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Self-Regulated Multifunctional Collaboration of Targeted Nanocarriers for Enhanced Tumor Therapy

机译:靶向纳米载体的自调控多功能协作,用于增强肿瘤治疗

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Exploring ideal nanocarriers for drug delivery systems has encountered unavoidable hurdles, especially the conflict between enhanced cellular uptake and prolonged blood circulation, which have determined the final efficacy of cancer therapy. Here, based on controlled self-assembly, surface structure variation in response to external environment was constructed toward overcoming the conflict. A novel micelle with mixed shell of hydrophilic poly(ethylene glycol) PEG and pH responsive hydrophobic poly(β-amino ester) (PAE) was designed through the self-assembly of diblock amphiphilic copolymers. To avoid the accelerated clearance from blood circulation caused by the surface exposed targeting group c(RGDfK), here c(RGDfK) was conjugated to the hydrophobic PAE and hidden in the shell of PEG at pH 7.4. At tumor pH, charge conversion occurred, and c(RGDfK) stretched out of the shell, leading to facilitated cellular internalization according to the HepG2 cell uptake experiments. Meanwhile, the heterogeneous surface structure endowed the micelle with prolonged blood circulation. With the self-regulated multifunctional collaborated properties of enhanced cellular uptake and prolonged blood circulation, successful inhibition of tumor growth was achieved from the demonstration in a tumor-bearing mice model. This novel nanocarrier could be a promising candidate in future clinical experiments.
机译:探索用于药物输送系统的理想纳米载体遇到了不可避免的障碍,尤其是细胞摄取增加和血液循环时间延长之间的冲突,这决定了癌症治疗的最终功效。在此,基于受控的自组装,构造表面结构响应于外部环境的变化以克服冲突。通过二嵌段两亲共聚物的自组装,设计了一种具有亲水性聚乙二醇PEG和pH响应性疏水性聚β-氨基酯(PAE)混合壳的新型胶束。为了避免由表面暴露的靶向基团c(RGDfK)引起的血液循环加速清除,此处将c(RGDfK)与疏水性PAE偶联并隐藏在pH 7.4的PEG壳中。在肿瘤pH下,发生了电荷转化,并且c(RGDfK)从壳中伸出,从而根据HepG2细胞摄取实验促进了细胞内在化。同时,异质的表面结构使胶束具有延长的血液循环。具有增强的细胞摄取和延长的血液循环的自我调节的多功能协同性质,通过在荷瘤小鼠模型中的证明,成功抑制了肿瘤的生长。这种新型的纳米载体可能是未来临床实验中有希望的候选者。

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