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Published in: BMC Clinical Pathology 1/2012

Open Access 01-12-2012 | Research article

Tenascin-W is a better cancer biomarker than tenascin-C for most human solid tumors

Authors: Florence Brellier, Enrico Martina, Martin Degen, Nathalie Heuzé-Vourc’h, Agnès Petit, Thomas Kryza, Yves Courty, Luigi Terracciano, Christian Ruiz, Ruth Chiquet-Ehrismann

Published in: BMC Clinical Pathology | Issue 1/2012

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Abstract

Background

Tenascins are large glycoproteins found in the extracellular matrix of many embryonic and adult tissues. Tenascin-C is a well-studied biomarker known for its high overexpression in the stroma of most solid cancers. Tenascin-W, the least studied member of the family, is highly expressed in the stroma of colon and breast tumors and in gliomas, but not in the corresponding normal tissues. Other solid tumors have not been analyzed. The present study was undertaken to determine whether tenascin-W could serve as a cancer-specific extracellular matrix protein in a broad range of solid tumors.

Methods

We analyzed the expression of tenascin-W and tenascin-C by immunoblotting and by immunohistochemistry on multiple frozen tissue microarrays of carcinomas of the pancreas, kidney and lung as well as melanomas and compared them to healthy tissues.

Results

From all healthy adult organs tested, only liver and spleen showed detectable levels of tenascin-W, suggesting that tenascin-W is absent from most human adult organs under normal, non-pathological conditions. In contrast, tenascin-W was detectable in the majority of melanomas and their metastases, as well as in pancreas, kidney, and lung carcinomas. Comparing lung tumor samples and matching control tissues for each patient revealed a clear overexpression of tenascin-W in tumor tissues. Although the number of samples examined is too small to draw statistically significant conclusions, there seems to be a tendency for increased tenascin-W expression in higher grade tumors. Interestingly, in most tumor types, tenascin-W is also expressed in close proximity to blood vessels, as shown by CD31 co-staining of the samples.

Conclusions

The present study extends the tumor biomarker potential of tenascin-W to a broad range of solid tumors and shows its accessibility from the blood stream for potential therapeutic strategies.
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Metadata
Title
Tenascin-W is a better cancer biomarker than tenascin-C for most human solid tumors
Authors
Florence Brellier
Enrico Martina
Martin Degen
Nathalie Heuzé-Vourc’h
Agnès Petit
Thomas Kryza
Yves Courty
Luigi Terracciano
Christian Ruiz
Ruth Chiquet-Ehrismann
Publication date
01-12-2012
Publisher
BioMed Central
Published in
BMC Clinical Pathology / Issue 1/2012
Electronic ISSN: 1472-6890
DOI
https://doi.org/10.1186/1472-6890-12-14

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