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      Sox11 expression in astrocytic gliomas: correlation with nestin/c-Met/IDH1-R132H expression phenotypes, p-Stat-3 and survival

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          Abstract

          Background:

          Sox11 is a transcription factor expressed in foetal and neoplastic brain tissue, including gliomas. It has been shown to suppress the tumourigenicity of glioma stem cells in vivo, thereby being hypothesised to function as a tumour suppressor.

          Methods:

          We investigated the expression of Sox11 in 132 diffuse astrocytomas in relation to the regulator cell marker nestin, c-Met and IDH1-R132H, which have shown to be differentially expressed among the molecular subgroups of malignant gliomas, as well as to an inducer of astrocytic differentiation, that is, signal transducer and activator of transcription (p-STAT-3), clinicopathological features and survival.

          Results:

          Sox11 immunoreactivity was identified in all tumours irrespective of grade, but being correlated with p-STAT-3. Three out of seven cases showed partial Sox11 promoter methylation. In >50% of our cases neoplastic cells coexpressed Sox11 and nestin, a finding further confirmed in primary glioblastoma cell cultures. Furthermore, nestin, c-Met and IDH1-R132H expression differed among grade categories. Cluster analysis identified four groups of patients according to c-Met, nestin and IDH1-R132H expression. The c-Met/nestin high-expressor group displayed a higher Sox11 expression. Sox11 expression was an indicator of favourable prognosis in glioblastomas, which remained in multivariate analysis and validated in an independent set of 72 cases. The c-Met/nestin high-expressor group was marginally with shorter survival in univariate analysis.

          Conclusions:

          We highlight the importance of Sox11 expression as a favourable prognosticator in glioblastomas. c-Met/nestin/IDH1-R132H expression phenotypes recapitulate the molecular subgroups of malignant glioma.

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          Author and article information

          Journal
          Br J Cancer
          Br. J. Cancer
          British Journal of Cancer
          Nature Publishing Group
          0007-0920
          1532-1827
          28 May 2013
          25 April 2013
          : 108
          : 10
          : 2142-2152
          Affiliations
          [1 ]First Department of Pathology, Laikon General Hospital, Athens University Medical School , Athens, 115 27, Greece
          [2 ]Department of Biological Chemistry, Athens University Medical School , Athens, 115 27, Greece
          [3 ]Department of Neurosurgery, Medical School, National and Kapodistrian University of Athens, Evangelismos Hospital , Athens, 106 76, Greece
          [4 ]Department of Pathology, Metropolitan Hospital , Athens, 185 47, Greece
          [5 ]Department of Neurosurgery, Metropolitan Hospital , Athens 185 47, Greece
          [6 ]Department of Pathology, Red Cross Hospital , Athens, 115 26, Greece
          [7 ]Department of Neurosurgery, Red Cross Hospital , Athens 115 26, Greece
          Author notes
          [8]

          These authors contributed equally to this work.

          Article
          bjc2013176
          10.1038/bjc.2013.176
          3670505
          23619925
          0b2e9bfb-6f12-404a-8015-0ed1bfa318fe
          Copyright © 2013 Cancer Research UK

          From twelve months after its original publication, this work is licensed under the Creative Commons Attribution-NonCommercial-Share Alike 3.0 Unported License. To view a copy of this license, visit http://creativecommons.org/licenses/by-nc-sa/3.0/

          History
          : 06 March 2013
          : 26 March 2013
          Categories
          Molecular Diagnostics

          Oncology & Radiotherapy
          sox11,nestin,c-met,idh1-r132h,glioblastoma
          Oncology & Radiotherapy
          sox11, nestin, c-met, idh1-r132h, glioblastoma

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