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Review Article

Molecular Targets in Metastasis: Lessons from Genomic Approaches

BARBARA FINGLETON
Cancer Genomics & Proteomics May 2007, 4 (3) 211-221;
BARBARA FINGLETON
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  • For correspondence: barbara.fingleton{at}Vanderbilt.edu
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Abstract

Microarray studies have yielded valuable information that can be used to determine a cancer patient's prognosis and allow for optimum treatment choices. Tumor profiling has also changed our perception of metastatic propensity. Genomic analyses clearly showed that a metastasis signature is encoded within the genome so that when a cancer develops, the likelihood of metastasis is high, whereas other cancers which do not have this genotype metastasize as a result of random mutations. It is certain however, that cells other than tumor cells contribute to the development of metastasis through their production of various pro-metastatic proteins. Here, we review the published metastasis profiling studies and the role of the host in metastasis. Collagen type I, CXCR4, CSF-1, OPN and RhoC are metastasis-associated genes for which evidence exists for a causal contribution to elements of the metastatic process. These genes are discussed in detail and represent excellent drug targets for anti-metastasis therapies.

Keywords:
  • Microarray
  • profile
  • host
  • collagen
  • rhoC
  • CXCR4
  • CSF-1
  • osteopontin
  • review

Footnotes

    • Received February 9, 2007.
    • Accepted February 20, 2007.
  • Copyright © 2007 The Author(s). Published by the International Institute of Anticancer Research.
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Cancer Genomics & Proteomics
Vol. 4, Issue 3
May-June 2007
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Molecular Targets in Metastasis: Lessons from Genomic Approaches
BARBARA FINGLETON
Cancer Genomics & Proteomics May 2007, 4 (3) 211-221;

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Molecular Targets in Metastasis: Lessons from Genomic Approaches
BARBARA FINGLETON
Cancer Genomics & Proteomics May 2007, 4 (3) 211-221;
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