IMMUNOBIOLOGY ICAM-1 on exosomes from mature dendritic cells is critical for efficient naive T-cell priming

نویسندگان

  • Elodie Segura
  • Carole Nicco
  • Bérangère Lombard
  • Philippe Véron
  • Graça Raposo
  • Frédéric Batteux
  • Sebastian Amigorena
  • Clotilde Théry
چکیده

Exosomes are secreted vesicles formed in lateendocyticcompartments. Immaturedendritic cells (DCs) secrete exosomes, which transfer functional major histocompatibility complex (MHC)–peptide complexes to other DCs. Since immature and mature DCs induce different functional T-cell responses (ie, tolerance versus priming), we asked whether DC maturation also influenced the priming abilities of their exosomes. We show that exosomes secreted by lipopolysaccharide (LPS)–treated mature DCs are 50to 100-fold more potent to induce antigenspecific T-cell activation in vitro than exosomes from immature DCs. In vitro, exosomes from mature DCs transfer to B lymphocytes the ability to prime naive T cells. In vivo, only mature exosomes trigger effector T-cell responses, leading to fast skingraft rejection.Proteomicandbiochemical analyses revealed that mature exosomes are enriched in MHC class II, B7.2, intercellular adhesion molecule 1 (ICAM-1), and bear little milk-fat globule–epidermal growth factor–factor VIII (MFG-E8) as compared with immature exosomes. Functional analysis using DC-derived exosomes from knock-out mice showed that MHC class II and ICAM-1 are required for mature exosomes to prime naive T cells, whereas B7.2 and MFG-E8 are dispensable. Therefore, changes in protein composition and priming abilities of exosomes reflect the maturation signals received by DCs. (Blood. 2005; 106:216-223)

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تاریخ انتشار 2005