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首页> 外文期刊>Journal of pharmaceutical sciences. >Development of a respirable, sustained release microcarrier for 5-fluorouracil II: In vitro and in vivo optimization of lipid coated nanoparticles.
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Development of a respirable, sustained release microcarrier for 5-fluorouracil II: In vitro and in vivo optimization of lipid coated nanoparticles.

机译:用于5-氟尿嘧啶II的可呼吸,缓释微载体的开发:脂质包覆纳米颗粒的体外和体内优化。

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摘要

The release rate of 5-fluorouracil (5-FU) from lipid-coated nanoparticles (LNPs) was determined to develop a respirable delivery system for use as adjuvant (postsurgery) therapy for lung cancer. LNPs were prepared by spray drying, and the in vitro release was measured by microdialysis. The composition of the core and shell affected the release rate. Increasing the core diameter at constant shell thickness and increasing shell thickness at constant core diameter reduced the release rate, suggesting that the lipid shell is the rate limiting step for the release of 5-FU. A model consisting of a sequential zero-order/first-order dependence on time from polydispersed cores within polydispersed shells was developed to describe the release. Based on studies of the effect of geometry of the layered particles, the optimal formulation was identified as a 600-nm diameter 5-FU/poly-(glutamic acid) core with a 200-nm thick tripalmitin/cetyl alcohol shell. This system is readily aerosolized by ultrasonic atomization, which did not change the release properties. Preliminary instillation and inhalation delivery studies to the hamster resulted in lung levels of the particles and 5-FU that were near the desired values. Through this effort, a sustained-release, respirable delivery system for adjuvant therapy of lung cancer in humans may ultimately be realized.
机译:确定了脂质包裹的纳米颗粒(LNP)中5-氟尿嘧啶(5-FU)的释放速率,以开发可呼吸的输送系统,用作肺癌的辅助治疗(手术后治疗)。通过喷雾干燥制备LNP,并通过微透析测量体外释放。核和壳的组成影响释放速率。在恒定的壳厚度下增加核直径,在恒定的壳直径下增加壳厚度会降低释放速率,这表明脂质壳是5-FU释放的速率限制步骤。建立了一个模型,该模型由多分散壳中的多分散核对时间的顺序零序/一阶依赖性组成,以描述释放。基于对层状颗粒几何形状影响的研究,确定了最佳配方,即直径为600 nm的5-FU /聚谷氨酸芯,外壳厚度为200 nm的三棕榈精蛋白/鲸蜡醇。该系统易于通过超声雾化雾化,而不会改变释放特性。对仓鼠的初步滴注和吸入递送研究结果表明,颗粒和5-FU的肺水平接近所需值。通过这种努力,可以最终实现用于肺癌的辅助治疗的缓释,可呼吸的递送系统。

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