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PEG-聚(胺-硫醚酯)的酶合成作为高效的 pH 和 ROS 双重响应的纳米载体用于抗癌药物输送。

Enzymatic synthesis of PEG-poly(amine-co-thioether esters) as highly efficient pH and ROS dual-responsive nanocarriers for anticancer drug delivery.

机构信息

School of Biomedical Engineering, Sun Yat-sen University, Guangzhou, Guangdong 510275, China.

出版信息

J Mater Chem B. 2019 Jan 28;7(4):651-664. doi: 10.1039/c8tb02882f. Epub 2019 Jan 8.

DOI:10.1039/c8tb02882f
PMID:32254798
Abstract

Novel multifunctional drug nanocarriers have been successfully fabricated from a new type of enzymatically synthesized, biodegradable block copolymer, PEG-poly(ω-pentadecalactone-co-N-methyldiethyleneamine-co-3,3'-thiodipropionate) (PEG-PPMT), which was responsive to tumor-relevant acidic pH (5.0-6.5) and intracellular reactive oxygen species (ROS) of tumor cells. The PEG-PPMT copolymers could self-assemble to form nano-scaled particles in aqueous solutions, which are stable in physiological solutions, but swell substantially upon reducing the pH from 7.4 to 5.0 and/or in the presence of ROS on account of the protonation of the tertiary amino groups and oxidation of the thioether groups, causing a hydrophobic to hydrophilic transition in the nanoparticle cores. Consistently, docetaxel (DTX) encapsulated in PEG-PPMT nanoparticles can be triggered in a synergistic manner by acidic pH and a high-ROS environment in tumor cells to release the hydrophobic drug at accelerated rates for efficient tumor growth inhibition. In particular, DTX encapsulated in PEG-PPMT-11% PDL and PEG-PPMT-28% PDL nanoparticles exhibit extraordinarily enhanced potency (95% and 93% tumor-inhibiting efficiency, respectively) in inhibiting the growth of ROS-rich CT-26 tumors xenografted in mice. Importantly, biosafety analyses show minimal toxicity of DTX-loaded PEG-PPMT nanoparticles toward normal organs including liver and kidneys during the in vivo antitumor treatments. These results demonstrate that the PEG-PPMT nanoparticles are promising pH and ROS dual-responsive multifunctional nanocarriers for tumor site specific, controlled release of anticancer drugs to treat ROS-rich tumors.

摘要

新型多功能药物纳米载体由新型酶合成的可生物降解嵌段共聚物 PEG-聚(ω-十五内酯-co-N-甲基二亚乙基三胺-co-3,3'-二硫代二丙酸盐)(PEG-PPMT)成功制备,该嵌段共聚物对肿瘤相关的酸性 pH(5.0-6.5)和肿瘤细胞内的活性氧物种(ROS)具有响应性。PEG-PPMT 共聚物可以在水溶液中自组装形成纳米级颗粒,在生理溶液中稳定,但在 pH 从 7.4 降低到 5.0 时会显著膨胀,并且/或者在 ROS 的存在下,由于叔氨基质子化和硫醚基团氧化,纳米颗粒核心发生从疏水性到亲水性的转变。一致地,由于酸性 pH 和肿瘤细胞中高 ROS 环境的协同作用,DTX 包封在 PEG-PPMT 纳米颗粒中可以以加速的速度触发释放疏水性药物,从而有效抑制肿瘤生长。特别是,DTX 包封在 PEG-PPMT-11%PDL 和 PEG-PPMT-28%PDL 纳米颗粒中,对富 ROS 的 CT-26 肿瘤异种移植小鼠的生长表现出非凡的增强效力(分别为 95%和 93%的肿瘤抑制效率)。重要的是,生物安全性分析表明,在体内抗肿瘤治疗期间,载有 DTX 的 PEG-PPMT 纳米颗粒对包括肝脏和肾脏在内的正常器官的毒性最小。这些结果表明,PEG-PPMT 纳米颗粒是一种有前途的 pH 和 ROS 双重响应多功能纳米载体,可用于在肿瘤部位特异性、控制释放抗癌药物以治疗富 ROS 肿瘤。

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