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聚乙二醇交联多臂聚(ε-苄氧羰基-L-赖氨酸)作为超两亲性分子:合成、自组装及其作为疏水性药物有效传递系统的评价。

Poly(ethylene glycol) crosslinked multi-armed poly(ε-benzyloxycarbonyl-L-lysine)s as super-amphiphiles: Synthesis, self-assembly, and evaluation as efficient delivery systems for poorly water-soluble drugs.

机构信息

Shantou University Medical College, 22 Xinling Road, Shantou 515041, China; School of Pharmaceutical Sciences, Sun Yat-Sen University, University Town, Guangzhou 510006, China.

Shantou University Medical College, 22 Xinling Road, Shantou 515041, China.

出版信息

Colloids Surf B Biointerfaces. 2019 Oct 1;182:110384. doi: 10.1016/j.colsurfb.2019.110384. Epub 2019 Jul 23.

DOI:10.1016/j.colsurfb.2019.110384
PMID:31357126
Abstract

Polymeric micelles with high thermodynamic stability and loading capacity are of tremendous significance for their potential applications in drug delivery. In the present study, super-amphiphiles in the form of poly(ethylene glycol)-crosslinked multi-armed polyethylenimine-g-poly(ε-benzyloxycarbonyl-L-lysine)s (PEZ-alt-PEG) were designed, synthesized, and optimized as nanocarriers for hydrophobic drugs. In an aqueous solution, the copolymer PEZ-alt-PEG self-assembled into sub-100-nm spherical shell crosslinked micelles with low toxicity in vitro and in vivo. The crosslinked super-amphiphilic structure of PEZ-alt-PEG could not only enhance the thermodynamic stability of polymeric micelles, but it could also significantly improve the loading capacity of hydrophobic drugs, such as curcumin (CUR). CUR-loaded PEZ-alt-PEG micelles could mediate effective drug delivery with sustained and complete CUR release. The use of PEZ-alt-PEG micellar nanocarriers remarkably improved the cellular uptake of CUR and therefore exhibited effective inhibitory activity on the growth of human hepatoma (HepG2) cells. Compared to free CUR, CUR-loaded polymeric micelles significantly accelerated the apoptosis rate of HepG2 cells. Therefore, PEZ-alt-PEG polymeric micelles, with their high thermodynamic stability, high drug-loading capacity, enhanced drug uptake and improved pharmacodynamic effects, could serve as efficient and promising nanocarriers for poorly water-soluble drugs.

摘要

具有高热力学稳定性和载药能力的聚合物胶束对于其在药物传递中的潜在应用具有重要意义。在本研究中,设计、合成并优化了超两亲性聚合物聚乙二醇交联多臂聚乙烯亚胺-g-聚(ε-苄氧羰基-L-赖氨酸)(PEZ-alt-PEG)作为疏水性药物的纳米载体。在水溶液中,共聚物 PEZ-alt-PEG 自组装成具有低毒性的亚 100nm 球形壳交联胶束,无论是在体外还是体内。PEZ-alt-PEG 的交联超两亲结构不仅可以增强聚合物胶束的热力学稳定性,还可以显著提高疏水性药物的载药量,如姜黄素(CUR)。载有 CUR 的 PEZ-alt-PEG 胶束可以介导有效的药物传递,实现 CUR 的持续和完全释放。使用 PEZ-alt-PEG 胶束纳米载体可显著提高 CUR 的细胞摄取率,从而对人肝癌(HepG2)细胞的生长表现出有效的抑制活性。与游离 CUR 相比,载药聚合物胶束可显著提高 HepG2 细胞的凋亡率。因此,PEZ-alt-PEG 聚合物胶束具有高热力学稳定性、高载药能力、增强的药物摄取和改善的药效学作用,可作为治疗疏水性差的药物的有效且有前途的纳米载体。

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