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首页> 外文期刊>The Prostate >Sequential combinations of flavopiridol and docetaxel inhibit prostate tumors, induce apoptosis, and decrease angiogenesis in the Ggamma/T-15 transgenic mouse model of prostate cancer.
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Sequential combinations of flavopiridol and docetaxel inhibit prostate tumors, induce apoptosis, and decrease angiogenesis in the Ggamma/T-15 transgenic mouse model of prostate cancer.

机译:黄酮哌啶醇和多西他赛的顺序组合可抑制前列腺癌的Ggamma / T-15转基因小鼠模型中的前列腺肿瘤,诱导细胞凋亡并减少血管生成。

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BACKGROUND: We investigated whether sequential combinations of flavopiridol and docetaxel can increase apoptotic cell death and inhibit the growth of primary and metastatic prostate tumors in the Ggamma/T-15 transgenic mouse model of prostate cancer. METHODS: Transgenic males were treated and the weights of primary and metastatic prostate tumors determined. Immunohistochemistry and Western blot was performed to evaluate the differences in apoptosis, proliferation, and angiogenesis. RESULTS: Docetaxel was slightly more effective than flavopiridol in inhibiting primary prostate tumors, but neither drug alone inhibited metastases. Single drug treatments decreased angiogenesis but did not increase apoptosis. Both sequential combinations resulted in greater inhibition of primary and metastatic prostate tumors, increased apoptosis, and decreased angiogenesis compared to control mice. CONCLUSIONS: Flavopiridol and docetaxel sequence combinations were effective in inhibiting prostate tumors in the Ggamma/T-15 transgenic mice. An increase in apoptosis and a decrease in angiogenesis resulted in the greatest inhibition of prostate cancers.
机译:背景:我们研究了黄酮哌啶醇和多西他赛的顺序组合是否可以增加凋亡的细胞死亡并抑制前列腺癌的Ggamma / T-15转基因小鼠模型中原发性和转移性前列腺肿瘤的生长。方法:治疗转基因男性,确定原发性和转移性前列腺肿瘤的重量。进行了免疫组织化学和蛋白质印迹以评估细胞凋亡,增殖和血管生成的差异。结果:多西他赛在抑制原发性前列腺肿瘤方面比氟哌啶醇稍有效,但没有一种药物能单独抑制转移。单药治疗减少血管生成,但不增加细胞凋亡。与对照小鼠相比,两种顺序组合均导致对原发性和转移性前列腺肿瘤的更大抑制,增加的细胞凋亡和减少的血管生成。结论:黄酮哌啶醇和多西紫杉醇序列组合可有效抑制Ggamma / T-15转基因小鼠的前列腺肿瘤。凋亡的增加和血管生成的减少导致对前列腺癌的最大抑制。

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