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Multiplexed Cell Signaling Analysis of Metastatic and Nonmetastatic Colorectal Cancer Reveals COX2-EGFR Signaling Activation as a Potential Prognostic Pathway Biomarker.

Authors :
Pierobon M
Calvert V
Belluco C
Garaci E
Deng J
Lise M
Nitti D
Mammano E
Marchi FD
Liotta L
Petricoin E
Source :
Clinical colorectal cancer [Clin Colorectal Cancer] 2009 Mar; Vol. 8 (2), pp. 110-7.
Publication Year :
2009

Abstract

The identification of prognostic determinants of colorectal cancer (CRC), including prediction of occult metastasis, is of urgent consideration, based on the tremendous differences in outcome and survival between patients who present with metastasis or develop metastasis versus those patients with organ-confined or nonrecurrent disease. Currently, a great deal of attention has been focused on using gene expression profiles of tumor specimens as a launch point for prognostic biomarker discovery. In our study, we chose to focus on functional protein-based pathway biomarkers as a new information archive because it is these proteins that form the functional signaling networks that control cell growth, motility, apoptosis, survival, and differentiation. We used reverse-phase protein microarray analysis of laser capture microdissected CRC tumor specimens to profile broad cell signaling pathways from patients who presented with liver metastasis versus patients who remained recurrence free after follow-up. Our results indicate that members of the EGFR and COX2 signaling pathways appear differentially activated in the primary tumors of patients with synchronous metastatic disease. If validated in larger study sets, this pathway defect might be useful as a prognostic clinical tool as well as a guide to potential therapeutic intervention strategies that target occult disease and/or preventative measure.

Details

Language :
English
ISSN :
1938-0674
Volume :
8
Issue :
2
Database :
MEDLINE
Journal :
Clinical colorectal cancer
Publication Type :
Academic Journal
Accession number :
19423505
Full Text :
https://doi.org/10.3816/CCC.2009.n.018