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Hierarchical design of a polymeric nanovehicle for efficient tumor regression and imaging

机译:分层设计的聚合物nanovehicle高效的肿瘤回归和成像

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摘要

Effective delivery of therapeutics to disease sites significantly contributes to drug efficacy, toxicity and clearance. Here we designed a hierarchical polymeric nanoparticle structure for anti-cancer chemotherapy delivery by utilizing state-of-the-art polymer chemistry and co-assembly techniques. This novel structural design combines the most desired merits for drug delivery in a single particle, including a long in vivo circulation time, inhibited non-specific cell uptake, enhanced tumor cell internalization, pH-controlled drug release and simultaneous imaging. This co-assembled nanoparticle showed exceptional stability in complex biological media. Benefiting from the synergistic effects of zwitterionic and multivalent galactose polymers, drug-loaded nanoparticles were selectively internalized by cancer cells rather than normal tissue cells. In addition, the pH-responsive core retained their cargo within their polymeric coating through hydrophobic interaction and released it under slightly acidic conditions. In vivo pharmacokinetic studies in mice showed minimal uptake of nanoparticles by the mononuclear phagocyte system and excellent blood circulation half-lives of 14.4 h. As a result, tumor growth was completely inhibited and no damage was observed for normal organ tissues. This newly developed drug nanovehicle has great potential in cancer therapy, and the hierarchical design principle should provide valuable information for the development of the next generation of drug delivery systems.
机译:有效的治疗疾病网站大大有助于药物功效,毒性和间隙。分层聚合物纳米结构抗癌化疗提供利用最先进的高分子化学和co-assembly技术。为药物设计结合了最理想的优点交付在一个粒子,包括一个长体内循环时间,抑制非特异性细胞吸收,增强肿瘤细胞内化,pH-controlled药物释放和同步成像。在复杂的生物异常稳定媒体。两性离子聚合物和多价半乳糖,药物纳米颗粒被选择性地由肿瘤细胞内化而不是正常的组织细胞。保留他们的货物在聚合物通过疏水作用和涂层在微酸性条件下释放它。在小鼠体内的药代动力学研究最小的纳米颗粒的吸收单核吞噬细胞系统和优秀的血液循环半衰期为14.4 h。因此,完全抑制了肿瘤的生长,也没有观察破坏正常组织器官。这个新开发的药物nanovehicle已经好了癌症治疗的潜力,和分层设计原则应该提供有价值的信息发展的未来一代的药物输送系统。

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