Antigen-presenting cells contain a specialized late endocytic compartment, MIIC (major histocompatibility complex [MHC] class II-enriched compartment), that harbors newly synthesized MHC class II molecules in transit to the plasma membrane. MIICs have a limiting membrane enclosing characteristic internal membrane vesicles. Both the limiting membrane and the internal vesicles contain MHC class II. In this study on B lymphoblastoid cells, we demonstrate by immunoelectron microscopy that the limiting membrane of MIICs can fuse directly with the plasma membrane, resulting in release from the cells of internal MHC class II-containing vesicles. These secreted vesicles, named exosomes, were isolated from the cell culture media by differential centrifugation followed by flotation on sucrose density gradients. The overall surface protein composition of exosomes differed significantly from that of the plasma membrane. Exosome-bound MHC class II was in a compact, peptide-bound conformation. Metabolically labeled MHC class II was released into the extracellular medium with relatively slow kinetics, 10 +/- 4% in 24 h, indicating that direct fusion of MIICs with the plasma membrane is not the major pathway by which MHC class II reaches the plasma membrane. Exosomes derived from both human and murine B lymphocytes induced antigen-specific MHC class II-restricted T cell responses. These data suggest a role for exosomes in antigen presentation in vivo.
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1 March 1996
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March 01 1996
B lymphocytes secrete antigen-presenting vesicles.
G Raposo,
G Raposo
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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H W Nijman,
H W Nijman
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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W Stoorvogel,
W Stoorvogel
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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R Liejendekker,
R Liejendekker
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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C V Harding,
C V Harding
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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C J Melief,
C J Melief
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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H J Geuze
H J Geuze
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
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G Raposo
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
H W Nijman
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
W Stoorvogel
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
R Liejendekker
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
C V Harding
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
C J Melief
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
H J Geuze
Department of Cell Biology, Faculty of Medicine and Institute for Biomembranes, Utrecht University, The Netherlands.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1996) 183 (3): 1161–1172.
Citation
G Raposo, H W Nijman, W Stoorvogel, R Liejendekker, C V Harding, C J Melief, H J Geuze; B lymphocytes secrete antigen-presenting vesicles.. J Exp Med 1 March 1996; 183 (3): 1161–1172. doi: https://doi.org/10.1084/jem.183.3.1161
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