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dc.contributor.authorGarcía Cerro, Susana 
dc.contributor.authorRueda Revilla, Noemí 
dc.contributor.authorVidal Sánchez, Verónica 
dc.contributor.authorPuente Bedia, Alba 
dc.contributor.authorCampa Fernández, Víctor Manuel
dc.contributor.authorLantigua Romero, Sara 
dc.contributor.authorNarcís Majos, Josep Oriol
dc.contributor.authorVelasco, Ana
dc.contributor.authorBartesaghi, Renata
dc.contributor.authorMartínez-Cué, Carmen 
dc.contributor.otherUniversidad de Cantabriaes_ES
dc.date.accessioned2021-04-16T18:23:03Z
dc.date.available2021-06-02T02:45:05Z
dc.date.issued2020-06-01
dc.identifier.issn0022-3166
dc.identifier.issn1541-6100
dc.identifier.otherPSI-2016- 76194-Res_ES
dc.identifier.urihttp://hdl.handle.net/10902/21334
dc.description.abstractBackground: The cognitive impairments that characterize Down syndrome (DS) have been attributed to brain hypocellularity due to neurogenesis impairment during fetal stages. Thus, enhancing prenatal neurogenesis in DS could prevent or reduce some of the neuromorphological and cognitive defects found in postnatal stages. Objectives: As fatty acids play a fundamental role in morphogenesis and brain development during fetal stages, in this study, we aimed to enhance neurogenesis and the cognitive abilities of the Ts65Dn (TS) mouse model of DS by administering oleic or linolenic acid. Methods: In total, 85 pregnant TS females were subcutaneously treated from Embryonic Day (ED) 10 until Postnatal Day (PD) 2 with oleic acid (400 mg/kg), linolenic acid (500 mg/kg), or vehicle. All analyses were performed on their TS and Control (CO) male and female progeny. At PD2, we evaluated the short-term effects of the treatments on neurogenesis, cellularity, and brain weight, in 40 TS and CO pups. A total of 69 TS and CO mice were used to test the long-term effects of the prenatal treatments on cognition from PD30 to PD45, and on neurogenesis, cellularity, and synaptic markers, at PD45. Data were compared by ANOVAs. Results: Prenatal administration of oleic or linolenic acid increased the brain weight (+36.7% and +45%, P < 0.01), the density of BrdU (bromodeoxyuridine)- (+80% and +115%; P < 0.01), and DAPI (4',6-diamidino-2-phenylindole)-positive cells (+64% and +22%, P < 0.05) of PD2 TS mice with respect to the vehicle-treated TS mice. Between PD30 and PD45, TS mice prenatally treated with oleic or linolenic acid showed better cognitive abilities (+28% and +25%, P < 0.01) and a higher density of the postsynaptic marker PSD95 (postsynaptic density protein 95) (+65% and +44%, P < 0.05) than the vehicle-treated TS animals. Conclusion: The beneficial cognitive and neuromorphological effects induced by oleic or linolenic acid in TS mice suggest that they could be promising pharmacotherapies for DS-associated cognitive deficits.es_ES
dc.description.sponsorshipThis study was supported by “Fondazione Generali e Assicurazioni Generali”, Italy; Fundación Tatiana Pérez de Guzmán el Bueno, IDIVAL (NVAL 19/23), and the Spanish Ministry of Economy and Competitiveness (PSI-2016- 76194-R, AEI/FEDER, EU).es_ES
dc.format.extent52 p.es_ES
dc.language.isoenges_ES
dc.publisherOxford University Presses_ES
dc.rights© Oxford University Press. This is a pre-copyedited, author-produced version of an article accepted for publication in The Journal of nutrition following peer review. The version of record J Nutr 2020 Jun 1;150(6):1631-1643 is available online at: https://doi.org/10.1093/jn/nxaa074es_ES
dc.sourceJ Nutr . 2020 Jun 1;150(6):1631-1643es_ES
dc.subject.otherDown Syndromees_ES
dc.subject.otherTs65Dn Micees_ES
dc.subject.otherCognitiones_ES
dc.subject.otherLinolenic Acides_ES
dc.subject.otherNeurogenesises_ES
dc.subject.otherOleic Acides_ES
dc.subject.otherPrenatal Treatmentes_ES
dc.titlePrenatal Administration of Oleic Acid or Linolenic Acid Reduces Neuromorphological and Cognitive Alterations in Ts65dn Down Syndrome Micees_ES
dc.typeinfo:eu-repo/semantics/articlees_ES
dc.relation.publisherVersionhttps://doi.org/10.1093/jn/nxaa074es_ES
dc.rights.accessRightsopenAccesses_ES
dc.identifier.DOI10.1093/jn/nxaa074
dc.type.versionacceptedVersiones_ES
dc.date.embargoEndDate2021-06-02


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