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dc.contributor.authorSwaminathan, Bhairavi
dc.contributor.authorGoikuria Iriondo, Haize
dc.contributor.authorVega, Reyes
dc.contributor.authorRodríguez-Antigüedad Zarranz, Alfredo
dc.contributor.authorLópez Medina, Antonio
dc.contributor.authorFreijo, María del Mar
dc.contributor.authorVandenbroeck, Koen
dc.contributor.authorAlloza Moral, Iraide
dc.date.accessioned2015-10-01T14:05:38Z
dc.date.available2015-10-01T14:05:38Z
dc.date.issued2014-12-12
dc.identifier.citationPLOS ONE 9 (12) : (2014) // Article ID e115176es
dc.identifier.issn1932-6203
dc.identifier.urihttp://hdl.handle.net/10810/15742
dc.description.abstractObjectives: The mechanism by which atheroma plaque becomes unstable is not completely understood to date but analysis of differentially expressed genes in stable versus unstable plaques may provide clues. This will be crucial toward disclosing the mechanistic basis of plaque instability, and may help to identify prognostic biomarkers for ischaemic events. The objective of our study was to identify differences in expression levels of 59 selected genes between symptomatic patients (unstable plaques) and asymptomatic patients (stable plaques). Methods: 80 carotid plaques obtained by carotid endarterectomy and classified as symptomatic (>70% stenosis) or asymptomatic (>80% stenosis) were used in this study. The expression levels of 59 genes were quantified by qPCR on RNA extracted from the carotid plaques obtained by endarterectomy and analyzed by means of various bioinformatic tools. Results: Several genes associated with autophagy pathways displayed differential expression levels between asymptomatic and symptomatic (i.e. MAP1LC3B, RAB24, EVA1A). In particular, mRNA levels of MAP1LC3B, an autophagic marker, showed a 5-fold decrease in symptomatic samples, which was confirmed in protein blots. Immune system-related factors and endoplasmic reticulum-associated markers (i.e. ERP27, ITPR1, ERO1LB, TIMP1, IL12B) emerged as differently expressed genes between asymptomatic and symptomatic patients. Conclusions: Carotid atherosclerotic plaques in which MAP1LC3B is underexpressed would not be able to benefit from MAP1LC3B-associated autophagy. This may lead to accumulation of dead cells at lesion site with subsequent plaque destabilization leading to cerebrovascular events. Identified biomarkers and network interactions may represent novel targets for development of treatments against plaque destabilization and thus for the prevention of cerebrovascular events.es
dc.description.sponsorshiphis work was supported by grants from the Basque Government (Proyectos de Investigacion Sanitaria; ref. 2008111024) (http://www.osasun.ejgv.euskadi.net) and from the Basque Government (Grupos de Investigacion del Sistema Universitario Vasco; ref. IT512-10 (http://www.hezkuntza.ejgv.euskadi.net). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.es
dc.language.isoenges
dc.publisherPublic Library Sciencees
dc.rightsinfo:eu-repo/semantics/openAccesses
dc.subjectendoplasmic-reticulum stresses
dc.subjecttransmembrane proteines
dc.subjectsystematic analysises
dc.subjectvulnerable plaquees
dc.subjectglobal burdenes
dc.subjectdiseasees
dc.subjectHMGB1es
dc.subjectatherogenesises
dc.subjectinflammationes
dc.subjectapoptosises
dc.titleAutophagic Marker MAP1LC3B Expression Levels Are Associated with Carotid Atherosclerosis Symptomatologyes
dc.typeinfo:eu-repo/semantics/articlees
dc.rights.holderß 2014 Swaminathan et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License , which permits unrestricted use, distribution, and repro- duction in any medium, provided the original author and source are credited.es
dc.relation.publisherversionhttp://journals.plos.org/plosone/article?id=10.1371/journal.pone.0115176#abstract0es
dc.identifier.doi10.1371/journal.pone.0115176
dc.departamentoesNeurocienciases_ES
dc.departamentoeuNeurozientziakes_ES
dc.subject.categoriaAGRICULTURAL AND BIOLOGICAL SCIENCES
dc.subject.categoriaBIOCHEMISTRY AND MOLECULAR BIOLOGY
dc.subject.categoriaMEDICINE


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