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dc.contributorWileyes_CL
dc.contributor.authorGonzález, Sergio Miguel [Chile. Universidad Mayor. Facultad de Odontología]es_CL
dc.contributor.authorAguilera, Sergio [s.af]es_CL
dc.contributor.authorAlliende, Cecilia [s.af]es_CL
dc.contributor.authorUrzúa, Ulises [Universidad de Chile. Facultad de Medicina]es_CL
dc.contributor.authorQuest, Andrew FG [Universidad de Chile. Facultad de Medicina]es_CL
dc.contributor.authorHerrera, Luisa [s.af]es_CL
dc.contributor.authorHermoso, Marcela A. [Universidad de Chile. Facultad de Medicina]es_CL
dc.contributor.authorBrito, Mónica [Chile. Universidad Mayor. Escuela de Tecnología Médica]es_CL
dc.contributor.authorLeyton, Cecilia [s.af]es_CL
dc.contributor.authorGonzález, María Julieta [s.af]es_CL
dc.contributor.authorPérez, Paola Jacqueline [National Institutes of Health]es_CL
dc.contributor.authorEwert, Patriciaes_CL
dc.contributor.authorMolina, Claudio [Chile. Universidad San Sebastián]es_CL
dc.contributor.authorRomo, Rafael [s.af]es_CL
dc.date.accessioned2018-08-23T00:20:58Z
dc.date.available2018-08-23T00:20:58Z
dc.date.issued2011es_CL
dc.identifier.citationGonzález S, Aguilera S, Alliende C, Urzúa U, Quest A, Herrera L, Leyton C, Molina C, Hermoso M, Ewert P, Brito M, Romo R, González M, Pérez P. Alterations in Type I Hemidesmosome Components Suggestive of Epigenetic Control in the Salivary Glands of Patients With Sjögren’s Syndrome [Internet]. Santiago, Chile: Universidad de Chile - ; 2011-04 [citado: 2018, agosto]. Disponible en: http://www.repositorio.uchile.cl/handle/2250/128889Ces_CL
dc.identifier.issnISSN: 0004-3591es_CL
dc.identifier.issnESSN 1529-0131es_CL
dc.identifier.urihttp://repositorio.umayor.cl/xmlui/handle/sibum/2496
dc.identifier.urihttps://onlinelibrary.wiley.com/doi/epdf/10.1002/art.30212es_CL
dc.identifier.urihttp://dx.doi.org/10.1002/art.30212es_CL
dc.description.abstractObjective. Acinar cells in the salivary glands of patients with Sjo¨gren’s syndrome (SS) display severe alterations in anchorage to the basal lamina. Bioinformatics analysis of the BP230 gene sequence has revealed the presence of CpG islands that might be involved in epigenetic control of gene expression, and methylation of the BP230 promotor region may be implicated as an epigenetic control mechanism in salivary gland damage. Thus, the present study was undertaken to evaluate the protein BP230, as well as proteins BP180, 6 4 integrin, and cytokeratin-18, for their expression levels, localization, and ability to form hemidesmosome adhesion complexes. Methods. Eighteen patients with primary SS and 14 healthy control subjects were studied. Levels of messenger RNA (mRNA) and protein were measured by reverse transcription–polymerase chain reaction and Western blotting, respectively. BP230 methylation was determined by methylation-sensitive polymerase chain reaction. Protein complexes were analyzed by immunoprecipitation and assessed for localization by immunofluorescence. Results. In patients with SS as compared with controls, BP230 mRNA levels were decreased while protein levels were increased, and the gene promotor region was hypermethylated. Augmented proteolysis of BP180 was detected, since levels of linear IgA disease fragment 1 were increased. The complex-forming ability of BP230, BP180, 6 4 integrin, and cytokeratin-18 was maintained in patients with SS, in contrast to that in controls. BP230 and BP180 colocalized at the basal membrane of acinar cells, and cleavage of BP180 coincided with a loss of colocalization. Conclusion. The decrease in BP230 mRNA levels may be explained by gene hypermethylation. We postulate that local epigenetic modifications of BP230 are produced in response to factors present in the damaged salivary glands of patients with SS. Additionally, the paradoxical increase in BP230 protein levels and the formation of both normal and altered adhesion complexes may help avoid cell death induced by the loss of anchorage.es_CL
dc.description.sponsorshipEste trabajo fue financiado por: Fondo Nacional de Desarrollo Científico y Tecnológico (FONDECYT-CHILE grants 1080006 and 1050192) y (FONDAP program grant 15010006).es_CL
dc.format.extentARTÍCULO ORIGINALes_CL
dc.language.isoenes_CL
dc.publisherFacultad de Cienciases_CL
dc.rightsAttribution-NonCommercial-NoDerivs 3.0 Chilees_CL
dc.subjectCIENCIAS DE LA SALUDes_CL
dc.titleAlterations in type i hemidesmosome components suggestive of epigenetic control in the salivary glands of patients with Sjogren's syndromees_CL
dc.typeArtículo o Paperes_CL
umayor.indizadorCOTes_CL
umayor.politicas.sherpa/romeoLicencia color: AMARILLO (Puede archivar el pre-print (ie la versión previa a la revisión por pares)) --Pre-print del autor: el autor puede archivar la versión pre-print (ie la versión previa a la revisión por pares) Post-print del autor: el autor puede archivar la versión post-print (ie la versión final posterior a la revisión por pares) siempre que se cumplan las restricciones: 12 months embargo for scientific, technical and medicine titles, 2 years embargo for humanities and social science titles Versión de editor/PDF: el autor no puede archivar la versión del editor/PDF. Condiciones generales: Algunas revistas tienen políticas independientes, consultar directamente con cada revista, On author's personal website, institutional repositories, arXiv, AgEcon, PhilPapers, PubMed Central, RePEc or Social Science Research Network, Author's pre-print may not be updated with Publisher's Version/PDF, Author's pre-print must acknowledge acceptance for publication, En un servidor sin ánimo de lucro, La versión de editor/PDF no puede utilizarse, Debe reconocerse la fuente de publicación con la cita, Must link to publisher version with set statement (see policy), If OnlineOpen is available, BBSRC, EPSRC, MRC, NERC and STFC authors, may self-archive after 12 months, If OnlineOpen is not available, BBSRC, EPSRC, MRC, NERC and STFC authors, may self-archive after 6 months, If OnlineOpen is available, AHRC and ESRC authors, may self-archive after 24 months, If OnlineOpen is not available, AHRC and ESRC authors, may self-archive after 12 monthses_CL
umayor.indexadoSCOPUSes_CL
dc.identifier.doi10.1002/art.30212es_CL]


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