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dc.contributor.authorTsanou, E.en
dc.contributor.authorIoachim, E.en
dc.contributor.authorBriassoulis, E. Chen
dc.contributor.authorCharchanti, A.en
dc.contributor.authorDamala, K.en
dc.contributor.authorKaravasilis, V.en
dc.contributor.authorPavlidis, Nicholasen
dc.contributor.authorAgnantis, Niki J.en
dc.creatorTsanou, E.en
dc.creatorIoachim, E.en
dc.creatorBriassoulis, E. Chen
dc.creatorCharchanti, A.en
dc.creatorDamala, K.en
dc.creatorKaravasilis, V.en
dc.creatorPavlidis, Nicholasen
dc.creatorAgnantis, Niki J.en
dc.date.accessioned2018-06-22T09:53:23Z
dc.date.available2018-06-22T09:53:23Z
dc.date.issued2004
dc.identifier.urihttps://gnosis.library.ucy.ac.cy/handle/7/41807
dc.description.abstractSyndecan-1, a cell surface proteoglycan found predominantly on epithelia of mature tissues, binds both extracellular matrix (ECM) components and basic fibroblast growth factor (bFGF) and is implicated in the restriction of growth and invasiveness of neoplastic cells, as it induces the adhesion capacity of neoplastic cells with the stroma. In this study we investigated breast carcinomas for the immunohistochemical expression of syndecan-1 protein and these results were assessed in relation to Clinicopathological parameters, in order to clarify its prognostic value. The possible relationship with hormone receptors content, p53, cell proliferation markers, and extracellular matrix components was also estimated. Tissue sections from 102 breast carcinomas were used and immunostainings were performed on formalin-fixed, paraffin-embedded tissue sections by the labelled streptavidin avidin biotin (LSAB) method. High expression levels were observed, as 75/102 (73.5%) cases expressed immunoreactivity in more than 80% of neoplastic cells, while 67/102 (65.7%) exhibited high staining intensity. The survival analysis showed an increased mortality risk associated with high syndecan-1 staining intensity with borderline significance (p=0.041). In addition, there was a strong negative correlation between syndecan-1 protein expression and ECM, specifically collagen IV (p=0.026) and tenascin (p=0.0067). The results of the present study show the implication of this protein in the remodeling of breast cancer tissue, through the interaction with other extracellular matrix components, probably influences the tumour progression.en
dc.language.isoengen
dc.sourceJournal of Experimental and Clinical Cancer Researchen
dc.subjectArticleen
dc.subjectHumanen
dc.subjectNeoplasmsen
dc.subjectHumansen
dc.subjectBreast neoplasmsen
dc.subjectMajor clinical studyen
dc.subjectCancer growthen
dc.subjectDisease progressionen
dc.subjectPriority journalen
dc.subjectPrognosisen
dc.subjectDisease-free survivalen
dc.subjectHuman tissueen
dc.subjectTime factorsen
dc.subjectNeoplasm metastasisen
dc.subjectCarcinomaen
dc.subjectImmunohistochemistryen
dc.subjectProtein expressionen
dc.subjectProtein p53en
dc.subjectTumor suppressor protein p53en
dc.subjectLymphatic metastasisen
dc.subjectNeoplasm invasivenessen
dc.subjectReceptorsen
dc.subjectBreast canceren
dc.subjectBreast carcinomaen
dc.subjectEstrogen receptoren
dc.subjectProgesterone receptoren
dc.subjectStreptavidinen
dc.subjectKi 67 antigenen
dc.subjectProgesteroneen
dc.subjectCancer invasionen
dc.subjectCohort studiesen
dc.subjectBreasten
dc.subjectTumoren
dc.subjectCell lineen
dc.subjectCell proliferationen
dc.subjectSyndecan 1en
dc.subjectDuctalen
dc.subjectAvidinen
dc.subjectBasement membraneen
dc.subjectBiotinen
dc.subjectCell adhesionen
dc.subjectCell membraneen
dc.subjectCollagen type 1en
dc.subjectCollagen type iven
dc.subjectCorrelation functionen
dc.subjectExtracellular matrixen
dc.subjectFibroblast growth factor 2en
dc.subjectFibronectinen
dc.subjectLamininen
dc.subjectMembrane glycoproteinsen
dc.subjectProteoglycansen
dc.subjectSyndecan-1en
dc.subjectSyndecansen
dc.subjectTenascinen
dc.titleClinicopathological study of the expression of syndecan-1 in invasive breast carcinomas. Correlation with extracellular matrix componentsen
dc.typeinfo:eu-repo/semantics/article
dc.description.volume23
dc.description.issue4
dc.description.startingpage641
dc.description.endingpage650
dc.author.facultyΙατρική Σχολή / Medical School
dc.author.departmentΙατρική Σχολή / Medical School
dc.type.uhtypeArticleen
dc.contributor.orcidPavlidis, Nicholas [0000-0002-2195-9961]
dc.contributor.orcidKaravasilis, V. [0000-0002-5806-9399]
dc.gnosis.orcid0000-0002-2195-9961
dc.gnosis.orcid0000-0002-5806-9399


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