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dc.contributor.authorSilva-Álvarez, Valeriaes
dc.contributor.authorFolle López, Ana Maitees
dc.contributor.authorRamos Odella, Ana Líaes
dc.contributor.authorKitano, E. S.es
dc.contributor.authorIwai, L. K.es
dc.contributor.authorCorraliza, I.es
dc.contributor.authorCórsico, B.es
dc.contributor.authorFerreira, Ana Maríaes
dc.date.accessioned2019-10-02T22:14:48Z-
dc.date.available2019-10-02T22:14:48Z-
dc.date.issued2016es
dc.date.submitted20191001es
dc.identifier.citationSilva, V., et al.Echinococcus granulosus Antigen B binds to monocytes and macrophages modulating cell response to inflammation. Parasites and Vectors, 2016 9 (1), art. no. 69. doi: 10.1186/s13071-016-1350-7es
dc.identifier.issn1756-3305es
dc.identifier.urihttps://hdl.handle.net/20.500.12008/22084-
dc.description.abstractBackground: Antigen B (EgAgB) is an abundant lipoprotein released by the larva of the cestode Echinococcus granulosus into the host tissues. Its protein moiety belongs to the cestode-specific family known as hydrophobic ligand binding protein (HLBP), and is encoded by five gene subfamilies (EgAgB8/1-EgAgB8/5). The functions of EgAgB in parasite biology remain unclear. It may play a role in the parasite's lipid metabolism since it carries host lipids that E. granulosus is unable to synthesise. On the other hand, there is evidence supporting immuno-modulating activities in EgAgB, particularly on innate immune cells. Both hypothetical functions might involve EgAgB interactions with monocytes and macrophages, which have not been formally analysed yet. Methods: EgAgB binding to monocytes and macrophages was studied by flow cytometry using inflammation-recruited peritoneal cells and the THP-1 cell line. Involvement of the protein and phospholipid moieties in EgAgB binding to cells was analysed employing lipid-free recombinant EgAgB subunits and phospholipase D treated-EgAgB (lacking the polar head of phospholipids). Competition binding assays with plasma lipoproteins and ligands for lipoprotein receptors were performed to gain information about the putative EgAgB receptor(s) in these cells. Arginase-I induction and PMA/LPS-triggered IL-1β, TNF-α and IL-10 secretion were examined to investigate the outcome of EgAgB binding on macrophage response. Results: Monocytes and macrophages bound native EgAgB specifically; this binding was also found with lipid-free rEgAgB8/1 and rEgAgB8/3, but not rEgAgB8/2 subunits. EgAgB phospholipase D-treatment, but not the competition with phospholipid vesicles, caused a strong inhibition of EgAgB binding activity, suggesting an indirect contribution of phospholipids to EgAgB-cell interaction. Furthermore, competition binding assays indicated that this interaction may involve receptors with affinity for plasma lipoproteins. At functional level, the exposure of macrophages to EgAgB induced a very modest arginase-I response and inhibited PMA/LPS-mediated IL-1β and TNF-α secretion in an IL-10-independent manner. Conclusion: EgAgB and, particularly its predominant EgAgB8/1 apolipoprotein, are potential ligands for monocyte and macrophage receptors. These receptors may also be involved in plasma lipoprotein recognition and induce an anti-inflammatory phenotype in macrophages upon recognition of EgAgB.es
dc.format.mimetypeapplication/pdfes
dc.language.isoenes
dc.publisherBioMed Central Ltd.es
dc.relation.ispartofParasites and Vectors, 2016 9 (1), art. no. 69es
dc.rightsLas obras depositadas en el Repositorio se rigen por la Ordenanza de los Derechos de la Propiedad Intelectual de la Universidad De La República. (Res. Nº 91 de C.D.C. de 8/III/1994 – D.O. 7/IV/1994) y por la Ordenanza del Repositorio Abierto de la Universidad de la República (Res. Nº 16 de C.D.C. de 07/10/2014)es
dc.subjectAntigen Bes
dc.subjectCell bindinges
dc.subjectEchinococcus granulosuses
dc.subjectHLBPes
dc.subjectLipoproteinses
dc.subjectMacrophageses
dc.subjectMonocyteses
dc.titleEchinococcus granulosus Antigen B binds to monocytes and macrophages modulating cell response to inflammationes
dc.typeArtículoes
dc.contributor.filiacionSilva-Álvarez, Valeria. Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológicaes
dc.contributor.filiacionFolle Lopez, Ana Maite. Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológicaes
dc.contributor.filiacionRamos Odella, Ana Lía. Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológicaes
dc.contributor.filiacionFerreira, Ana María. Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológicaes
dc.rights.licenceLicencia Creative Commons Atribución (CC –BY 4.0)es
dc.identifier.doi10.1186/s13071-016-1350-7es
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