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首页> 外文期刊>ACS nano >Synergistic targeting of cell membrane, cytoplasm, and nucleus of cancer cells using rod-shaped nanoparticles
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Synergistic targeting of cell membrane, cytoplasm, and nucleus of cancer cells using rod-shaped nanoparticles

机译:使用棒状纳米颗粒协同靶向癌细胞的细胞膜,细胞质和细胞核

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Design of carriers for effective delivery and targeting of drugs to cellular and subcellular compartments is an unmet need in medicine. Here, we report pure drug nanoparticles comprising camptothecin (CPT), trastuzumab (TTZ), and doxorubicin (DOX) to enable cell-specific interactions, subcellular accumulation, and growth inhibition of breast cancer cells. CPT is formulated in the form of nanorods which are coated with TTZ. DOX is encapsulated in the TTZ corona around the CPT nanoparticle. Our results show that TTZ/DOX-coated CPT nanorods exhibit cell-specific internalization in BT-474 breast cancer cells, after which TTZ is recycled to the plasma membrane, leaving CPT nanorods in the perinuclear region and delivering DOX into the nucleus of the cells. The effects of CPT-TTZ-DOX nanoparticles on growth inhibition are synergistic (combination index = 0.17 ± 0.03) showing 10-10 000-fold lower inhibitory concentrations (IC_(50)) compared to those of individual drugs. The design of antibody-targeted pure drug nanoparticles offers a promising design strategy to facilitate intracellular delivery and therapeutic efficiency of anticancer drugs.
机译:有效地递送药物并将药物靶向至细胞和亚细胞区室的载体设计是药物中尚未满足的需求。在这里,我们报告纯净的药物纳米颗粒,包括喜树碱(CPT),曲妥珠单抗(TTZ)和阿霉素(DOX),可实现乳腺癌细胞的细胞特异性相互作用,亚细胞蓄积和生长抑制。 CPT以纳米棒的形式配制,并涂有TTZ。 DOX封装在CPT纳米粒子周围的TTZ电晕中。我们的结果表明,涂​​覆TTZ / DOX的CPT纳米棒在BT-474乳腺癌细胞中表现出细胞特异性内在化,此后TTZ被回收到质膜,将CPT纳米棒保留在核周区域中,并将DOX传递到细胞核中。 CPT-TTZ-DOX纳米颗粒对生长抑制的作用具有协同作用(组合指数= 0.17±0.03),与单个药物相比,抑制浓度(IC_(50))低10-10倍。以抗体为靶标的纯药物纳米颗粒的设计提供了一种有希望的设计策略,以促进细胞内递送和抗癌药物的治疗效率。

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