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Hyaluronic acid coated poly(butyl cyanoacrylate) nanoparticles as anticancer drug carriers.

机译:透明质酸涂层的聚(氰基丙烯酸丁酯)纳米颗粒作为抗癌药物载体。

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The hyaluronic acid (HA) coated poly(butyl cyanoacrylate) (PBCA) nanoparticles were synthesized through radical polymerization of butyl cyanoarylate (BCA) initiated by cerium ions in the presence of HA. The chemical coupling between HA and PBCA was demonstrated by FTIR, (1)H NMR and X-ray diffraction. The sizes of the nanoparticles with different HA/BCA ratios were 291-325 nm at cerium concentration of 0.8 mmol/L and HA molecular weight of 18,000 Da. Paclitaxel (PTX), a model anticancer drug, was encapsulated in negatively charged nanoparticles with a maximal encapsulation efficiency of 90%. In vitro release demonstrated that HA modification could effectively reduce the initial burst release in the first 10h and provide a sustained release in the subsequent 188 h. As evidenced by the hemolysis assay and MTT assay, HA coating could significantly reduce the cytotoxicity. Cellular uptake indicated that uptake of HA-PBCA nanoparticles by Sarcoma-180 (S-180) cells was 9.5-fold higher than that of PBCA nanoparticles. PTX-loaded HA-PBCA nanoparticles were more potent in tumor growth suppression than PTX-loaded PBCA nanoparticles or PTX injection following intravenous administration to S-180 tumor bearing mice. Therefore, the HA-PBCA nanoparticles could be an effective and safe vehicle for systemic administration of hydrophobic anticancer drugs.
机译:透明质酸(HA)包覆的聚氰基丙烯酸丁酯(PBCA)纳米粒子是通过在HA存在下由铈离子引发的氰基芳基丙烯酸酯(BCA)自由基聚合而合成的。 HA和PBCA之间的化学偶联通过FTIR,(1)H NMR和X射线衍射证明。在铈浓度为0.8 mmol / L和HA分子量为18,000 Da的情况下,具有不同HA / BCA比的纳米粒子的尺寸为291-325 nm。紫杉醇(PTX)是一种抗癌药物,被封装在带负电荷的纳米粒子中,最大封装效率为90%。体外释放表明,HA修饰可在头10h内有效减少初始突释释放,并在随后的188h内提供持续释放。如溶血试验和MTT试验所证明,HA涂层可显着降低细胞毒性。细胞摄取表明肉瘤-180(S-180)细胞摄取HA-PBCA纳米颗粒比PBCA纳米颗粒摄取高9.5倍。在向具有S-180肿瘤的小鼠静脉内给药后,负载PTX的HA-PBCA纳米颗粒比负载PTX的PBCA纳米颗粒或PTX注射更有效地抑制肿瘤生长。因此,HA-PBCA纳米颗粒可能是疏水性抗癌药物全身给药的有效和安全的载体。

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