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Cadherin Expression Profiles Define Glioblastoma Differentiation and Patient Prognosis. | LitMetric

Cadherin Expression Profiles Define Glioblastoma Differentiation and Patient Prognosis.

Cancers (Basel)

Cancer Metastasis, i3S, Institute for Research and Innovation in Health, University of Porto, 4200-135 Porto, Portugal.

Published: June 2024

AI Article Synopsis

  • Cadherins are important proteins involved in cell adhesion and play a crucial role in cancer progression, particularly in glioblastoma, which is an aggressive brain tumor.
  • A study analyzed N-, E-, and P-cadherin expression in a large group of GBM cases and found that N-cadherin was most common, while P-cadherin was notably upregulated in recurrent tumors.
  • Co-expression of different cadherins revealed distinct GBM subgroups, with E- and N-cadherin linked to better survival outcomes, while those expressing P-cadherin were associated with more aggressive tumor characteristics and poorer prognosis.

Article Abstract

Cadherins are cell-cell adhesion proteins which have been strongly implicated in cancer invasion, dissemination and metastasis capacity; thus, they are key players in the epithelial-to-mesenchymal transition (EMT) program. However, their role in glioblastoma (GBM), a primary central nervous system aggressive tumor, remains to be clarified. N-, E- and P-cadherin expression was analyzed on a large series of GBMs, characterized with clinical, imaging and neuropathological parameters, as well as with patients' survival data. In addition, cadherins' expression was studied in match-recurrent cases. Using TCGA data, cadherin expression profiles were also evaluated according to GBM transcription subtypes. N-cadherin expression was observed in 81.5% of GBM, followed by E-cadherin in 31% and P-cadherin in 20.8%. Upon tumor recurrence, P-cadherin was the only significantly upregulated cadherin compared with the primary tumor, being positive in 65.8% of the cases. Actually, P-cadherin gain was observed in 51.4% of matched primary-recurrent cases. Cadherins' co-expression was also explored. Interestingly, E- and N-cadherin co-expression identified a GBM subgroup with frequent epithelial differentiation and a significant survival benefit. On the other hand, subgroups with P-cadherin expression carried the worse prognosis. P- and N-cadherin co-expression correlated with the presence of a mesenchymal phenotype. Expressions of isolated P-cadherin or E- and P-cadherin co-expression were associated with imaging characteristics of aggressiveness, to highly heterogeneous tumors, an d to worse patient survival. Classical cadherins co-expression subgroups present consistent clinical, imaging, neuropathological and survival differences, which probably reflect different states of an EMT-like program in GBM.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11240393PMC
http://dx.doi.org/10.3390/cancers16132298DOI Listing

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