Abstract
1 min readIntroduction: Cardiovascular disease (CVD) is a major cause of death in COPD. Numerous studies describe clinical evidence of endothelial dysfunction in COPD but the molecular pathways which link COPD and CVD remain unclear. Late outgrowth endothelial progenitor cells (EPC) could serve as a research tool to investigate endothelial defects in COPD patients. Aim and objectives: To examine whether EPC from COPD patients exhibit dysfunctional characteristics, illustrating the underlying molecular process of endothelial dysfunction in COPD. Methods: EPC were isolated from peripheral blood samples received from 16 healthy non smoking volunteers (age ± SEM, 57±2.7yr), 10 healthy smokers (57±2.6yr) and 16 COPD patients (67±1.6yr). The mononuclear fraction was placed in culture in the presence of endothelial growth factors. Late outgrowth colonies of EPC appeared between day 7 and 24, as characteristic cobblestone monolayers. The cells were grown to confluence in T-25 or T-75 flasks and used at passages 4 to 6 for all experiments. Endothelial senescence was measured by senescence-associated β-galactosidase (SA-β-Gal) activity and sirtuin (SIRT) 1 protein levels by Western blotting. Results: EPC from healthy smokers and COPD patients displayed significantly increased senescence and reduced SIRT1 protein levels compared to healthy non smoking subjects. SIRT1 protein levels negatively correlated with endothelial senescence. Conclusions: The results from our study demonstrate that EPC from smokers and COPD patients display epigenetic molecular dysfunctions linked to increased senescence. These defects may contribute to endothelial dysfunction and cardiovascular events.
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