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dc.contributor.author Ugalde, Valentina
dc.contributor.author Contreras, Francisco
dc.contributor.author Prado, Carolina
dc.contributor.author Chovar, Ornella
dc.contributor.author Espinoza, Alexandra
dc.contributor.author Pacheco, Rodrigo
dc.date.accessioned 2024-09-26T00:26:44Z
dc.date.available 2024-09-26T00:26:44Z
dc.date.issued 2021-05
dc.identifier.issn 1933-0219
dc.identifier.uri https://repositorio.uss.cl/handle/uss/12169
dc.description Publisher Copyright: © 2020, Society for Mucosal Immunology.
dc.description.abstract Evidence from inflammatory bowel diseases (IBD) patients and animal models has indicated that gut inflammation is driven by effector CD4+ T-cell, including Th1 and Th17. Conversely, Treg seem to be dysfunctional in IBD. Importantly, dopamine, which is abundant in the gut mucosa under homoeostasis, undergoes a sharp reduction upon intestinal inflammation. Here we analysed the role of the high-affinity dopamine receptor D3 (DRD3) in gut inflammation. Our results show that Drd3 deficiency confers a stronger immunosuppressive potency to Treg, attenuating inflammatory colitis manifestation in mice. Mechanistic analyses indicated that DRD3-signalling attenuates IL-10 production and limits the acquisition of gut-tropism. Accordingly, the ex vivo transduction of wild-type Treg with a siRNA for Drd3 induced a potent therapeutic effect abolishing gut inflammation. Thus, our findings show DRD3-signalling as a major regulator of Treg upon gut inflammation. [Figure not available: see fulltext.] en
dc.language.iso eng
dc.relation.ispartof vol. 14 Issue: no. 3 Pages: 652-666
dc.source Mucosal Immunology
dc.title Dopaminergic signalling limits suppressive activity and gut homing of regulatory T cells upon intestinal inflammation en
dc.type Artículo
dc.identifier.doi 10.1038/s41385-020-00354-7
dc.publisher.department Facultad de Medicina y Ciencia


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