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Targeting combinations of liposomal drugs to both tumor vasculature cells and tumor cells for the treatment of HER2-positive breast cancer

机译:将脂质体药物靶向肿瘤血管系统细胞和肿瘤细胞靶向治疗HER2阳性乳腺癌

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Purpose: We used two ligand-modified liposomal drugs to selectively deliver two different chemotherapeutics to tumor cells (TC) and tumor vasculature endothelial (TV) cells, and examined the therapeutic effect of altering the order of treatment administration, and the effect of the temporal spacing of the treatments on the accumulation of a second dose of liposomes and therapeutic activity. Methods: Studies were completed in an orthotopic mouse model of human epidermal growth factor receptor 2 (HER2)-positive breast cancer, utilizing liposomal doxorubicin, targeted to TC via αHER2 Fab′ fragments, and liposomal vincristine, targeted to CD13 on TV cells via NGR peptides. Results and discussion: Combination treatment with TV-targeted plus TC-targeted therapies was therapeutically superior to either single agent; switching the order of administration of the combination did not alter treatment efficacy. The tumor accumulation of a second dose of liposomes was increased if administered at 4 days after pre-treatment with TV-targeted therapy. Using a treatment schedule exploiting this increase, the dose of simultaneously administered combination therapy was halved without compromising therapeutic effect. Conclusion: Proof-of-concept studies revealed the therapeutic potential of a dual-targeted two drug approach against HER2-positive breast cancer, and may be applicable to the treatment of other solid tumors.
机译:目的:我们使用两种配体修饰的脂质体药物选择性地向肿瘤细胞(TC)和肿瘤血管系统内皮(TV)细胞提供两种不同的化学治疗药物,并研究了改变治疗顺序的治疗效果以及颞叶的治疗效果。在第二剂量脂质体的积累上治疗间隔和治疗活性。方法:在人类表皮生长因子受体2(HER2)阳性乳腺癌的原位小鼠模型中,通过脂质体阿霉素(通过αHER2Fab'片段靶向TC)和脂质体长春新碱(通过NGR在TV细胞上靶向CD13)完成了研究肽。结果与讨论:以电视为靶点和以TC为靶点的疗法的联合治疗在治疗上优于任何一种药物。改变组合的给药顺序不会改变治疗效果。如果在电视靶向疗法的治疗前4天给药,第二剂量脂质体的肿瘤蓄积会增加。使用利用这种增加的治疗方案,将同时施用的联合疗法的剂量减半而不损害治疗效果。结论:概念验证研究显示了双重靶向两种药物治疗HER2阳性乳腺癌的治疗潜力,并且可能适用于其他实体瘤的治疗。

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