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• W2380807696 abstract "AIM To study anti- tumor effects of paclitaxel micelle(PTX- PM) for injection on tumorbearing mice in vivo. METHODS Male nude mice were implanted with xenograft fragments of human lung adenocarcinoma A549 or human colorectal cancer HT29 tissue subcutaneously in the right flank. When tumor in the nude mice reached a tumor volume of 100 mm3, the nude mice bearing tumor were divided into 6 groups(control, polymeric micelle(PM), paclitaxel injection(PTXI), three PTX- PM treated groups). Each group had 6 mice. A single dose of PTX- PM in saline was administered intravenously at 10, 20 mg·kg-1every three days. PTXI in saline was also administered intravenously at 20 mg·kg-1every three days, 7- 8 times in the experiment. While in the PTX- PM 50 mg·kg-1group only 4 times were given. In control experiments, saline and PM vehicle were used. Tumor size and body weight was measured before every time for the duration of the study,and tumor volume, relative tumor volume or relative proliferation rate of tumor was calculated. RESULTS None of the animals treated with PTX- PM died in the two model experiments during the experimental period. Only the tumor- bearing mice in the PTX- PM 50 mg·kg-1group appeared response slowing, activity decreasing, poor skin luster, loose stools and body weight losing(P 0.05 or P 0.01) after administered 4 times. There were no obviously abnormal reactions in the mice of the 10 or 20 mg·kg-1group. In the PTX- PM 20 or 50 mg·kg-1group of the two model experiments, the relative tumor proliferation rates were less than 40% and the relative tumor volumes were significant different from the control group till the end of the experiment. While in the PTX- PM10 mg·kg-1group or PM group the relative tumor proliferation rates were greater than 40% and the relative tumor volumes were similar to the control group. CONCLUSION Under the experimental conditions, PTX- PM 20 or50 mg·kg-1could inhibit HT29 and A549 xenografts growth in nude mice, and had a significant anti- tumor effect, but the systematic toxicity of PTX- PM 50 mg·kg-1dose was significantly higher than 20 mg·kg-1." @default.
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• W2380807696 date "2014-01-01" @default.
• W2380807696 modified "2023-09-25" @default.
• W2380807696 title "Anti-tumor effects of paclitaxel micelle for injection in vivo" @default.
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