Exosomes released during reticulocyte maturation bind to fibronectin via integrin α4β1
2000
Rieu, Stéphanie | Géminard, Charles | Rabesandratana, Herisoa | SainteâMarie, Josette | Vidal, Michel
Exosomes are vesicles formed in the endosomal compartment and released in the extracellular medium during reticulocyte maturation into erythrocytes. They have a clearing function because of their enrichment with some proteins known to decrease or disappear from the cell surface during maturation, e.g. acetylcholinesterase and transferrin receptor. We show here that integrin α4β1, present on the surface of erythroid precursors but absent from the mature red cell membrane, is at least partly cleared from the reticulocyte plasma membrane by the exosomal pathway. Using flow cytometry, we found that the α4 subunit disappears from the reticulocyte surface during in vitro maturation. Two different monoclonal antibodies (Bâ5G10 and HP 2/1) were used to demonstrate the presence of the α4 chain on the exosome surface. Moreover, membrane acetylcholinesterase and lumenal peroxidaseâlike (i.e. hemoglobin) enzymatic activities were assayed to demonstrate exosome binding to plates coated with increasing fibronectin (FN) concentrations. This interaction was dependent on divalent cations (MnCl2â>âMgCl2â>âCaCl2). Similarly, vesicles bound to plates coated with the chymotryptic 40âK fragment (FNâ40) containing the heparinâbinding region of FN. This binding was inhibited by exosome preincubation with fibronectin CS1 peptide and with a monoclonal antibody (HP 2/1) against the integrin α4âchain, confirming an α4β1–induced interaction. The importance of the exosome clearance function is highlighted here, since the presence of VLAâ4 on reticulocytes often leads to blood circulation complications in some diseases. Moreover, the presence of α4β1 on the exosome surface, by allowing binding to endothelial cells through vascular cell adhesion molecule 1 (VCAMâ1), might confer another physiological function to the secreted vesicles.
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