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Antitumor efficacy of Folic Acid conjugated Polymeric Nanoparticles of SN-38 after oral delivery

机译:叶酸偶联的SN-38纳米聚合物在口服后的抗肿瘤作用

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The objective of the present research was to develop folic acid conjugated polymeric nanoparticles (FCsPNP) and to investigate its therapeutic effectiveness in xenograft Colon tumor models after oral delivery. Chitosan coated PLGA nanoparticles (CsPNP) were prepared by polyelectrolyte complexation method and it was further conjugated with Folic acid. Optimized formulation was investigated for particle size, zeta potential, polydispersity index (PdI), % entrapment drug loading and in vitro release. The morphology was observed by SEM and TEM images. Tumor regression studies were conducted on Balb/c mice implanted with Colo-26 cells. FCsPNP were successfully prepared and optimized. In vitro parameters viz. Particle size, Zeta potential, PdI were found to be optimum. The in vitro % release is directly correlated with the nature of polymers and folate conjugation. In vivo tumor regression studies found the formulations to be less toxic than Irinotecan hydrochloride (IHCl). CsPNP and FCsPNP were successfully prepared and evaluated for antitumor efficacy after oral delivery. FCsPNP were more effective in the colon tumor treatment and found to be less toxic than IHCl thus making it a potential drug delivery candidate for future anticancer therapy.
机译:本研究的目的是开发叶酸共轭聚合物纳米颗粒(FCsPNP),并研究其在口服后异种移植结肠肿瘤模型中的治疗效果。通过聚电解质络合法制备了壳聚糖包覆的PLGA纳米粒子(CsPNP),并进一步与叶酸结合。研究了最佳配方的粒径,ζ电位,多分散指数(PdI),包封药物载量和体外释放。通过SEM和TEM图像观察形态。对植入了Colo-26细胞的Balb / c小鼠进行了肿瘤消退研究。 FCsPNP已成功制备和优化。体外参数发现粒度,Zeta电位,PdI是最佳的。体外%释放与聚合物和叶酸结合的性质直接相关。体内肿瘤消退研究发现,该制剂的毒性低于盐酸伊立替康(IHCl)。成功制备了CsPNP和FCsPNP并评估了口服给药后的抗肿瘤功效。 FCsPNP在结肠肿瘤治疗中更有效,并且毒性比IHCl低,因此使其成为将来抗癌治疗的潜在药物候选药物。

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