An electrostatic layer-by-layer self-assembly technique was used to encapsulate solid core paclitaxel nanoparticles within a polymeric nanometer-scale shell. This approach provides a new strategy for the development of polymeric vehicles that control drug release and target diseased tissues and cells specific to the ailment, such as breast cancer. Core paclitaxel nanoparticles, 153 +/- 28 nm in diameter, were prepared using a modified nanoprecipitation technique. A nanoshell composed of multilayered polyelectrolytes, poly(allylamine hydrochloride) and poly(styrene-4-sulfonate) was assembled stepwise onto core charged drug nanoparticles. In vitro studies were performed to determine the anticancer activity of paclitaxel core-shell nanoparticles. Paclitaxel core-shell nanoparticles induced cell cycle arrest in the G2/M phase after 24 and 48 h of incubation with a human breast carcinoma cell line, MCF-7. Changes in MCF-7 cell morphology, fragmentation of the nucleus, and loss of cell-cell contacts indicated that the cells responded to paclitaxel core nanoparticles upon treatment for 24 and 48 h. Cells arrested in G2/M phase illustrated abnormal microtubule and actin cytoskeleton morphology. The core-shell drug nanoparticles fabricated using this procedure provide a new approach in the delivery of paclitaxel devoid of Cremophor EL, a solvent that causes adverse side effects in patients undergoing chemotherapy for treatment of metastasized mammary cancers.

译文

:静电逐层自组装技术用于将固体核紫杉醇纳米颗粒包裹在聚合物纳米级壳中。该方法为开发控制药物释放并靶向特定于疾病的患病组织和细胞(例如乳腺癌)的聚合物载体提供了新的策略。使用改良的纳米沉淀技术制备了直径153 /-28 nm的核心紫杉醇纳米颗粒。将由多层聚电解质,聚(烯丙胺盐酸盐)和聚(苯乙烯-4-磺酸盐)组成的纳米壳逐步组装到带核电荷的药物纳米颗粒上。进行了体外研究以确定紫杉醇核-壳纳米颗粒的抗癌活性。与人乳腺癌细胞系MCF-7孵育24和48小时后,紫杉醇核-壳纳米颗粒诱导了G2 / M期的细胞周期停滞。 MCF-7细胞形态的变化,细胞核的碎裂以及细胞与细胞之间的接触损失表明,处理24小时和48小时后,细胞对紫杉醇核心纳米颗粒有反应。在G2 / M期停滞的细胞说明微管和肌动蛋白细胞骨架形态异常。使用该程序制备的核-壳药物纳米颗粒为不含紫杉醇的紫杉醇的递送提供了一种新方法,紫杉醇不含Cremophor EL,该溶剂在接受化疗的转移性乳腺癌患者中引起不良副作用。

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