R-etodolac induces E-cadherin and suppresses colitis-related mouse colon tumorigenesis

  • Authors:
    • Takuya Inoue
    • Mitsuyuki Murano
    • Yukiko Yoda
    • Takanori Kuramoto
    • Kazuki Kakimoto
    • Kumi Ishida
    • Ken Kawakami
    • Yosuke Abe
    • Eijiro Morita
    • Naoko Murano
    • Satoshi Tokioka
    • Kentaro Maemura
    • Eiji Umegaki
    • Kazuhide Higuchi
  • View Affiliations

  • Published online on: December 1, 2010     https://doi.org/10.3892/or_00001009
  • Pages: 1487-1492
Metrics: Total Views: 0 (Spandidos Publications: | PMC Statistics: )
Total PDF Downloads: 0 (Spandidos Publications: | PMC Statistics: )


Abstract

Colorectal cancer is one of the most serious complications of ulcerative colitis (UC), and the risk of UC-associated neoplasia increases as the region and duration of the disease increase. Selective cyclooxygenase (COX)-2 inhibitors effectively diminish carcinogenesis in a murine UC model. However, this may exacerbate colitis. The selective COX-2 inhibitor etodolac is marketed as a racemic mixture of the R- and S-enantiomers. The biochemical and pharmacological effects of etodolac are caused by the S-enantiomer, while the R-enantiomer lacks COX-inhibitory activity. In this study, we evaluated the effect of R-etodolac on colitis-related mouse colon tumorigenesis. The mice received 1,2-dimethlhydrazine (DMH), and then chronic colitis was induced by administration of two cycles of DSS (each cycle: 3% DSS for 7 days followed by distilled water for 14 days). The mice were sacrificed 28 days after the completion of both cycles. Mice were divided into the following groups: group A served as a disease control; group B received a low (2-mg/kg) dose of R-etodolac every 3 days during the entire period; group C received a high (10-mg/kg) dose of R-etodolac on the same schedule as group B; and group D served as a normal control. Administration of R-etodolac decreased the disease activity index during the DSS administration cycle. The mean number of tumors was 17.8, 15.2, 6.0, and 0 in groups A-D, respectively. In group C, R-etodolac significantly suppressed the occurrence of neoplasia (p<0.05). Although R-etodolac treatment did not affect COX-2 expression, it significantly enhanced expression of E-cadherin in both neoplastic lesions and background mucosa (i.e., lesion-free colon). Thus, administration of R-etodolac exerts a suppressive effect on the development of neoplasia in a murine model of DSS-induced colitis without exacerbation of the colitis. These results suggest that R-etodolac could be useful in the prevention of UC-associated neoplasia.

Related Articles

Journal Cover

December 2010
Volume 24 Issue 6

Print ISSN: 1021-335X
Online ISSN:1791-2431

Sign up for eToc alerts

Recommend to Library

Copy and paste a formatted citation
x
Spandidos Publications style
Inoue T, Murano M, Yoda Y, Kuramoto T, Kakimoto K, Ishida K, Kawakami K, Abe Y, Morita E, Murano N, Murano N, et al: R-etodolac induces E-cadherin and suppresses colitis-related mouse colon tumorigenesis . Oncol Rep 24: 1487-1492, 2010.
APA
Inoue, T., Murano, M., Yoda, Y., Kuramoto, T., Kakimoto, K., Ishida, K. ... Higuchi, K. (2010). R-etodolac induces E-cadherin and suppresses colitis-related mouse colon tumorigenesis . Oncology Reports, 24, 1487-1492. https://doi.org/10.3892/or_00001009
MLA
Inoue, T., Murano, M., Yoda, Y., Kuramoto, T., Kakimoto, K., Ishida, K., Kawakami, K., Abe, Y., Morita, E., Murano, N., Tokioka, S., Maemura, K., Umegaki, E., Higuchi, K."R-etodolac induces E-cadherin and suppresses colitis-related mouse colon tumorigenesis ". Oncology Reports 24.6 (2010): 1487-1492.
Chicago
Inoue, T., Murano, M., Yoda, Y., Kuramoto, T., Kakimoto, K., Ishida, K., Kawakami, K., Abe, Y., Morita, E., Murano, N., Tokioka, S., Maemura, K., Umegaki, E., Higuchi, K."R-etodolac induces E-cadherin and suppresses colitis-related mouse colon tumorigenesis ". Oncology Reports 24, no. 6 (2010): 1487-1492. https://doi.org/10.3892/or_00001009