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  • Localization of nuclear cathepsin L and its association with disease progression and poor outcome in colorectal cancer.

Localization of nuclear cathepsin L and its association with disease progression and poor outcome in colorectal cancer.

International journal of cancer (2009-03-18)
Shane Sullivan, Miriam Tosetto, David Kevans, Alan Coss, Laimun Wang, Diarmuid O'Donoghue, John Hyland, Kieran Sheahan, Hugh Mulcahy, Jacintha O'Sullivan
ABSTRACT

Previous in vitro studies have identified a nuclear isoform of Cathepsin L. The aim of this study was to examine if nuclear Cathepsin L exists in vivo and examine its association with clinical, pathological and patient outcome data. Cellular localization (nuclear and cytoplasmic) and expression levels v of Cathespin L in 186 colorectal cancer cases using immunohistochemistry. The molecular weight and activity of nuclear and cytoplasmic Cathepsin L in vivo and in vitro were assessed by Western blotting and ELISA, respectively. Epithelial nuclear staining percentage (p = 0.04) and intensity (p = 0.006) increased with advancing tumor stage, whereas stromal cytoplasmic staining decreased (p = 0.02). Using multivariate statistical analysis, survival was inversely associated with staining intensity in the epithelial cytoplasm (p = 0.01) and stromal nuclei (p = 0.007). In different colorectal cell lines and in vivo tumors, pro- and active Cathepsin L isoforms were present in both the cytoplasm and nuclear samples, with pro-Cathepsin L at 50 kDa and active Cathepsin L at 25 kDa. Purified nuclear and cytoplasmic fractions from cell lines and tumors showed active Cathepsin L activity. The identification of nuclear Cathepsin L may play an important prognostic role in colorectal disease progression and patient outcome. Moreover, these findings suggest that altering active nuclear Cathepsin L may significantly influence disease progression.

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Sigma-Aldrich
InnoZyme Cathepsin L Activity Kit, Fluorogenic