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Clinical Cancer Research Vol. 12, 5951-5959, October 15, 2006
© 2006 American Association for Cancer Research


Human Cancer Biology

GRO{alpha} Is Highly Expressed in Adenocarcinoma of the Colon and Down-Regulates Fibulin-1

Yu Wen1, Sarah F. Giardina3, David Hamming2, Jennifer Greenman1,2, Emmanuel Zachariah1, Manny D. Bacolod3, Hao Liu1, Jinru Shia4, Peter S. Amenta1, Francis Barany3, Phillip Paty4, William Gerald4 and Daniel Notterman1,2

Authors' Affiliations: 1 Robert Wood Johnson Medical School and Cancer Institute of New Jersey, New Brunswick, New Jersey; 2 Princeton University, Princeton, New Jersey; 3 Weil Medical College of Cornell University; and 4 Memorial-Sloan Kettering Cancer Center, New York, New York

Requests for reprints: Daniel A. Notterman, Departments of Pediatrics and Molecular Genetics, Robert Wood Johnson Medical School, 125 Patterson Street, MEB 306, New Brunswick, NJ 08903. Phone: 732-235-7900; Fax: 732-235-6102; E-mail: d.notterman{at}umdnj.edu.

Purpose: The growth-related oncogene {alpha} (GRO{alpha}) is a secreted interleukin-like molecule that interacts with the CXCR2 G-protein–coupled receptor. We found that the mRNA and protein products of GRO{alpha} are more highly expressed in neoplastic than normal colon epithelium, and we studied potential mechanisms by which GRO{alpha} may contribute to tumor initiation or growth.

Experimental Design: Cell lines that constitutively overexpress GRO{alpha} were tested for growth rate, focus formation, and tumor formation in a xenograft model. GRO{alpha} expression was determined by Affymetrix GeneChip (241 microdissected colon samples), real-time PCR (n = 32), and immunohistochemistry. Primary colon cancer samples were also employed to determine copy number changes and loss of heterozygosity related to the GRO{alpha} and fibulin-1 genes.

Results: In cell cultures, GRO{alpha} transfection transformed NIH 3T3 cells, whereas inhibition of GRO{alpha} by inhibitory RNA was associated with apoptosis, decreased growth rate, and marked up-regulation of the matrix protein fibulin-1. Forced expression of GRO{alpha} was associated with decreased expression of fibulin-1. Expression of GRO{alpha} mRNA was higher in primary adenocarcinomas (n = 132), adenomas (n = 32), and metastases (n = 52) than in normal colon epithelium (P < 0.001). These results were confirmed by real-time PCR and by immunohistochemistry. Samples of primary and metastatic colon cancer showed underexpression of fibulin-1 when compared with normal samples. There were no consistent changes in gene copy number of GRO{alpha} or fibulin-1, implying a transcriptional basis for these findings.

Conclusion: Elevated expression of GRO{alpha} is frequent in adenocarcinoma of the colon and is associated with down-regulation of the matrix protein fibulin-1 in experimental models and in clinical samples. GRO{alpha} overexpression abrogates contact inhibition in cell culture models, whereas inhibition of GRO{alpha} expression is associated with apoptosis. Importantly, coexpression of fibulin-1 with GRO{alpha} abrogates key aspects of the transformed phenotype, including tumor formation in a murine xenograft model. Targeting GRO proteins may provide new opportunities for treatment of colon cancer.




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M. D. Bacolod, G. S. Schemmann, S. Wang, R. Shattock, S. F. Giardina, Z. Zeng, J. Shia, R. F. Stengel, N. Gerry, J. Hoh, et al.
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[Abstract] [Full Text] [PDF]




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Copyright © 2006 by the American Association for Cancer Research.