Membrane Vesicles Released by Intestinal Epithelial Cells Infected with Rotavirus Inhibit T-Cell Function

Membrane Vesicles Released by Intestinal Epithelial Cells Infected with Rotavirus Inhibit T-Cell Function

Rotavirus (RV) predominantly replicates in intestinal epithelial cells (IEC), and “danger signals” released by these cells may modulate viral immunity. We have recently shown that human model IEC (Caco-2 cells) infected with rhesus-RV release a non-inflammatory group of immunomodulators that include...

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Veröffentlicht in:Viral immunology 2010-12, Vol.23 (6), p.595-608
Hauptverfasser: Barreto, Alfonso, Rodríguez, Luz-Stella, Rojas, Olga Lucía, Wolf, Marie, Greenberg, Harry B., Franco, Manuel A., Angel, Juana
Format: Artikel
Sprache:eng
Schlagworte:
Adaptive Immunity
Antigens, CD - metabolism
Antigens, Viral - metabolism
Blotting, Western
Caco-2 Cells
Capsid Proteins - metabolism
CD4-Positive T-Lymphocytes - immunology
Child, Preschool
Epithelial cells
Epitopes - immunology
Epitopes - ultrastructure
Exosomes - immunology
Exosomes - metabolism
Female
Gastroenteritis - immunology
Gastroenteritis - metabolism
Gastroenteritis - virology
Health aspects
Heat-Shock Proteins - immunology
Heat-Shock Proteins - metabolism
Humans
Immune response
Immunity, Cellular
Infant
Intestinal Mucosa - virology
Male
Microscopy, Electron, Transmission
Microscopy, Fluorescence
Physiological aspects
Platelet Membrane Glycoproteins - metabolism
Rotavirus
Rotavirus Infections - immunology
Rotaviruses
T cells
Tetraspanin 30
Transforming Growth Factor beta1 - immunology
Transforming Growth Factor beta1 - metabolism
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Zusammenfassung:Rotavirus (RV) predominantly replicates in intestinal epithelial cells (IEC), and “danger signals” released by these cells may modulate viral immunity. We have recently shown that human model IEC (Caco-2 cells) infected with rhesus-RV release a non-inflammatory group of immunomodulators that includes heat shock proteins (HSPs) and TGF-β1. Here we show that both proteins are released in part in association with membrane vesicles (MV) obtained from filtrated Caco-2 supernatants concentrated by ultracentrifugation. These MV express markers of exosomes (CD63 and others), but not of the endoplasmic reticulum (ER) or nuclei. Larger quantities of proteins associated with MV were released by RV-infected cells than by non-infected cells. VP6 co-immunoprecipitated with CD63 present in these MV, and VP6 co-localized with CD63 in RV-infected cells, suggesting that this viral protein is associated with the MV, and that this association occurs intracellularly. CD63 present in MV preparations from stool samples from 36 children with gastroenteritis due or not due to RV were analyzed. VP6 co-immunoprecipitated with CD63 in 3/8 stool samples from RV-infected children, suggesting that these MV are released by RV-infected cells in vivo . Moreover, fractions that contained MV from RV-infected cells induced death and inhibited proliferation of CD4 + T cells to a greater extent than fractions from non-infected cells. These effects were in part due to TGF-β, because they were reversed by treatment of the T cells with the TGF-β-receptor inhibitor ALK5i. MV from RV-infected and non-infected cells were heterogeneous, with morphologies and typical flotation densities described for exosomes (between 1.10 and 1.18 g/mL), and denser vesicles (>1.24 g/mL). Both types of MV from RV-infected cells were more efficient at inhibiting T-cell function than were those from non-infected cells. We propose that RV infection of IEC releases MV that modulate viral immunity.
ISSN:0882-8245
1557-8976
DOI:10.1089/vim.2009.0113