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Tytuł pozycji:

Gene expression and immunohistochemical analyses identify SOX2 as major risk factor for overall survival and relapse in Ewing sarcoma patientsResearch in context

Tytuł:
Gene expression and immunohistochemical analyses identify SOX2 as major risk factor for overall survival and relapse in Ewing sarcoma patientsResearch in context
Autorzy:
Giuseppina Sannino
Aruna Marchetto
Andreas Ranft
Susanne Jabar
Constanze Zacherl
Rebeca Alba-Rubio
Stefanie Stein
Fabienne S. Wehweck
Merve M. Kiran
Tilman L.B. Hölting
Julian Musa
Laura Romero-Pérez
Florencia Cidre-Aranaz
Maximilian M.L. Knott
Jing Li
Heribert Jürgens
Ana Sastre
Javier Alonso
Willian Da Silveira
Gary Hardiman
Julia S. Gerke
Martin F. Orth
Wolfgang Hartmann
Thomas Kirchner
Shunya Ohmura
Uta Dirksen
Thomas G.P. Grünewald
Temat:
Medicine
Medicine (General)
R5-920
Źródło:
EBioMedicine, Vol 47, Iss , Pp 156-162 (2019)
Wydawca:
Elsevier, 2019.
Rok publikacji:
2019
Kolekcja:
LCC:Medicine
LCC:Medicine (General)
Typ dokumentu:
article
Opis pliku:
electronic resource
Język:
English
ISSN:
2352-3964
Relacje:
http://www.sciencedirect.com/science/article/pii/S2352396419305183; https://doaj.org/toc/2352-3964
DOI:
10.1016/j.ebiom.2019.08.002
Dostęp URL:
https://doaj.org/article/519688e9d40c4215ae075d85d43e55cd  Link otwiera się w nowym oknie
Numer akcesji:
edsdoj.519688e9d40c4215ae075d85d43e55cd
Czasopismo naukowe
Background: Up to 30–40% of Ewing sarcoma (EwS) patients with non-metastatic disease develop local or metastatic relapse within a time span of 2–10 years. This is in part caused by the absence of prognostic biomarkers that can identify high-risk patients and thus assign them to risk-adapted monitoring and treatment regimens. Since cancer stemness has been associated with tumour relapse and poor patient outcomes, we investigated in the current study the prognostic potential SOX2 (sex determining region Y box 2) – a major transcription factor involved in development and stemness – which was previously described to contribute to the undifferentiated phenotype of EwS. Methods: Two independent patient cohorts, one consisting of 189 retrospectively collected EwS tumours with corresponding mRNA expression data (test-cohort) and the other consisting of 141 prospectively collected formalin-fixed and paraffin-embedded resected tumours (validation and cohort), were employed to analyse SOX2 expression levels through DNA microarrays or immunohistochemistry, respectively, and to compare them with clinical parameters and patient outcomes. Two methods were employed to test the validity of the results at both the mRNA and protein levels. Findings: Both cohorts showed that only a subset of EwS patients (16–20%) expressed high SOX2 mRNA or protein levels, which significantly correlated with poor overall survival. Multivariate analyses of our validation-cohort revealed that high SOX2 expression represents a major risk-factor for poor survival (HR = 3·19; 95%CI 1·74–5·84; p

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