Abstract EN:

Adipose tissue (AT) contains stem/progenitor cells included in the CD34+/CD31- fraction which have adipogenic and angiogenic abilities. The aim of this work was to characterize human CD34+/CD31- cell phenotype and location within AT and to study the effect of the microenvironment on their proliferation, differentiation and mobilization capacities. The present work demonstrate that native AT stem/progenitor cells are positive for the CD34 antigen that is inversely correlated to cell expansion in vitro whereas the expression of pericyte makers is induced by cell culture. The CD34+/CD31- cells are localized in AT stroma and nearby capillaries but rarely display a pericytic position. The CD34+/CD31- cells exhibit a proliferative activity in situ which is increased by the degree of obesity. Concerning the effect of microenvironment on CD34+/CD31- cell proliferation, adipocyte- and capillary endothelial cells (CECs)-conditioned media (CM), hypoxia, leptin, IL-6, LPA, and VEGF, all increase CD34+/CD31- cell proliferation in vitro. Macrophage-CM has an anti-proliferative effect that is suppressed by an antioxidant. During AT extensive development, the appearance of a population of small adipocytes, in situ, is associated with a decrease in CD34+/CD31- cell number and molecular profile modifications toward an adipogenic lineage suggesting a commitment of CD34+/CD31- cells toward an adipogenic phenotype. Conversely, adipocyte-, CECs- and macrophage-CM have an angiogenic activity on CD34+/CD31- cells in vitro. Finally, the migration and differentiation of CD34+/CD31- cells are modulated by CECs in vitro. SDF-1 secreted by CECs promote the chemotaxis and differentiation of CD34+/CD31- cells and thus might contribute to the formation of AT-vascular network during the development of AT. Taken together, these results characterize the influence of the "adipose niche" on the control of AT-stem/progenitor cell proliferation, differentiation and migration.