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首页> 外文期刊>Biomaterials >Tumor acidity-sensitive linkage-bridged block copolymer for therapeutic siRNA delivery
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Tumor acidity-sensitive linkage-bridged block copolymer for therapeutic siRNA delivery

机译:肿瘤酸性敏感键桥联嵌段共聚物,用于治疗性siRNA的递送

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The design of ideal nanoparticle delivery systems should be capable of meeting the requirements of several stages of drug delivery, including prolonged circulation, enhanced accumulation and penetration in the tumor, facilitated cellular internalization and rapid release of the active drug in the tumor cells. However, among the current design strategies, meeting the requirements of one stage often conflicts with the other. Herein, a tumor pH-labile linkage-bridged block copolymer of poly(ethylene glycol) with poly(lacide-co-glycolide) (PEG-Dlink(m)-PLGA) was used for siRNA delivery to fulfill all aforementioned requirements of these delivery stages. The obtained siRNA-encapsulating PEG-Dlink(m)-PLGA nanoparticle gained efficiently prolonged circulation in the blood and preferential accumulation in tumor sites via the PEGylation. Furthermore, the PEG surface layer was detached in response to the tumor acidic micro environment to facilitate cellular uptake, and the siRNA was rapidly released within tumor cells due to the hydrophobic PLGA layer. Hence, PEG-Dlink(m)-PLGA nanoparticles met the requirements of several stages of drug delivery, and resulted in the enhanced therapeutic effect of the nanoparticular delivery systems. (C) 2016 Elsevier Ltd. All rights reserved.
机译:理想的纳米颗粒递送系统的设计应能够满足药物递送几个阶段的要求,包括延长循环,增强在肿瘤中的积累和渗透,促进细胞内在化以及活性药物在肿瘤细胞中的快速释放。但是,在当前的设计策略中,满足一个阶段的要求通常会与另一个阶段发生冲突。在本文中,将聚乙二醇与聚(丙交酯-共-乙交酯)的肿瘤pH不稳定的键桥联嵌段共聚物(PEG-Dlink(m)-PLGA)用于siRNA递送,以满足这些递送的所有上述要求。阶段。所获得的包裹siRNA的PEG-Dlink(m)-PLGA纳米颗粒通过PEG化有效地延长了血液在血液中的循环并在肿瘤部位优先积累。此外,响应于肿瘤酸性微环境,PEG表面层脱离以促进细胞摄取,并且由于疏水性PLGA层,siRNA在肿瘤细胞内迅速释放。因此,PEG-Dlink(m)-PLGA纳米颗粒满足药物递送几个阶段的要求,并导致纳米颗粒递送系统的治疗效果增强。 (C)2016 Elsevier Ltd.保留所有权利。

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