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dc.contributor.otherGrupo de Metabolismo y Función Vascular (MET-VASC)-
dc.contributor.otherUniversidad San Pablo-CEU. Facultad de Farmacia-
dc.creatorGonzález Blázquez, Raquel-
dc.creatorAlcalá Díaz-Mor, Martín-
dc.creatorFernández Alfonso, María Soledad-
dc.creatorMuscha Steckelings, Ulrike-
dc.creatorLorenzo García, María Paz-
dc.creatorViana Arribas, Marta-
dc.creatorBoisvert, William A.-
dc.creatorUnger, Thomas-
dc.creatorGil Ortega, Marta-
dc.creatorSomoza Hernández, Beatriz-
dc.date.accessioned2023-12-04T11:49:35Z-
dc.date.available2023-12-04T11:49:35Z-
dc.date.issued2021-05-11-
dc.identifier.citationRaquel González-Blázquez, Martín Alcalá, María S. Fernández-Alfonso, Ulrike Muscha Steckelings, M. Paz Lorenzo, Marta Viana, William A. Boisvert, Thomas Unger, Marta Gil-Ortega, Beatriz Somoza; C21 preserves endothelial function in the thoracic aorta from DIO mice: role for AT2, Mas and B2 receptors. Clin Sci (Lond) 14 May 2021; 135 (9): 1145–1163. doi: https://doi.org/10.1042/CS20210049es_ES
dc.identifier.issn1470-8736-
dc.identifier.urihttp://hdl.handle.net/10637/14694-
dc.descriptionEste artículo es la versión preprint, siguiendo la política de acceso abierto de la editorial Portland Presses_ES
dc.description.abstractCompound 21 (C21), a selective agonist of angiotensin type 2 receptor (AT2R), induces vasodilation through NO release. Since AT2R seems to be overexpressed in obesity, we hypothesize that C21 prevents the development of obesity-related vascular alterations. The main goal of this study was to assess the effect of C21on thoracic aorta endothelial function in a model of diet-induced obesity and to elucidate the potential crosstalk between AT2R, MasR and/or B2R in this response. 5-week-old male C57BL6J mice were fed a standard (CHOW) or a high-fat diet (HF) for 6 weeks and treated daily with C21 (1mg/Kg p.o) or vehicle, generating four groups: CHOW-C, CHOW-C21, HF-C, HF-C21. Vascular reactivity experiments were performed in thoracic aorta rings. Human endothelial cells (EA.hy926) were used to elucidate the signaling pathways, both at receptor and intracellular levels. Arteries from HF mice exhibited increased contractions to Ang II than CHOW mice, effect that was prevented by C21. PD123177, A779 and HOE-140 (AT2R, Mas and B2R antagonists) significantly enhanced Ang II-induced contractions in CHOW but not in HF-C rings, suggesting a lack of functionality of those receptors in obesity. C21 prevented those alterations and favoured the formation of AT2R/MasR and MasR/B2R heterodimers. HF mice also exhibited impaired relaxations to acetylcholine due to a reduced NO availability. C21 preserved NO release through PKA/p-eNOS and AKT/peNOS signaling pathways. In conclusion, C21 favours the interaction between AT2R, MasR and B2R and prevents the development of obesity-induced endothelial dysfunction by stimulating NO release through PKA/p-eNOS and AKT/p-eNOS signaling pathways.es_ES
dc.formatapplication/pdf-
dc.language.isoenes_ES
dc.publisherPortland Presses_ES
dc.relation.ispartofClinical Science-
dc.rightshttp://creativecommons.org/licenses/by-nc-nd/4.0/deed.es-
dc.subjectCompound 21es_ES
dc.subjectNitric oxidees_ES
dc.subjectAngiotensin II type 2 receptores_ES
dc.subjectMas receptores_ES
dc.subjectBradykinin type 2 receptores_ES
dc.subjectDiet-induced obesityes_ES
dc.titleC21 preserves endothelial function in the thoracic aorta from DIO mice: role for AT2, Mas and B2 receptorses_ES
dc.typeArtículoes_ES
dc.identifier.doi10.1042/CS20210049-
dc.centroUniversidad San Pablo-CEU-
Aparece en las colecciones: Facultad de Farmacia




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