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优化载环丙沙星复合物的 PLGA 纳米粒用于囊性纤维化肺部感染的治疗:实验设计方法。

Optimization of ciprofloxacin complex loaded PLGA nanoparticles for pulmonary treatment of cystic fibrosis infections: Design of experiments approach.

机构信息

MJR PharmJet GmbH, Industriestr. 1B, 66802 Überherrn, Germany; Biopharmaceutics and Pharmaceutical Technology, Department of Pharmacy, Saarland University, 66123 Saarbrücken, Germany.

MJR PharmJet GmbH, Industriestr. 1B, 66802 Überherrn, Germany.

出版信息

Int J Pharm. 2016 Dec 30;515(1-2):343-351. doi: 10.1016/j.ijpharm.2016.10.025. Epub 2016 Oct 12.

Abstract

Design of Experiments (DoE) is a powerful tool for systematic evaluation of process parameters' effect on nanoparticle (NP) quality with minimum number of experiments. DoE was employed for optimization of ciprofloxacin loaded PLGA NPs for pulmonary delivery against Pseudomonas aeruginosa infections in cystic fibrosis (CF) lungs. Since the biofilm produced by bacteria was shown to be a complicated 3D barrier with heterogeneous meshes ranging from 100nm to 500nm, nanoformulations small enough to travel through those channels were assigned as target quality. Nanoprecipitation was realized utilizing MicroJet Reactor (MJR) technology based on impinging jets principle. Effect of MJR parameters flow rate, temperature and gas pressure on particle size and PDI was investigated using Box-Behnken design. The relationship between process parameters and particle quality was demonstrated by constructed fit functions (R=0.9934 p<0.0001 and R=0.9983 p<0.0001, for particle size and PDI, respectively). Prepared nanoformulations varied between 145.2 and 979.8nm with PDI ranging from 0.050 to 1.00 and showed encapsulation efficiencies >65%. Response surface plots provided experimental data-based understanding of MJR parameters' effect, thus NP quality. Presented work enables ciprofloxacin loaded PLGA nanoparticle preparations with pre-defined quality to fulfill the requirements of local drug delivery under CF disease conditions.

摘要

实验设计(DoE)是一种强大的工具,可用于系统地评估工艺参数对纳米颗粒(NP)质量的影响,同时使用最少的实验次数。DoE 被用于优化载有环丙沙星的 PLGA NP 用于治疗囊性纤维化(CF)肺部铜绿假单胞菌感染的肺部给药。由于细菌产生的生物膜被证明是一种复杂的 3D 屏障,其异质网格尺寸范围从 100nm 到 500nm,因此纳米制剂的尺寸必须足够小才能通过这些通道,这被指定为目标质量。纳米沉淀是利用基于冲击射流原理的微射流反应器(MJR)技术实现的。使用 Box-Behnken 设计研究了 MJR 参数流速、温度和气压对粒径和 PDI 的影响。通过构建拟合函数(粒径的 R=0.9934 p<0.0001,PDI 的 R=0.9983 p<0.0001),证明了工艺参数与颗粒质量之间的关系。所制备的纳米制剂的粒径在 145.2nm 至 979.8nm 之间,PDI 范围在 0.050 至 1.00 之间,包封效率>65%。响应面图提供了基于实验数据的对 MJR 参数影响的理解,从而了解 NP 质量。本工作使载有环丙沙星的 PLGA 纳米颗粒制剂能够满足 CF 疾病条件下局部药物输送的要求,具有预定义的质量。

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