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Intraductally administered pegylated liposomal doxorubicin reduces mammary stem cell function in the mammary gland but in the long term induces malignant tumors

机译:内部施用的聚乙二醇化脂质体DOXORUBININ减少了乳腺中的乳腺干细胞功能但长期诱导恶性肿瘤

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摘要

Previously, we have shown that the intraductal (i.duc) administration of pegylated liposomal doxorubicin (PLD) to Her2eu transgenic mice is associated with mammary tumor regression and prevention. Exploring the mechanism underlying the protection afforded by PLD, we studied: the effects of i.duc PLD-treatment with a subsequent pregnancy on outgrowth of tumors in Her2eu mice; whether the i.duc PLD antitumor effect was mediated partially through changes in normal mammary stem cells (MaSCs); and the long-term safety of i.duc PLD into the normal mouse mammary gland. Her2eu mice were treated with two i.duc injections of PLD given four weeks apart; pregnancy was induced and mice were followed up for changes in physiology, and tumor formation. We found that all pups born to i.duc PLD-treated Her2eu mice died without weight gain within 7 days after birth. Despite an additional pregnancy, compared to vehicle control PLD-treated Her2eu mice had a significantly longer latency and lower frequency of tumor development. Mammary epithelial cells isolated from untreated and i.duc PLD-treated 6–8 months-old multiparous FVB/N mice were analyzed for their repopulating ability in mammary fat pads of naïve recipients. Mice were also monitored for abnormalities in mammary gland morphology and function, including tumor formation. PLD-treated FVB/N mice displayed histomorphologic changes and a significant reduction in the outgrowth potential of cells from the mammary glands. Thus, i.duc PLD administration altered the mammary gland structurally and functionally by reducing the MaSC population, which could compromise milk production. Followed long term, i.duc PLD-treated FVB/N mice developed malignant mammary tumors, confirming similar published findings on doxorubicin injected into the mammary gland of rats. Unless there are fundamental species differences in PLD metabolism in rodents and humans, this finding seriously limits the consideration of i.duc PLD use in the clinic for treatment or prevention of breast cancer.
机译:以前,我们已经表明,将Pegymated脂质体DOXORUBICIN(PLD)施用给HER2 / NEU转基因小鼠的内部(I.DUC)施用与乳腺肿瘤回归和预防相关。我们研究了探讨了保护潜在的保护的机制:研究了I.DUC PLD治疗的影响,随后怀孕了HER2 / Neu小鼠的肿瘤过剩;是否通过普通乳腺干细胞(MASC)的变化部分地介导I.DUC PLD抗肿瘤效应;以及I.DUC PLD的长期安全性进入正常的小鼠乳腺。 Her2 / Neu小鼠用两只I. DUC注射了四周的PLD治疗;诱导妊娠,并随访小鼠进行生理学的变化和肿瘤形成。我们发现所有出生于I. DUC的幼苗治疗的Her2 / Neu小鼠在出生后7天内没有重量增长。尽管怀孕额外怀孕,与载体控制PLD治疗的Her2 / Neu小鼠相比具有显着更长的潜伏期和肿瘤发育频率。分析了从未治疗的乳腺上皮细胞和I.DUC PLD治疗的6-8个月左右的多体式FVB / N小鼠进行了乳腺脂肪垫的重新释放能力。还监测小鼠的乳腺形态和功能异常,包括肿瘤形成。 PLD处理的FVB / N小鼠展示了组织形态的变化和来自乳腺细胞的产卵潜力的显着降低。因此,I.DUC PLD施用通过减少麦克斯卡斯人来改变结构上和功能性地改变乳腺,这可能会损害牛奶生产。其次是长期,I.DUC PLD治疗的FVB / N小鼠发育恶性乳腺癌,确认在对大鼠乳腺注入的多柔比星中的类似已发表的结果。除非在啮齿动物和人类中有基本物种差异,否则这一发现严重限制了I.duc PLD在临床治疗或预防乳腺癌中的考虑。

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