par Vanorle, Marion 
;Lemaire, Anne ;Di Pietrantonio, Larissa ;Horckmans, Michael ;Communi, Didier
Référence Purinergic Signalling
Publication Publié, 2021-07-11
;Lemaire, Anne ;Di Pietrantonio, Larissa ;Horckmans, Michael ;Communi, Didier Référence Purinergic Signalling
Publication Publié, 2021-07-11
Article révisé par les pairs
| Résumé : | The ability of cardiac adipose–derived stem cells (cADSC) to differentiate into multiple cell types has opened new perspectives in cardiac cell–based regenerative therapies. P2Y nucleotide receptors have already been described as regulators of adipogenic differentiation of cADSC and bone marrow–derived stem cells. In this study, we defined UTP as a regulator of cADSC endothelial differentiation. A daily UTP stimulation of cADSC during endothelial predifferentiation increased their capacity to form an endothelial network in matrigel. Additionally, pro-angiogenic UTP target genes such as epiregulin and hyaluronan synthase-1 were identified in predifferentiated cADSC by RNA sequencing experiments. Their regulation by UTP was confirmed by qPCR and ELISA experiments. We then evaluated the capacity of UTP-treated predifferentiated cADSC to increase post-ischemic revascularization in mice subjected to left anterior descending artery ligation. Predifferentiated cADSC treated or not with UTP were injected in the periphery of the infarcted zone, 3 days after ligation. We observed a significant increase of capillary density 14 and 30 days after UTP-treated predifferentiated cADSC injection, correlated with a reduction of cardiac fibrosis. This revascularization increase was not observed after injection of UTP-treated cADSC deficient for UTP and ATP nucleotide receptor P2Y2. The present study highlights the P2Y2 receptor as a regulator of cADSC endothelial differentiation and as a potential target for the therapeutic use of cADSC in post-ischemic heart revascularization. |
