Human Aortic Valve Interstitial Cells Display Proangiogenic Properties During Calcific Aortic Valve Disease

Nicolas Gendron; Nicolas Gendron; Mickaël Rosa; Mickaël Rosa; Adeline Blandinières; Adeline Blandinières; Yoann Sottejeau; Yoann Sottejeau; Elisa Rossi; Elisa Rossi; Éric Van Belle; Éric Van Belle; Salim Idelcadi; Salim Idelcadi; Séverine Lecourt; Séverine Lecourt; André Vincentelli; André Vincentelli; Audrey Cras; Audrey Cras; Ramadan Jashari; Ramadan Jashari; Richard Chocron; Richard Chocron; Yaël Baudouin; Yaël Baudouin; Thibault Pamart; Thibault Pamart; Ivan Bièche; Ivan Bièche; Nathalie Névo; Nathalie Névo; Bernard Cholley; Bernard Cholley; Jeanne Rancic; Jeanne Rancic; Bart Staels; Bart Staels; Pascale Gaussem; Pascale Gaussem; Annabelle Dupont; Annabelle Dupont; Alain Carpentier; Alain Carpentier; Sophie Susen; Sophie Susen; David M. Smadja; David M. Smadja

doi:10.1161/atvbaha.120.314287

Abstract

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Objective: The study’s aim was to analyze the capacity of human valve interstitial cells (VICs) to participate in aortic valve angiogenesis. Approach and Results: VICs were isolated from human aortic valves obtained after surgery for calcific aortic valve disease and from normal aortic valves unsuitable for grafting (control VICs). We examined VIC in vitro and in vivo potential to differentiate in endothelial and perivascular lineages. VIC paracrine effect was also examined on human endothelial colony-forming cells. A pathological VIC (VIC p ) mesenchymal-like phenotype was confirmed by CD90 + /CD73 + /CD44 + expression and multipotent-like differentiation ability. When VIC p were cocultured with endothelial colony-forming cells, they formed microvessels by differentiating into perivascular cells both in vivo and in vitro. VIC p and control VIC conditioned media were compared using serial ELISA regarding quantification of endothelial and angiogenic factors. Higher expression of VEGF (vascular endothelial growth factor)-A was observed at the protein level in VIC p -conditioned media and confirmed at the mRNA level in VIC p compared with control VIC. Conditioned media from VIC p induced in vitro a significant increase in endothelial colony-forming cell proliferation, migration, and sprouting compared with conditioned media from control VIC. These effects were inhibited by blocking VEGF-A with blocking antibody or siRNA approach, confirming VIC p involvement in angiogenesis by a VEGF-A dependent mechanism. Conclusions: We provide here the first proof of an angiogenic potential of human VICs isolated from patients with calcific aortic valve disease. These results point to a novel function of VIC p in valve vascularization during calcific aortic valve disease, with a perivascular differentiation ability and a VEGF-A paracrine effect. Targeting perivascular differentiation and VEGF-A to slow calcific aortic valve disease progression warrants further investigation.

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Human Aortic Valve Interstitial Cells Display Proangiogenic Properties During Calcific Aortic Valve Disease

Abstract

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