Objective. Exosomes are membrane vesicles of endosomal origin that are distinct from apoptotic bodies and are thought to represent an acellular mechanism for antigen transfer to classic antigen-presenting cells, as well as for direct antigen presentation with the capacity to induce immune response or tolerance. Nevertheless, it is not known whether exosomes are involved in the induction or regulation of immune responses against intracellular autoantigens that characterize autoimmune diseases. Exosomes have been shown to be secreted by several types of cells, whereas studies of non-neoplastic epithelial cells are lacking. This study was undertaken to investigate the capacity of nonneoplastic salivary gland epithelial cells (SGECs) to release exosomes, and to determine whether epithelial exosomes contain RNPs, which are major autoantigens in systemic rheumatic diseases.Methods. Exosomes were isolated by ultracentrifugation from culture supernatants of 26 non-neoplastic SGEC lines established from patients with various rheumatic disorders. They were analyzed by electron microscopy, immunoblotting, or immunoprecipitation.Results. All SGEC lines were found to release comparable and significant amounts of exosomes. Similar to other cell systems, exosome secretion was constitutive and was unrelated to activation or apoptotic processes. SGEC-derived exosomes were found to contain the autoantigenic Ro/SSA, La/SSB, and Sm RNPs, as well as epithelial-specific cytokeratins.Conclusion. SGECs constitutively secrete exosomes that contain the major autoantigens Ro/SSA, La/SSB, and Sm. This mechanism may represent a pathway whereby intracellular autoantigens are presented to the immune system with an immunogenic or tolerogenic outcome.Autoimmune diseases are characterized by the development of humoral responses against self antigens, most of which are intracellular proteins. Although thought to involve typical antigen-driven responses, the precise mechanism(s) involved in the presentation of such intracellular autoantigens to the immune system is unclear (1). Apoptosis and the resulting release of autoantigen-containing apoptotic vesicles are considered potential pathways for the generation of autoimmune responses (2).During the last decade, a novel cell-free mechanism of antigen presentation has been recognized (3) that involves small (30-100 nm) membrane vesicles, which are termed exosomes and are distinct from apoptotic bodies. These are different from the exosome protein complex, which is implicated in RNA processing and degradation processes. Exosomal vesicles are secreted following the fusion of multivesicular late endosome/lysosomes with the plasma membrane. Exosome production has been observed in a variety of cell types, including reticulocytes, platelets, cytotoxic T lymphocytes and B lymphocytes, dendritic cells, and neoplastic intestinal epithelial cells, whereas studies of non-neoplastic epithelial cells are lacking. Several physiologic roles have been assigned to exosomes, including the expulsion of obsolete membran...
