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dc.contributor.authorSuárez-Martins, Mariana-
dc.contributor.authorGonzález-Alayón, Ignacio-
dc.contributor.authorCasaravilla, Cecilia-
dc.contributor.authorBoon, Louis-
dc.contributor.authorPapotto, Pedro H.-
dc.contributor.authorFinlay, Conor M.-
dc.contributor.authorJenkins, Stephen J.-
dc.contributor.authorAllen, Judith E.-
dc.contributor.authorDíaz, Álvaro-
dc.date.accessioned2025-12-15T20:09:12Z-
dc.date.available2025-12-15T20:09:12Z-
dc.date.issued2025-
dc.identifier.citationSuárez-Martins, M., González-Alayón, I., Casaravilla, C. y otros. "Macrophage IL-4 polarization is restricted by soluble CD40 agonists and antigen-induced CD154 but not by constitutive CD154 expressed by CD4+ T cells" [Preprint]. Journal of Leukocyte Biology [en línea] v. 117, n°7, 2025. -- eqiaf069. 75 p.es
dc.identifier.urihttps://hdl.handle.net/20.500.12008/52982-
dc.description.abstractStimulation of macrophages via CD40 promotes their classical activation. Therefore, CD154 (CD40 ligand) can be expected to oppose macrophage polarization and proliferation induced by IL-4. However, there is limited experimental data to support this, which is additionally complicated by the possibility of differential effects of CD40 agonists in different formats/contexts. Whereas canonically CD4+ T cells upregulate CD154 strongly following exposure to cognate antigen, naïve CD4+ cells constitutively express significant levels of CD154, which could be a tonic signal. Soluble CD154 and agonistic CD40 antibodies also trigger CD40 signaling. We explored these questions in a reductionist model of IL-4 delivery to mouse peritoneal cavity cells in vitro and in vivo. Soluble CD40 agonists inhibited M(IL-4) polarization, with a stronger effect on RELMa than on Ym1 (Chil3), as well as inhibiting IL-4 induced proliferation. CD154 provided by CD4+ cells in the context of an antigen-specific interaction blunted macrophage RELM-a expression but did not affect Ym1. Macrophages negatively regulated, via CD40, constitutive cell-surface CD154 on naïve CD4+ cells, both in vitro and in vivo. The large peritoneal macrophages of CD40 KO mice showed a moderately enhanced RELMa response to IL-4, but this was not a cell-autonomous effect. No differences between WT and CD40 KO mice were detected in IL-4-induced macrophage proliferation. We conclude that strong CD40 stimulation, included stimulation by CD154 expressed by antigen-specific CD4+ cells, blunts selected macrophage responses to IL-4, and that constitutive CD4+-cell CD154, in spite of interacting with CD40 on macrophages, does not directly influence macrophage responses to IL-4.es
dc.format.extent75 p.es
dc.format.mimetypeapplication/pdfes
dc.language.isoenes
dc.publisherOxford University Presses
dc.relation.isformatofPDFes
dc.relation.ispartofJournal of Leukocyte Biology, v. 117, n°7, 2025. -- eqiaf069es
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.subjectCD40es
dc.subjectCD154es
dc.subjectMacrófagoes
dc.subjectCavidad peritoneales
dc.titleMacrophage IL-4 polarization is restricted by soluble CD40 agonists and antigen-induced CD154 but not by constitutive CD154 expressed by CD4+ T cellses
dc.typePreprintes
dc.contributor.filiacionSuárez-Martins Mariana, Universidad de la República (Uruguay). Facultad de Química. Departamento de Biociencias. Área Inmunología and Facultad de Ciencias. Instituto de Química Biológica. Cátedra de Inmunología-
dc.contributor.filiacionGonzález-Alayón Ignacio, Universidad de la República (Uruguay). Facultad de Química. Departamento de Biociencias. Área Inmunología and Facultad de Ciencias. Instituto de Química Biológica. Cátedra de Inmunología-
dc.contributor.filiacionCasaravilla Cecilia, Universidad de la República (Uruguay). Facultad de Química. Departamento de Biociencias. Área Inmunología and Facultad de Ciencias. Instituto de Química Biológica. Cátedra de Inmunología-
dc.contributor.filiacionBoon Louis, JJP Biologics (Poland)-
dc.contributor.filiacionPapotto Pedro H., University of Manchester (UK). Faculty of Biology Medicine and Health. School of Biological Sciences. Lydia Becker Institute of Immunology and Inflammation-
dc.contributor.filiacionFinlay Conor M., University of Manchester (UK). Faculty of Biology Medicine and Health. School of Biological Sciences. Lydia Becker Institute of Immunology and Inflammation; Trinity College Dublin (Ireland). School of Medicine. Trinity Translational Medicine Institute. Trinity Kidney Centre-
dc.contributor.filiacionJenkins Stephen J., University of Edinburgh (UK). Institute for Regeneration and Repair. Centre for Inflammation Research-
dc.contributor.filiacionAllen Judith E., University of Manchester (UK). Faculty of Biology Medicine and Health. School of Biological Sciences. Lydia Becker Institute of Immunology and Inflammation-
dc.contributor.filiacionDíaz Álvaro, Universidad de la República (Uruguay). Facultad de Química. Departamento de Biociencias. Área Inmunología and Facultad de Ciencias. Instituto de Química Biológica. Cátedra de Inmunología-
dc.rights.licenceLicencia Creative Commons Atribución - No Comercial - Sin Derivadas (CC - By-NC-ND 4.0)es
dc.identifier.doi10.1093/jleuko/qiaf069-
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