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Commentary

Post-translational modifications of the extracellular matrix are key events in cancer progression: Opportunities for biochemical marker development

, , , , &
Pages 193-205 | Received 11 Nov 2010, Accepted 20 Jan 2011, Published online: 20 Apr 2011
 

Abstract

The aim of this review is to discuss the potential usefulness of a novel class of biochemical markers, designated neoepitopes. Neoepitopes are post-translational modifications (PTMs) of proteins and are derived by processes, such as protease cleavage, citrullination, nitrosylation, glycosylation and isomerization. Each PTM results from a specific local physiological or pathobiologial process. Identification of each modification to a tissue-specific protein may reveal a unique disease-specific biochemical marker. During cancer metastasis, the host tissue is extensively degraded and replaced by cancer-associated extracellular matrix (ECM) proteins. Furthermore, severe cellular stress and inflammation, caused by cancer, results in generation of PTMs, which will be distributed throughout the ECM. This gives rise to release of protein-specific fragments to the circulation. Here we highlight the importance of remodeling of the ECM in cancer and the generation of PTMs, which may be cancer specific and reflect disease progression; thus having potential for biochemical marker development.

Corrigendum

This version contains a different figure 1 to the previous version published online as permission to use the original figure was not obtained

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