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Therapeutic effect of nimesulide on colorectal carcinogenesis in experimental murine ulcerative colitis
Author(s) -
Inoue Takuya,
Murano Mitsuyuki,
Abe Yosuke,
Morita Eijiro,
Murano Naoko,
Yasumoto Shingo,
Toshina Ken,
Nishikawa Takashi,
Maemura Kentaro,
Hirata Ichiro,
Katsu Kenichi
Publication year - 2007
Publication title -
journal of gastroenterology and hepatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.214
H-Index - 130
eISSN - 1440-1746
pISSN - 0815-9319
DOI - 10.1111/j.1440-1746.2007.04866.x
Subject(s) - nimesulide , medicine , colorectal cancer , ulcerative colitis , gastroenterology , colitis , dysplasia , cancer , celecoxib , carcinogenesis , disease
Background: Patients with ulcerative colitis (UC) exhibit an increased risk for the development of cancer of the colon and rectum. Cyclooxygenase (COX)‐2 inhibitors are known to suppress sporadic colorectal cancer, but it is unknown whether selective COX‐2 inhibitors exhibit a preventive effect in UC‐associated neoplasia. This study investigated the preventive effect of nimesulide, a selective COX‐2 inhibitor, on colorectal carcinogenesis in an experimental model of murine UC. Methods: Chronic colitis was induced in mice by administration of four cycles of dextran sulfate sodium (DSS) (each cycle: 5% DSS for 7 days and then distilled water for 14 days). The mice were killed 120 days after the completion of the fourth cycle. The mice were divided into the following five groups: group A served as a disease control; group B received a diet mixed with 400 p.p.m. of nimesulide during the whole period; group C received nimesulide during the four cycles of DSS administration (active phase); group D received nimesulide for 120 days from the end of the fourth cycle (remission phase); group E received no agents including DSS and served as a normal control. Results: The incidence of dysplasia and/or cancer was 28%, 15%, 11.8%, 6.7% and 0% in groups A–E, respectively. In group D, nimesulide significantly suppressed the occurrence of dysplasia and/or cancer ( P < 0.05). Strong COX‐2 expression was detected by immunohistochemistry in cancer and dysplastic lesions while diffusely weak COX‐2 expression was also found in the residual colon (i.e. lesion‐free colon). The mucosal concentration of prostaglandin E 2 was significantly lower in groups B and D than in group A. Conclusions: The administration of the selective COX‐2 inhibitor nimesulide (especially during the remission phase) exerts a suppressive effect on the development of dysplasia and/or cancer in a murine model of DSS‐induced colitis. These findings may have relevance to long‐standing UC in humans.