首页> 外文期刊>International Journal of Pharmaceutics >Release modulation and cytotoxicity of hydroxycamptothecin-loaded electrospun fibers with 2-hydroxypropyl-beta-cyclodextrin inoculations.
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Release modulation and cytotoxicity of hydroxycamptothecin-loaded electrospun fibers with 2-hydroxypropyl-beta-cyclodextrin inoculations.

机译:用2-羟丙基-β-环糊精接种对羟基喜树碱负载的电纺纤维进行释放调节和细胞毒性。

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摘要

Hydroxycamptothecin (HCPT) is valid to various malignant tumors, but its insoluble and unstable lactone ring in physiological environment have restricted the clinic application. This work was aimed to formulate HCPT-loaded poly(DL-lactic acid)-poly(ethylene glycol) (PELA) fibrous mats through blend electrospinning with 2-hydroxypropyl-beta-cyclodextrin (HPCD) to modulate the drug release and matrix degradation, and to enhance the structural integrity and cytotoxicity of the released HCPT. The entire drug fraction retained its active lactone form within electrospun fibers, and that was maintained over 85% during incubation for over 1 month. A biphasic release pattern was determined for HCPT-loaded electrospun fibers, which can be modulated by the addition of HPCD. HPCD served as solubilizer to maintain a large concentration gradient for HCPT between saturation and diffusion, and liberated HPCD created microstructure of ultrafine fibers, leading a faster release profile in the second phase. In vitro cytotoxicity test showed over 7 times higher inhibitory activity against cancer cells for HCPT-loaded electrospun fibers than free drug during 72h incubation. Higher apoptosis rates and the arrest of the cell cycle during the S and G(2)/M phases were detected through flow cytometry analysis. It indicated therapeutic potentials of HCPT-loaded electrospun fibers as implantable anti-cancer agents for local chemotherapy.
机译:羟基喜树碱(HCPT)对各种恶性肿瘤均有效,但其在生理环境中的不溶性和不稳定的内酯环限制了其临床应用。这项工作旨在通过与2-羟丙基-β-环糊精(HPCD)混纺静电纺丝来调制负载HCPT的聚(DL-乳酸)-聚(乙二醇)(PELA)纤维毡,从而调节药物释放和基质降解,并增强释放的HCPT的结构完整性和细胞毒性。整个药物级分在电纺纤维中保留了其活性内酯形式,并且在孵育1个月以上的时间内保持了85%以上。确定了加载HCPT的电纺纤维的双相释放模式,可以通过添加HPCD对其进行调节。 HPCD用作增溶剂,以维持HCPT在饱和和扩散之间的较大浓度梯度,并且释放的HPCD形成了超细纤维的微观结构,从而导致第二阶段释放速度更快。体外细胞毒性测试显示,在72小时的孵育过程中,对HCPT负载的电纺丝纤维对癌细胞的抑制活性是游离药物的7倍以上。通过流式细胞仪分析检测到较高的凋亡率和S和G(2)/ M阶段的细胞周期的逮捕。它表明了加载HCPT的电纺纤维作为局部化疗的可植入抗癌剂的治疗潜力。

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