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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Doxorubicin and mitoxantrone drug eluting beads for the treatment of experimental peritoneal carcinomatosis in colorectal cancer.
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Doxorubicin and mitoxantrone drug eluting beads for the treatment of experimental peritoneal carcinomatosis in colorectal cancer.

机译:阿霉素和米托蒽醌药物洗脱珠用于治疗大肠癌的实验性腹膜癌病。

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We investigated the therapeutic efficiency of sulfonate-modified polyvinyl alcohol beads loaded with doxorubicin, irinotecan or mitoxantrone in vitro and in vivo in a model of experimental peritoneal carcinomatosis (PC). In vitro, cell proliferation was efficiently impaired by doxorubicin drug eluting bead (DEB) treatment while mitoxantrone DEBs were less effective than. Irinotecan showed little effect for both DEBs and free drug. Apoptosis was not different between free mitoxantrone and the DEB form while more apoptosis induction was observed in cells incubated with free doxorubicin and irinotecan. Experimental PC was produced in mice. The therapeutic efficiency of either mitoxantrone and doxorubicin DEB or free drugs were compared. Mice were treated either once on day 12 or by 3 repetitive applications on days 7, 10 and 12. Mice treated by DEBs showed less weight loss and mortality. Therapeutic effect was determined by measuring tumor volume and tumor load on the day 15 after tumor inoculation. For the single application on the day 12, an advantage could be observed for the free drugs. After 3 repeated injections of both free and mitoxantrone DEB no difference in tumor load or tumor volume could be observed. Least tumor load and tumor volume was observed in mice that received 3 repeated injections of doxorubicin DEB. No animal survived 3 injections of free doxorubicin. We conclude that bead encapsulation of chemotherapeutic drugs may show the advantage of less toxicity in peritoneal spread of colorectal cancer.
机译:我们在实验性腹膜癌(PC)模型中,研究了在体外和体内用阿霉素,伊立替康或米托蒽醌负载的磺酸盐改性聚乙烯醇珠的治疗效果。在体外,阿霉素药物洗脱微珠(DEB)处理有效地削弱了细胞增殖,而米托蒽醌DEB的效果却不如后者。伊立替康对DEB和游离药物均显示出很小的作用。游离米托蒽醌和DEB形式之间的凋亡没有区别,而在用游离阿霉素和伊立替康孵育的细胞中观察到更多的凋亡诱导。在小鼠中产生实验PC。比较了米托蒽醌和阿霉素DEB或游离药物的治疗效率。在第12天对小鼠进行了一次治疗,或者在第7、10和12天进行了3次重复性应用。用DEB进行治疗的小鼠的体重减轻和死亡率降低。通过在肿瘤接种后第15天测量肿瘤体积和肿瘤负荷来确定治疗效果。对于第12天的单一应用,可以观察到游离药物的优势。重复注射游离和米托蒽醌DEB 3次后,未观察到肿瘤负荷或肿瘤体积的差异。在接受3次重复注射阿霉素DEB的小鼠中观察到最小的肿瘤负荷和肿瘤体积。没有动物存活3次注射游离阿霉素。我们得出的结论是,化疗药物的珠粒封装可能在结直肠癌的腹膜扩散中显示出毒性较小的优势。

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