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dc.contributor.authorSánchez Fernández, Alba-
dc.contributor.authorZandee, Stephanie-
dc.contributor.authorMastrogiovanni, Mauricio-
dc.contributor.authorCharabati, Marc-
dc.contributor.authorRubbo, Homero-
dc.contributor.authorPrat, Alexandre-
dc.contributor.authorLópez-Vales, Rubèn-
dc.date.accessioned2026-04-21T16:00:55Z-
dc.date.available2026-04-21T16:00:55Z-
dc.date.issued2022-
dc.identifier.citationSánchez Fernández A, Zandee S, Mastrogiovanni M y otros. Administration of Maresin-1 ameliorates the physiopathology of experimental autoimmune encephalomyelitis. Journal of Neuroinflammation [en línea]. 2022;19(1). 18 p.es
dc.identifier.urihttps://hdl.handle.net/20.500.12008/54515-
dc.description.abstractBackground: Resolution of inflammation is an active and regulated process that leads to the clearance of cell debris and immune cells from the challenged tissue, facilitating the recovery of homeostasis. This physiological response is coordinated by endogenous bioactive lipids known as specialized pro-resolving mediators (SPMs). When resolution fails, inflammation becomes uncontrolled leading chronic inflammation and tissue damage, as occurs in multiple sclerosis (MS). Methods: SPMs and the key biosynthetic enzymes involved in SPM production were analysed by metabololipidomics and qPCR in active brain lesions, serum and peripheral blood mononuclear cells (PBMC) of MS patients as well as in the spinal cord of mice with experimental autoimmune encephalomyelitis (EAE). We also tested the therapeutic actions of the SPM coined Maresin-1 (MaR1) in EAE mice and studied its impact on inflammation by doing luminex and flow cytometry analysis. Results: We show that levels of MaR1 and other SPMs were below the limit of detection or not increased in the spinal cord of EAE mice, whereas the production of pro-inflammatory eicosanoids was induced during disease progression. Similarly, we reveal that SPMs were undetected in serum and active brain lesion samples of MS patients, which was linked to impaired expression of the enzymes involved in the biosynthetic pathways of SPMs. We demonstrate that exogenous administration of MaR1 in EAE mice suppressed the protein levels of various pro-inflammatory cytokines and reduced immune cells counts in the spinal cord and blood. MaR1 also decreased the numbers of Th1 cells but increased the accumulation of regulatory T cells and drove macrophage polarization towards an anti-inflammatory phenotype. Importantly, we provide clear evidence that administration of MaR1 in mice with clinical signs of EAE enhanced neurological outcomes and protected from demyelination. Conclusions: This study reveals that there is an imbalance in the production of SPMs in MS patients and in EAE mice, and that increasing the bioavailability of SPMs, such as MaR1, minimizes inflammation and mediates therapeutic actions. Thus, these data suggest that immunoresolvent therapies, such as MaR1, could be a novel avenue for the treatment of MS.es
dc.format.extent18 p.es
dc.format.mimetypeapplication/pdfes
dc.language.isoenes
dc.publisherBioMed Centrales
dc.relation.ispartofJournal of Neuroinflammation. 2022;19(1)es
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.subjectExperimental autoimmune encephalomyelitises
dc.subjectInflammationes
dc.subjectMaresin-1es
dc.subjectMultiple Sclerosises
dc.subjectResolution of inflammationes
dc.subjectSpecialized pro-resolving mediatorses
dc.subject.otherANTIINFLAMATORIOSes
dc.subject.otherANIMALESes
dc.subject.otherFARMACOLOGÍAes
dc.subject.otherMETABOLISMOes
dc.subject.otherENCEFALOMIELITIS AUTOINMUNE EXPERIMENTALes
dc.subject.otherHUMANOSes
dc.subject.otherINFLAMACIÓNes
dc.subject.otherRATONESes
dc.subject.otherLEUCOCITOS MONONUCLEARESes
dc.subject.otherRATONES ENDOGÁMICOS C57BLes
dc.subject.otherMÉDULA ESPINALes
dc.subject.otherPATOLOGÍA CLÍNICAes
dc.titleAdministration of Maresin-1 ameliorates the physiopathology of experimental autoimmune encephalomyelitises
dc.typeArtículoes
dc.contributor.filiacionSánchez Fernández Alba, Universitat Autonoma de Barcelona (España). Facultat de Medicina. Fisiologia i Immunologia-
dc.contributor.filiacionZandee Stephanie, Université de Montréal (Canadá). Faculté de Médecine. Département de Neurosciences-
dc.contributor.filiacionMastrogiovanni Mauricio, Universidad de la República (Uruguay). Facultad de Medicina. Centro de Investigaciones Biomédicas-
dc.contributor.filiacionCharabati Marc, Université de Montréal (Canadá). Faculté de Médecine. Département de Neurosciences-
dc.contributor.filiacionRubbo Homero, Universidad de la República (Uruguay). Facultad de Medicina. Centro de Investigaciones Biomédicas-
dc.contributor.filiacionPrat Alexandre, Université de Montréal (Canadá). Faculté de Médecine. Département de Neurosciences-
dc.contributor.filiacionLópez-Vales Rubèn, Centro de Investigación Biomédica en Red de Enfermedades Neurodegenerativas (España)-
dc.rights.licenceLicencia Creative Commons Atribución (CC - By 4.0)es
dc.identifier.doi10.1186/s12974-022-02386-1-
dc.identifier.eissn1742-2094-
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