Publication details

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

Authors

JELÍNKOVÁ Šárka SLEIMAN Yvonne FOJTÍK Petr AIMOND Franck FINAN Amanda HUGON Gerald SCHEUERMANN Valerie BECKEROVÁ Deborah CAZORLA Olivier VINCENTI Marie AMEDRO Pascal RICHARD Sylvain JAROŠ Josef DVOŘÁK Petr LACAMPAGNE Alain CARNAC Gilles ROTREKL Vladimír MELI Albano C.

Year of publication 2021
Type Article in Periodical
Magazine / Source International Journal of Molecular Sciences
MU Faculty or unit

Faculty of Medicine

Citation
Web https://www.mdpi.com/1422-0067/22/9/5025
Doi http://dx.doi.org/10.3390/ijms22095025
Keywords duchenne muscular dystrophy; mdx mouse; cardiovascular progenitors; c-kit; genomic instability; dilated cardiomyopathy
Description 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 (mdx) to investigate age-dependent CVPC properties. Using quantitative PCR, flow cytometry, speckle tracking echocardiography, and immunofluorescence, we revealed that young mdx mice exhibit elevated CVPCs. We observed a rapid age-related CVPC depletion, coinciding with the progressive onset of cardiac dysfunction. Moreover, mdx 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.
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