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Transformable nanoparticles triggered by cancer-associated fibroblasts for improving drug permeability and efficacy in desmoplastic tumors

机译:可变形的纳米粒子引发的癌症相关的成纤维细胞为提高药物渗透率和有效性在肿瘤多见

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摘要

Cancer-associated fibroblasts (CAFs) are important barriers for nanoparticles (NPs) to deeply penetrate into tumors and severely limit the antitumor efficacy of nanomedicines. Herein, we proposed a CAF-triggered transformable drug delivery system based on a cleavable peptide responsive to fibroblast activation protein-alpha (FAP-alpha) specifically overexpressed on the surface of CAFs. The NPs were composed of cationic poly(amidoamine) (PAMAM) dendrimers cross-linked by our designed peptide, a chemotherapeutical drug was incorporated onto PAMAM using disulfide bonds and finally, hyaluronic acid (HA) was conjugated to improve the tumor targetability as well as biocompatibility through electrostatic interactions. These NPs had an initial size of similar to 200 nm and negative zeta potential favorable for stable blood circulation; however, after docking with CAFs, they dissociated into smaller NPs and exposed the relative positive surface charge to facilitate penetration and enter the tumor cells together with CAFs. An interesting finding was that this system intracellularly released different levels of drugs in these two kinds of cells, which was beneficial for the disruption of the stromal barrier and increasing the local drug accumulation. Our investigation confirmed that the constructed system could alleviate the biological barriers and hold promising therapeutic efficiency for desmoplastic solid tumors.
机译:癌症相关的成纤维细胞(保护)是很重要的纳米粒子的障碍(NPs)渗透肿瘤,严重限制了抗肿瘤纳米药物的效果。提出了一个CAF-triggered可变形的药物交付系统基于可分裂的肽对成纤维细胞激活protein-alpha(FAP-alpha)专门上过表达战乱国家的表面。阳离子聚(amidoamine) (PAMAM)树枝状分子交联由我们设计的肽,chemotherapeutical成立到毒品PAMAM使用二硫键和最后,透明质酸(HA)是提高共轭肿瘤targetability以及生物相容性通过静电交互。类似于200 nm和消极的电动电势有利于稳定血液循环;与战乱国家对接后,他们分离较小的NPs和暴露了相对积极的促进渗透和表面电荷和战乱国家一起进入肿瘤细胞。有趣的发现是,这个系统细胞不同程度的释放这两种细胞中药物,有利于基质的破坏障碍,增加当地的药物积累。所构造的系统可以缓解生物屏障和承诺治疗效率多固体肿瘤。

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