Efficient T‐cell priming and activation requires signaling through prostaglandin E2 (EP) receptors

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dc.contributor.authorSreeramkumar, Vinatha
dc.contributor.authorHons, Miroslav
dc.contributor.authorPunzón, Carmen
dc.contributor.authorStein, Jens V.
dc.contributor.authorSancho, David
dc.contributor.authorFresno, Manuel
dc.contributor.authorCuesta Rubio, Natalia
dc.date.accessioned2019-10-09T14:43:38Z
dc.date.available2019-10-09T14:43:38Z
dc.date.issued2016
dc.description.abstractUnderstanding the regulation of T-cell responses during inflammation and auto-immunity is fundamental for designing efficient therapeutic strategies against immune diseases. In this regard, prostaglandin E2 (PGE2) is mostly considered a myeloid-derived immunosuppressive molecule. We describe for the first time that T cells secrete PGE2 during T-cell receptor stimulation. In addition, we show that autocrine PGE2 signaling through EP receptors is essential for optimal CD4(+) T-cell activation in vitro and in vivo, and for T helper 1 (Th1) and regulatory T cell differentiation. PGE2 was found to provide additive co-stimulatory signaling through AKT activation. Intravital multiphoton microscopy showed that triggering EP receptors in T cells is also essential for the stability of T cell-dendritic cell (DC) interactions and Th-cell accumulation in draining lymph nodes (LNs) during inflammation. We further demonstrated that blocking EP receptors in T cells during the initial phase of collagen-induced arthritis in mice resulted in a reduction of clinical arthritis. This could be attributable to defective T-cell activation, accompanied by a decline in activated and interferon-γ-producing CD4(+) Th1 cells in draining LNs. In conclusion, we prove that T lymphocytes secret picomolar concentrations of PGE2, which in turn provide additive co-stimulatory signaling, enabling T cells to attain a favorable activation threshold. PGE2 signaling in T cells is also required for maintaining long and stable interactions with DCs within LNs. Blockade of EP receptors in vivo impairs T-cell activation and development of T cell-mediated inflammatory responses. This may have implications in various pathophysiological settings.spa
dc.description.filiationUEMspa
dc.description.impact4.557 JCR (2016) Q2, 57/190 Cell Biology, 39/151 Immunologyspa
dc.description.sponsorshipSin financiaciónspa
dc.identifier.citationSreeramkumar, V., Hons, M., Punzón, C., Stein, J. V., Sancho, D., Fresno, M., & Cuesta, N. (2016). Efficient T‐cell priming and activation requires signaling through prostaglandin E2 (EP) receptors. Immunology and Cell Biology, 94(1), 39-51. https://doi.org/10.1038/icb.2015.62spa
dc.identifier.doi10.1038/icb.2015.62
dc.identifier.issn0818-9641
dc.identifier.issn1440-1711
dc.identifier.urihttp://hdl.handle.net/11268/8316
dc.language.isoengspa
dc.peerreviewedSispa
dc.rights.accessRightsrestricted accessspa
dc.subject.uemLinfocitos Tspa
dc.subject.uemProstaglandinasspa
dc.subject.unescoBiología celularspa
dc.subject.unescoLucha contra las enfermedadesspa
dc.titleEfficient T‐cell priming and activation requires signaling through prostaglandin E2 (EP) receptorsspa
dc.typejournal articlespa
dspace.entity.typePublication
relation.isAuthorOfPublicationc22eded3-8c34-4a25-9028-cb562fbc3a62
relation.isAuthorOfPublication23e27743-6319-4aee-86a9-20de8bdafc98
relation.isAuthorOfPublication.latestForDiscoveryc22eded3-8c34-4a25-9028-cb562fbc3a62

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