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dc.contributor.authorGonzalez Fernandez, Raquel
dc.date.accessioned2021-07-28T19:52:37Z
dc.date.available2021-07-28T19:52:37Z
dc.date.issued2021-05-19es_MX
dc.identifier.urihttp://cathi.uacj.mx/20.500.11961/18600
dc.description.abstractBackground: Chronic psychological distress is considered today a pandemic due to the modern lifestyle and has been associated with various neurodegenerative, autoimmune, or systemic inflammation-related diseases. Stress is closely related to liver disease exacerbation through the high activity of the endocrine and autonomic nervous systems, and the connection between the development of these pathologies and the physiological effects induced by oxidative stress is not yet completely understood. The use of nootropics, as the cognitive enhancer and antioxidant piracetam, is attractive to repair the oxidative damage. A proteomic approach provides the possibility to obtain an in-depth comprehension of the affected cellular processes and the possible consequences for the body. Therefore, we considered to describe the effect of distress and piracetam on the liver proteome. Methods: We used a murine model of psychological stress by predatory odor as a distress paradigm. Female Sprague-Dawley rats were distributed into four experimental groups (n = 6 - 7/group) and were exposed or not to the stressor for five days and treated or not with piracetam (600 mg/kg) for six days. We evaluated the liver proteome by one-dimensional sodium dodecyl sulfate-polyacrylamide gel electrophoresis (1D-SDS-PAGE) followed by liquid chromatography-tandem mass spectrometry (GeLC-MS/MS). Besides, we analyzed the activity of liver antioxidant enzymes, the biochemical parameters in plasma and rat behavior. Results: Our results showed that distress altered a wide range of proteins involved in amino acids metabolism, glucose, and fatty acid mobilization and degradation on the way to produce energy, protein folding, trafficking and degradation, redox metabolism, and its implications in the development of the non-alcoholic fatty liver disease (NAFLD). Piracetam reverted the changes in metabolism caused by distress exposure, and, under physiological conditions, it increased catabolism rate directed towards energy production. These results confirm the possible relationship between chronic psychological stress and the progression of NAFLD, as well as we newly evidenced the controversial beneficial effects of piracetam. Finally, we propose new distress biomarkers in the liver as the protein DJ-1 (PARK7), glutathione peroxidase 1 (GPX), peroxiredoxin-5 (PRDX5), glutaredoxin 5 (GLRX5), and thioredoxin reductase 1 (TXNDR1), and in plasma as biochemical parameters related to kidney function such as urea and blood urea nitrogen (BUN) levels.es_MX
dc.description.urihttps://peerj.com/articles/11483/es_MX
dc.language.isoenes_MX
dc.relation.ispartofProducto de investigación ICBes_MX
dc.relation.ispartofInstituto de Ciencias Biomédicases_MX
dc.subjectDistresses_MX
dc.subjectEmotional stresses_MX
dc.subjectLiver proteomees_MX
dc.subjectNAFLDes_MX
dc.subjectNootropicses_MX
dc.subjectRedox enzymeses_MX
dc.subject.otherinfo:eu-repo/classification/cti/2es_MX
dc.titleLiver proteome alterations in psychologically distressed rats and a nootropic druges_MX
dc.typeArtículoes_MX
dcterms.thumbnailhttp://ri.uacj.mx/vufind/thumbnails/rupiicb.pnges_MX
dcrupi.institutoInstituto de Ciencias Biomédicases_MX
dcrupi.cosechableSies_MX
dcrupi.volumen2021es_MX
dcrupi.nopagina1-32es_MX
dc.identifier.doi10.7717/peerj.11483es_MX
dc.contributor.coauthorValero Galván, José
dc.contributor.coauthorMartinez-Martinez, Alejandro
dc.contributor.alumno124778es_MX
dc.contributor.alumno160376es_MX
dc.journal.titlePeerJes_MX
dc.lgacESTRÉS METABÓLICO: DISEÑO, SÍNTESIS Y EVALUACIÓN DE FÁRMACOS NOOTRÓPICOSes_MX
dc.cuerpoacademicoBioquímica Funcional y Proteómica del Estréses_MX
dc.contributor.coauthorexternoRuiz-May, Eliel
dc.contributor.coauthorexternoElizalde-Contreras, José Miguel
dc.contributor.coauthorexternoGrigoruta, Mariana
dc.contributor.coauthorexternoChavezz-Martínez, Sarahi


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