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首页> 外文期刊>Molecular pharmaceutics >Preparation of chondroitin sulfate-g-poly(ε-caprolactone) copolymers as a CD44-targeted vehicle for enhanced intracellular uptake
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Preparation of chondroitin sulfate-g-poly(ε-caprolactone) copolymers as a CD44-targeted vehicle for enhanced intracellular uptake

机译:硫酸软骨素-g-聚(ε-己内酯)共聚物的制备作为靶向CD44的载体,可增强细胞内摄取

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Chondroitin sulfate-g-poly(ε-caprolactone) (CP) copolymers were synthesized via atom transfer radical addition (ATRA). The CP copolymers self-assembled into micelles in water, and the micelles could be used to encapsulate a hydrophobic anticancer drug, camptothecin (CPT), in the core for tumor targeting delivery. The physicochemical properties of the micelles and CPT-loaded micelles were thoroughly characterized. For the in vitro test, the CPT release, the protection of the lactone ring of CPT from hydrolysis and the cellular uptake of CPT were studied. The cell-killing and apoptosis-inducing effects using the CPT-loaded micelles were significantly better than using free CPT against CRL-5802 cells. The micellar internalization into CRL-5802 cells was primarily via CD44 and clathrin dual-mediated endocytosis. For the in vivo test, the therapeutic efficacy of the CPT-loaded micelles was studied in a non-small-cell lung cancer xenograft animal model. The CPT-loaded micelles showed good inhibition in tumor growth as compared with a commercial product, CPT-11, in CRL-5802 tumor-bearing mice. The in vitro and in vivo data suggested the CP-based micelles are promising anticancer drug vehicles for lung cancer targeting.
机译:通过原子转移自由基加成(ATRA)合成硫酸软骨素-g-聚(ε-己内酯)(CP)共聚物。 CP共聚物在水中自组装成胶束,该胶束可用于将疏水性抗癌药喜树碱(CPT)包裹在核心中,以靶向肿瘤。胶束和载有CPT的胶束的理化特性得到了彻底的表征。为了进行体外测试,研究了CPT的释放,CPT内酯环的水解保护和CPT的细胞摄取。使用载有CPT的胶束对细胞杀伤和诱导凋亡的作用明显优于使用游离CPT对CRL-5802细胞的杀伤和凋亡诱导作用。胶束内在化进入CRL-5802细胞的过程主要是通过CD44和网格蛋白双重介导的内吞作用。对于体内测试,在非小细胞肺癌异种移植动物模型中研究了加载了CPT的胶束的治疗效果。与市售产品CPT-11相比,载有CPT的胶束在带有CRL-5802荷瘤的小鼠中显示出对肿瘤生长的良好抑制作用。体外和体内数据表明,基于CP的胶束有望成为靶向肺癌的抗癌药物。

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