TY - JOUR AB - We investigated the antitumor activity of TS-1 in comparison with that of UFT and cisplatin (CDDP) against cervical cancer using xenografts of a human uterine cervical squamous cell cancer cell line, CaSki, transplanted into female Balb/cA JcL-nu mice. CaSki cell xenografts were prepared by subcutaneous (s.c.) implantation of 3x106 cells/animal into the right dorsal region of the mice. The tumor volume was measured twice a week and the relative tumor volume (RTV) was calculated. We divided the animals into four groups according to the treatment administered; TS-1 (10 mg/kg orally, once daily for 14 consecutive days), UFT (24 mg/kg orally, once daily for 14 consecutive days), CDDP (7.6 mg/kg injected intravenously once on the 1st day) and control (no treatment) groups. The antitumor effects of the drugs were measured. On the 35th day after the completion of treatment, the mean tumor volume in the mice treated with TS-1 or CDDP changed from 132.873±11.783 mm3 to 706.401±613.122 mm3 and 133.809±19.366 mm3 to 722.630±855.509 mm3, respectively. The mean tumor volume in the groups treated with TS-1 or CDDP was significantly lower compared to that in the control group (p<0.001; one-tailed Student's t-test). The relative inhibition of the tumor growth was 65.31 in the TS-1 group, 48.31 in the UFT group and 64.51 in the CDDP group. We conclude that TS-1 administered orally for 14 consecutive days showed the highest antitumor activity. AD - Department of Obstetrics and Gynecology, Hiroshima City Asa Hospital, Hiroshima 731-0293, Japan. n-nagai@asa-hosp.city.hiroshima.jp null AU - Nagai,Nobutaka AU - Komatsu,Masaaki AU - Yunokawa,Mayu AU - Shiroyama,Yuko AU - Hirata,Eiji DA - 2008/11/01 DO - 10.3892/or_00000123 EP - 1156 IS - 5 JO - Oncol Rep PY - 2008 SN - 1021-335X 1791-2431 SP - 1149 ST - Preclinical analysis of the antitumor efficacy of TS-1 using human uterine cervical cancer tumor xenografts T2 - Oncology Reports TI - Preclinical analysis of the antitumor efficacy of TS-1 using human uterine cervical cancer tumor xenografts UR - https://doi.org/10.3892/or_00000123 VL - 20 ER -