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Abstract

Vol.53 No.11 November 2005

Experimental chemoendocrine therapy using S-1 and tamoxifen on human breast carcinoma xenografts

Takaya Yamada1), Miki Tongu2), Osamu Hiraku3), Asako Hashimoto1), Koichiro Atsuda2,4), Tatsuo Suzuki1), Yukio Suzuki1), Fumiki Asanuma5) and Yoshinori Yamada5)

1)Biomedical Laboratory, Kitasato Institute Hospital, 5-9-1 Shirokane, Minato-ku, Tokyo, Japan
2)Department of Pharmacy, Kitasato Institute Hospital
3)Laboratory Animal Center, Center for Basic Research, Kitasato Institute
4)College of Pharmacy, Kitasato University
5)Department of Surgery, Kitasato Institute Hospital

Abstract

The antitumor activity of combined chemoendocrine therapy, fluoropyrimidine derivatives and tamoxifen (TAM), was examined with three human breast carcinoma xenografts, MCF-7, R-27, and Br-10, which are estrogen receptor (ER) positive tumors. Treatments based on maximum tolerated doses were initiated in four groups: control, 5-fluorouracil (5-FU) 60 mg/kg i.p. every four days for a total of three times, S-1 20 mg/kg (as tegafur) p.o. five times a week for three weeks, and TAM 5 mg/kg p.o. six times a week for three weeks. The antitumor activity of each agent were assessed by the T/C (treated/control) ratio of relative mean tumor weight. Values for 5-FU with MCF-7, R-27 and Br-10 were 68.6, 80.4, and 52.7%, and those for S-1 were 49.0, 60.0, and 29.6%, showing higher antitumor activity than 5-FU. For TAM, values were 50.5, 62.3, and 39.8%. The activity of combination therapy, 5-FU+TAM and S-1+TAM, was tested with R-27 which showed the lowest sensitivity to each of the three agents. Values were 51.9% for 5-FU+TAM and 28.7% for S-1+TAM. Determination in thymidylate synthase (TS) inhibition and dihydropyrimidine dehydrogenase (DPD) activity then measured to examine the role of 5-FU metabolism in the antitumor effect enhancement, which showed no statistically significant difference between treatment groups, S-1 alone and S-1+TAM. 5-FU concentrations in the tumor also showed no statistically significant differences between groups. It is negative that 5-FU in the tumor is modified by TAM and another mechanism might contribute to the enhancement of antitumor effect with this combination. S-1+TAM appears to be a promising combination against advanced or recurrent hormone receptor positive breast cancer.

Key word

breast cancer, animal model, tamoxifen, combination therapy, S-1

Received

July 13, 2005

Accepted

September 27, 2005

Jpn. J. Chemother. 53 (11): 679-685, 2005