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Experimental Therapeutics

Antiangiogenic and Antitumor Activities of Cyclooxygenase-2 Inhibitors

Jaime L. Masferrer, Kathleen M. Leahy, Alane T. Koki, Ben S. Zweifel, Steven L. Settle, B. Mark Woerner, Dorothy A. Edwards, Amy G. Flickinger, Rosalyn J. Moore and Karen Seibert
Jaime L. Masferrer
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Kathleen M. Leahy
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Alane T. Koki
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Ben S. Zweifel
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Steven L. Settle
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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B. Mark Woerner
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Dorothy A. Edwards
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Amy G. Flickinger
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Rosalyn J. Moore
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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Karen Seibert
G. D. Searle/Monsanto Company, St. Louis, Missouri 63167
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DOI:  Published March 2000
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Abstract

We provide evidence that cyclooxygenase (COX)-2-derived prostaglandins contribute to tumor growth by inducing newly formed blood vessels (neoangiogenesis) that sustain tumor cell viability and growth. COX-2 is expressed within human tumor neovasculature as well as in neoplastic cells present in human colon, breast, prostate, and lung cancer biopsy tissue. COX-1 is broadly distributed in normal, as well as in neoplastic, tissues. The contribution of COX-2 to human tumor growth was indicated by the ability of celecoxib, an agent that inhibits the COX-2 enzyme, to suppress growth of lung and colon tumors implanted into recipient mice. Mechanistically, celecoxib demonstrated a potent antiangiogenic activity. In a rat model of angiogenesis, we observe that corneal blood vessel formation is suppressed by celecoxib, but not by a COX-1 inhibitor. These and other data indicate that COX-2 and COX-2-derived prostaglandins may play a major role in development of cancer through numerous biochemical mechanisms, including stimulation of tumor cell growth and neovascularization. The ability of celecoxib to block angiogenesis and suppress tumor growth suggests a novel application of this anti-inflammatory drug in the treatment of human cancer.

  • Received July 13, 1999.
  • Accepted January 7, 2000.
  • ©2000 American Association for Cancer Research.
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March 2000
Volume 60, Issue 5
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Antiangiogenic and Antitumor Activities of Cyclooxygenase-2 Inhibitors
Jaime L. Masferrer, Kathleen M. Leahy, Alane T. Koki, Ben S. Zweifel, Steven L. Settle, B. Mark Woerner, Dorothy A. Edwards, Amy G. Flickinger, Rosalyn J. Moore and Karen Seibert
Cancer Res March 1 2000 (60) (5) 1306-1311;

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Antiangiogenic and Antitumor Activities of Cyclooxygenase-2 Inhibitors
Jaime L. Masferrer, Kathleen M. Leahy, Alane T. Koki, Ben S. Zweifel, Steven L. Settle, B. Mark Woerner, Dorothy A. Edwards, Amy G. Flickinger, Rosalyn J. Moore and Karen Seibert
Cancer Res March 1 2000 (60) (5) 1306-1311;
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