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Anticancer benefits of early versus late use of rapamycin in a rat model of urothelial carcinoma

机译:雷帕霉素在尿路上皮癌大鼠模型中早期和晚期使用的抗癌作用

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Background We previously reported both in vivo and in vitro effects of rapamycin on urothelial carcinoma. Clinically, the use of rapamycin could not completely prevent the recurrence of urothelial carcinoma. Therefore, we designed this study to compare the difference of efficacy between early and late use of rapamycin in a rat model of urothelial carcinoma. Methods The rat model of urothelial carcinoma was induced by adding 0.05% N-butyl-N-(4-hydroxybutyl) nitrosamine (BBN) to the drinking water for up to 20 weeks in male Fisher-344 rats. Rapamycin was fed orally from the 1st day, 5th week, 9th week, 13th week, and 17th week. The antitumor effects of different periods of rapamycin treatment were assessed grossly and microscopically. Results Papillary tumors of urinary bladder were successfully induced in the BBN group. Simultaneous use of rapamycin and BBN from the 1st day of treatment significantly reduced the tumor growth in urinary bladder: 80% of the rats had no tumor and 20% had low-grade tumors. Adding rapamycin from the 5th week was associated with more tumor growth: 20% of the rats had no tumors, 20% had low-grade tumors, and 60% had high-grade tumors. Moreover, in the groups with rapamycin treatment from the 9th week, 13th week, and 17th week, all rats developed high-grade papillary tumors in urinary bladder, as did the control group that received no rapamycin. Conclusions The study results suggest that the anticancer effect of rapamycin on urothelial carcinoma is stage dependent. Early use of rapamycin provides better anticancer effect, whereas late use of rapamycin fails to inhibit the cancer growth.
机译:背景我们以前曾报道雷帕霉素对尿路上皮癌的体内和体外作用。在临床上,雷帕霉素的使用不能完全预防尿路上皮癌的复发。因此,我们设计了这项研究,以比较雷帕霉素在尿路上皮癌大鼠模型中早期和晚期使用雷帕霉素的疗效差异。方法对雄性Fisher-344大鼠在饮用水中添加0.05%的N-丁基-N-(4-羟丁基)亚硝胺(BBN)诱导长达20周,以建立尿路上皮癌大鼠模型。从第1天,第5周,第9周,第13周和第17周开始口服雷帕霉素。对雷帕霉素治疗不同时期的抗肿瘤作用进行了总体和微观评估。结果BBN组成功诱导出膀胱乳头状肿瘤。从治疗的第一天开始同时使用雷帕霉素和BBN会显着降低膀胱肿瘤的生长:80%的大鼠没有肿瘤,而20%的患者患有低度肿瘤。从第5周开始添加雷帕霉素与更多的肿瘤生长相关:20%的大鼠无肿瘤,20%的小鼠为低度肿瘤,60%的患者为高度肿瘤。此外,在从第9周,第13周和第17周开始接受雷帕霉素治疗的组中,所有大鼠均出现膀胱高度乳头状肿瘤,而未接受雷帕霉素的对照组也是如此。结论研究结果表明雷帕霉素对尿路上皮癌的抗癌作用是阶段性的。早期使用雷帕霉素可提供更好的抗癌作用,而晚期使用雷帕霉素则不能抑制癌症的生长。

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