62500 Brno, Czech Republic.

ICRC, St Anne's University Hospital, Pekařská 53, 65691 Brno, Czech Republic.

出版信息

Int J Mol Sci. 2021 May 10;22(9):5025. doi: 10.3390/ijms22095025.

DOI:10.3390/ijms22095025
PMID:34068508
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8125982/
Abstract

Duchenne muscular dystrophy (DMD) is a devastating condition shortening the lifespan of young men. DMD patients suffer from age-related dilated cardiomyopathy (DCM) that leads to heart failure. Several molecular mechanisms leading to cardiomyocyte death in DMD have been described. However, the pathological progression of DMD-associated DCM remains unclear. In skeletal muscle, a dramatic decrease in stem cells, so-called satellite cells, has been shown in DMD patients. Whether similar dysfunction occurs with cardiac muscle cardiovascular progenitor cells (CVPCs) in DMD remains to be explored. We hypothesized that the number of CVPCs decreases in the dystrophin-deficient heart with age and disease state, contributing to DCM progression. We used the dystrophin-deficient mouse model ( to investigate age-dependent CVPC properties. Using quantitative PCR, flow cytometry, speckle tracking echocardiography, and immunofluorescence, we revealed that young mice exhibit elevated CVPCs. We observed a rapid age-related CVPC depletion, coinciding with the progressive onset of cardiac dysfunction. Moreover, CVPCs displayed increased DNA damage, suggesting impaired cardiac muscle homeostasis. Overall, our results identify the early recruitment of CVPCs in dystrophic hearts and their fast depletion with ageing. This latter depletion may participate in the fibrosis development and the acceleration onset of the cardiomyopathy.

摘要

杜氏肌营养不良症(DMD)是一种缩短年轻男性寿命的毁灭性疾病。DMD 患者患有与年龄相关的扩张型心肌病(DCM),导致心力衰竭。已经描述了导致 DMD 中心肌细胞死亡的几种分子机制。然而,DMD 相关 DCM 的病理进展仍不清楚。在骨骼肌中,已在 DMD 患者中显示出干细胞,即所谓的卫星细胞数量急剧减少。在 DMD 中,心肌心血管祖细胞(CVPC)是否存在类似的功能障碍仍有待探索。我们假设随着年龄和疾病状态的增加,缺乏 dystrophin 的心脏中 CVPC 的数量减少,导致 DCM 进展。我们使用缺乏 dystrophin 的小鼠模型(进行研究。使用定量 PCR、流式细胞术、斑点跟踪超声心动图和免疫荧光,我们揭示了年轻的 小鼠中 CVPC 数量增加。我们观察到与心脏功能障碍进行性发作相一致的快速与年龄相关的 CVPC 耗竭。此外, CVPC 显示出增加的 DNA 损伤,表明心脏肌肉内稳态受损。总体而言,我们的研究结果表明,在 DMD 心脏中早期招募 CVPC,随着年龄的增长迅速耗竭。后者的耗竭可能参与纤维化的发展和心肌病的加速发作。

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