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dc.contributor.authorMadeira, Ana
dc.contributor.authorSerena, Carolina
dc.contributor.authorEjarque, Miriam
dc.contributor.authorMaymó-Masip, Elsa
dc.contributor.authorMillán, Mónica
dc.contributor.authorNavarro-Ruiz, Carmen
dc.contributor.authorGuzmán Ruiz, R.
dc.contributor.authorMalagón, María M.
dc.contributor.authorEspin, Eloy
dc.contributor.authorMartí, Marc
dc.contributor.authorMenacho, Margarita
dc.contributor.authorMegía, Ana
dc.contributor.authorVendrell, Joan
dc.contributor.authorFernández-Veledo, Sonia
dc.date.accessioned2021-04-21T09:19:14Z
dc.date.available2021-04-21T09:19:14Z
dc.date.issued2021
dc.identifier.urihttp://hdl.handle.net/10396/21287
dc.description.abstractOur understanding of the interplay between human adipose tissue and the immune system is limited. The mesothelium, an immunologically active structure, emerged as a source of visceral adipose tissue. After investigating the mesothelial properties of human visceral and subcutaneous adipose tissue and their progenitors, we explored whether the dysfunctional obese and Crohn’s disease environments influence the mesothelial/mesenchymal properties of their adipocyte precursors, as well as their ability to mount an immune response. Using a tandem transcriptomic/proteomic approach, we evaluated the mesothelial and mesenchymal expression profiles in adipose tissue, both in subjects covering a wide range of body-mass indexes and in Crohn’s disease patients. We also isolated adipose tissue precursors (adipose-derived stem cells, ASCs) to assess their mesothelial/mesenchymal properties, as well as their antigen-presenting features. Human visceral tissue presented a mesothelial phenotype not detected in the subcutaneous fat. Only ASCs from mesenteric adipose tissue, named creeping fat, had a significantly higher expression of the hallmark mesothelial genes mesothelin (MSLN) and Wilms’ tumor suppressor gene 1 (WT1), supporting a mesothelial nature of these cells. Both lean and Crohn’s disease visceral ASCs expressed equivalent surface percentages of the antigen-presenting molecules human leucocyte antigen—DR isotype (HLA-DR) and CD86. However, lean-derived ASCs were predominantly HLA-DR dim, whereas in Crohn’s disease, the HLA-DR bright subpopulation was increased 3.2-fold. Importantly, the mesothelial-enriched Crohn’s disease precursors activated CD4+ T-lymphocytes. Our study evidences a mesothelial signature in the creeping fat of Crohn’s disease patients and its progenitor cells, the latter being able to present antigens and orchestrate an immune response.es_ES
dc.format.mimetypeapplication/pdfes_ES
dc.language.isoenges_ES
dc.publisherMDPIes_ES
dc.rightshttps://creativecommons.org/licenses/by/4.0/es_ES
dc.sourceInternational Journal of Molecular Sciences 22(8), 4292 (2021)es_ES
dc.subjectCrohn’s diseasees_ES
dc.subjectAdipose tissuees_ES
dc.subjectMesotheliumes_ES
dc.subjectAdipose-derived stem cellses_ES
dc.titleCrohn’s Disease Increases the Mesothelial Properties of Adipocyte Progenitors in the Creeping Fates_ES
dc.typeinfo:eu-repo/semantics/articlees_ES
dc.relation.publisherversionhttp://dx.doi.org/10.3390/ijms22084292es_ES
dc.relation.projectIDGobierno de España. PI14/00228es_ES
dc.relation.projectIDGobierno de España. PI17/01503es_ES
dc.relation.projectIDGobierno de España. SAF2015-65019-Res_ES
dc.relation.projectIDGobierno de España. BFU2015-70454- REDTes_ES
dc.relation.projectIDGobierno de España. BFU2017-90578-REDTes_ES
dc.relation.projectIDGobierno de España. BFU2016-76711-Res_ES
dc.relation.projectIDGobierno de España. PI15/00143es_ES
dc.relation.projectIDGobierno de España. PI18/00037es_ES
dc.relation.projectIDInstituto de Salud Carlos III. CB07708/0012es_ES
dc.relation.projectIDGobierno de España. FJCI-2014-23060es_ES
dc.relation.projectIDGobierno de España. IJCI-2016-30572es_ES
dc.relation.projectIDInstituto de Salud Carlos III. CP10/00438es_ES
dc.relation.projectIDInstituto de Salud Carlos III. CPII16/00008es_ES
dc.relation.projectIDGobierno de España. RYC2013-13186es_ES
dc.rights.accessRightsinfo:eu-repo/semantics/openAccesses_ES


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