Abstract
To evaluate the influence of inhibitors of prostaglandin synthesis on the incidence of DMH-induced colon cancer, 90 male Sprague-Dawley rats were randomly assigned to: 1) indomethacin 20 mg per liter drinking water, 2) meclofenamate 50 mg per liter drinking water, or 3) normal drinking water (control group). Dimethylhydrazine was given by weekly subcutaneous injections (20 mg/kg body weight) during the first 20 weeks. Thirty-two weeks after the start of treatment and carcinogen exposure, the animals were killed and examined for the number, size, location, and spread of intestinal tumors. Colon cancer incidence was significantly lower in animals receiving indomethacin (56 per cent) compared with the control group (88 per cent) and with the meclofenamate group (90 per cent) (P<0.005). The corresponding figures for tumors in the small intestine were 31, 46, and 35 per cent, respectively. The tumors in indomethacin-treated animals did not differ in number, size, location, or spread from tumors of the other groups, suggesting that indomethacin might influence the carcinogenic process itself, rather than the natural course of the established disease. We conclude that indomethacin significantly reduces the incidence of large-bowel cancer in this animal model and that this observation may have some potential for future chemopreventive studies in human high-risk groups (e.g. ulcerative colitis, familial polyposis).
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References
Tutton PJ, Barkla DH. Influence of prostaglandin analogues on epithelial cell proliferation and xenograft growth. Br J Cancer 1980;41:47–51.
Maskens AP. Mechanism of histogenesis and carcinogenesis in dimethylhydrazine-induced rat colon cancer. In: Gerard A, ed. Gastrointestinal tumors, a clinical and experimental approach. Oxford: Pergamon Press, 1978:95–104.
Sunter JP, Hull DL, Appleton DR, Watson AJ. Cell proliferation of colonic neoplasms in dimethylhydrazine-treated rats. Br J Cancer 1980;42:95–102.
Bennet A, Berstock DA, Carroll MA. Increased survival of cancer-bearing mice treated with inhibitors of prostaglandin synthesis alone or with chemotherapy. Br J Cancer 1982;45:762–8.
Lynch NR, Castes M, Astoin M, Salomon JC. Mechanism of inhibition of tumor growth by aspirin and indomethacin. Br J Cancer 1978;38:503–9.
Trevisiani A, Ferretti E, Capuzzo A, Tomasi V. Elevated levels of prostaglandin E2 in Yoshida hepatoma and the inhibition of tumor growth by nonsteroidal anti-inflammatory drugs. Br J Cancer 1980;41:341–7.
DeRubertis FR, Craven PA. Early alterations in rat colonic mucosal cyclic necleotide metabolism and protein kinase activity induced by 1.2-dimethylhydrazine. Cancer Res 1980;40:r589–98.
Robert A. Cytoprotection by prostaglandins. Gastroenterology 1979;77:761–9.
Plescia OJ, Smith AH, Grinwich K. Subversion of immune system by tumor cells and role of prostaglandins. Proc Natl Acad Sci 1975;72:1848.
Bussey HJ, DeCosse JJ, Deschner EE, et al., A randomized trial of ascorbic acid in polyposis coli. Cancer 1982;50:1434–9.
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Metzger, U., Meier, J., Uhlschmid, G. et al. Influence of various prostaglandin synthesis inhibitors on DMH-induced rat colon cancer. Dis Colon Rectum 27, 366–369 (1984). https://doi.org/10.1007/BF02553001
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DOI: https://doi.org/10.1007/BF02553001