Dual-pH Sensitive Charge-Reversal Polypeptide Micelles for Tumor-Triggered Targeting Uptake and Nuclear Drug Delivery

胶束 生物物理学 化学 药物输送 对偶(语法数字) 毒品携带者 药品 纳米技术 靶向给药 组合化学 药理学 材料科学 医学 生物 有机化学 水溶液 文学类 艺术
作者
Shisong Han,Ze‐Yong Li,Jingyi Zhu,Kai Han,Zhengyang Zeng,Wei Hong,Wenxin Li,Huizhen Jia,Yun Liu,Ren‐Xi Zhuo,Xian‐Zheng Zhang
出处
期刊:Small [Wiley]
卷期号:11 (21): 2543-2554 被引量:256
标识
DOI:10.1002/smll.201402865
摘要

A novel dual-pH sensitive charge-reversal strategy is designed to deliver antitumor drugs targeting to tumor cells and to further promote the nuclei internalization by a stepwise response to the mildly acidic extracellular pH (≈6.5) of a tumor and endo/lysosome pH (≈5.0). Poly(l-lysine)-block–poly(l-leucine) diblock copolymer is synthesized and the lysine amino residues are amidated by 2,3-dimethylmaleic anhydride to form β-carboxylic amide, making the polypeptides self-assemble into negatively charged micelles. The amide can be hydrolyzed when exposed to the mildly acidic tumor extracellular environment, which makes the micelles switch to positively charged and they are then readily internalized by tumor cells. A nuclear targeting Tat peptide is further conjugated to the polypeptide via a click reaction. The Tat is amidated by succinyl chloride to mask its positive charge and cell-penetrating function and thus to inhibit nonspecific cellular uptake. After the nanoparticles are internalized into the more acidic intracellular endo/lysosomes, the Tat succinyl amide is hydrolyzed to reactivate the Tat nuclear targeting function, promoting nanoparticle delivery into cell nuclei. This polypeptide nanocarrier facilitates tumor targeting and nuclear delivery simultaneously by simply modifying the lysine amino residues of polylysine and Tat into two different pH-sensitive β-carboxylic amides.
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