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Chitosan-Coated Flexible Liposomes Magnify the Anticancer Activity and Bioavailability of Docetaxel: Impact on Composition

机译:壳聚糖包衣的柔性脂质体放大了多西他赛的抗癌活性和生物利用度:对组成的影响

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摘要

Flexible liposomes (FLs) were developed as promising nano-carriers for anticancer drugs. Coating them with chitosan (CS) could improve their drug delivery properties. The aim of this study was to investigate the physicochemical characteristics, pharmacokinetics behavior, and cytotoxic efficacy of docetaxel (DTX)-loaded CS-coated FLs (C-FLs). DTX-loaded FLs and C-FLs were produced via thin-film evaporation and electrostatic deposition methods, respectively. To explore their physicochemical characterization, the particle size, zeta potential, encapsulation efficiency (EE%), morphology, and DTX release profiles were determined. In addition, pharmacokinetic studies were performed, and cytotoxic effect was assessed using colon cancer cells (HT29). Various FLs, dependent on the type of surfactant, were formed with particle sizes in the nano-range, 137.6 ± 6.3 to 238.2 ± 14.2 nm, and an EE% of 59–94%. Moreover, the zeta potential shifted from a negative to a positive value for C-FL with increased particle size and EE%, and the in vitro sustained-release profiles of C-FL compared to those of FL were evident. The optimized C-FL containing sodium deoxycholate (NDC) and dicetyl phosphate (DP) elicited enhanced pharmacokinetic parameters and cytotoxic efficiency compared to those of the uncoated ones and Onkotaxel®. In conclusion, this approach offers a promising solution for DTX delivery.
机译:柔性脂质体(FLs)被开发为抗癌药物的有前途的纳米载体。用壳聚糖(CS)涂层可以改善其药物传递性能。这项研究的目的是调查装载多西他赛(DTX)的CS涂层FL(C-FL)的理化特性,药代动力学行为和细胞毒性功效。分别通过薄膜蒸发和静电沉积方法生产DTX负载的FL和C-FL。为了探索其理化特性,确定了粒径,ζ电势,包封效率(EE%),形态和DTX释放曲线。此外,进行了药代动力学研究,并使用结肠癌细胞(HT29)评估了细胞毒性作用。取决于表面活性剂的类型,形成的各种FL的粒径在纳米范围内,为137.6±6.3至238.2±14.2 nm,EE%为59–94%。此外,随着粒径和EE%的增加,C-FL的ζ电位从负值转变为正值,并且与FL相比,C-FL的体外持续释放曲线很明显。与未包被和Onkotaxel ®相比,优化的含有脱氧胆酸钠(NDC)和双鲸蜡磷酸酯(DP)的C-FL可以提高药代动力学参数和细胞毒性效率。总之,这种方法为DTX交付提供了有希望的解决方案。

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