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Poly(styrene)-b-poly(DL-lactide) copolymer-based nanoparticles for anticancer drug delivery

机译:基于聚(苯乙烯)-b-聚(DL-丙交酯)共聚物的纳米颗粒用于抗癌药物的递送

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摘要

Poly(styrene)-b-poly(DL-lactide) (PS-PDLLA) copolymer-based nanoparticles (NPs) of a narrow size distribution, negative zeta potential, and spherical shape were fabricated for the delivery of docetaxel (DCT). The particle size was consistently maintained in serum for 24 hours and a sustained drug release pattern was observed for 10 days in the tested formulations. The cytotoxicity of the developed blank NPs was negligible in prostate cancer (PC-3) cells. Cellular uptake and distribution of the constructed NPs containing a hydrophobic fluorescent dye was monitored by confocal laser scanning microscopy (CLSM) for 24 hours. Anti-tumor efficacy of the PS-PDLLA/DCT NPs in PC-3 cells was significantly more potent than that of the group treated with commercially available DCT, Taxotere® (P<0.05). Blood biochemistry tests showed that no serious toxicity was observed with the blank NPs in the liver and kidney. In a pharmacokinetic study of DCT in rats, in vivo clearance of PS-PDLLA/DCT NPs decreased while the half-life in blood increased compared to the Taxotere-treated group (P<0.05). The PS-PDLLA NPs are expected to be a biocompatible and efficient nano-delivery system for anticancer drugs.
机译:制备具有窄尺寸分布,负ζ电位和球形的聚(苯乙烯)-b-聚(DL-丙交酯)(PS-PDLLA)共聚物基纳米颗粒(NPs),用于递送多西他赛(DCT)。粒径在血清中持续保持24小时,并且在测试的制剂中观察到持续的药物释放模式持续10天。在前列腺癌(PC-3)细胞中,开发的空白NP的细胞毒性可以忽略不计。通过共聚焦激光扫描显微镜(CLSM)监测24小时内含有疏水性荧光染料的NP的细胞摄取和分布。 PS-PDLLA / DCT NPs在PC-3细胞中的抗肿瘤效力比市售DCT Taxotere ®处理组显着更强(P <0.05)。血液生化测试表明,肝脏和肾脏中的空白NP没有观察到严重的毒性。在大鼠DCT的药代动力学研究中,与紫杉醇治疗组相比,PS-PDLLA / DCT NPs的体内清除率降低,而血液半衰期延长(P <0.05)。 PS-PDLLA NP有望成为生物相容且高效的抗癌药物纳米递送系统。

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