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Drugs in development for tuberculosis.正在研发中的结核病药物。
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Molecular implications in the nanoencapsulation of the anti-tuberculosis drug rifampicin within flower-like polymeric micelles.纳米包裹抗结核药物利福平于花状聚合物胶束中的分子意义。
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Polymeric micelles for parenteral delivery of sagopilone: physicochemical characterization, novel formulation approaches and their toxicity assessment in vitro as well as in vivo.聚轮烷胶束用于萨格匹隆的注射给药:理化特性表征、新制剂方法及其在体外表征和体内评估。
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Freeze thaw: a simple approach for prediction of optimal cryoprotectant for freeze drying.冻融:预测冷冻干燥最佳冷冻保护剂的简单方法。
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Efavirenz-loaded polymeric micelles for pediatric anti-HIV pharmacotherapy with significantly higher oral bioavailability [corrected].载有依非韦伦的聚合物胶束用于儿科抗 HIV 治疗,可显著提高口服生物利用度[更正]。
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载利福平花状聚合物胶束的 cryoprotection-冻干和物理稳定化。

Cryoprotection-lyophilization and physical stabilization of rifampicin-loaded flower-like polymeric micelles.

机构信息

The Group of Biomaterials and Nanotechnology for Improved Medicines (BIONIMED), Department of Pharmaceutical Technology, Faculty of Pharmacy and Biochemistry, University of Buenos Aires, Buenos Aires 1113, Argentina.

出版信息

J R Soc Interface. 2012 Mar 7;9(68):487-502. doi: 10.1098/rsif.2011.0414. Epub 2011 Aug 24.

DOI:10.1098/rsif.2011.0414
PMID:21865255
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3262430/
Abstract

Rifampicin-loaded poly(ε-caprolactone)-b-poly(ethylene glycol)-poly(ε-caprolactone) flower-like polymeric micelles display low aqueous physical stability over time and undergo substantial secondary aggregation. To improve their physical stability, the lyoprotection-lyophilization process was thoroughly characterized. The preliminary cryoprotectant performance of mono- and disaccharides (e.g. maltose, glucose), hydroxypropyl-β-cyclodextrin (HPβCD) and poly(ethylene glycol) (PEG) of different molecular weights was assessed in freeze-thawing assays at -20°C, -80°C and -196°C. The size and size distribution of the micelles at the different stages were measured by dynamic light scattering (DLS). A cryoprotectant factor (f(c)) was determined by taking the ratio between the size immediately after the addition of the cryoprotectant and the size after the preliminary freeze-thawing assay. The benefit of a synergistic cryoprotection by means of saccharide/PEG mixtures was also assessed. Glucose (1 : 20), maltose (1 : 20), HPβCD (1 : 5) and glucose or maltose mixtures with PEG3350 (1 : 20) (copolymer:cryoprotectant weight ratio) were the most effective systems to protect 1 per cent micellar systems. Conversely, only HPβCD (1 : 5) cryoprotected more concentrated drug-loaded micelles (4% and 6%). Then, those micelle/cryoprotectant systems that displayed f(c) values smaller than 2 were freeze-dried. The morphology of freeze-dried powders was characterized by scanning electron microscopy and atomic force microscopy and the residual water content analysed by the Karl Fisher method. The HPβCD-added lyophilisates were brittle porous cakes (residual water was between 0.8% and 3%), easily redispersable in water to form transparent systems with a minimal increase in the micellar size, as determined by DLS.

摘要

载利福平的聚(ε-己内酯)-b-聚(乙二醇)-聚(ε-己内酯)花状聚合物胶束在长时间内表现出低的水物理稳定性,并经历大量的二次聚集。为了提高其物理稳定性,对其冷冻保护-冷冻干燥过程进行了彻底的表征。在-20°C、-80°C 和-196°C 的冻融试验中,评估了单糖和二糖(如麦芽糖、葡萄糖)、羟丙基-β-环糊精(HPβCD)和不同分子量的聚乙二醇(PEG)的初步冷冻保护剂性能。通过动态光散射(DLS)测量胶束在不同阶段的粒径和粒径分布。通过将添加冷冻保护剂后立即的粒径与初步冻融试验后的粒径之比,确定冷冻保护剂因子(f(c))。还评估了通过糖/PEG 混合物协同冷冻保护的益处。葡萄糖(1:20)、麦芽糖(1:20)、HPβCD(1:5)和葡萄糖或麦芽糖与 PEG3350(1:20)的混合物(共聚物:冷冻保护剂重量比)是保护 1%胶束系统的最有效体系。相反,只有 HPβCD(1:5)能保护更浓的载药胶束(4%和 6%)。然后,将那些 f(c)值小于 2 的胶束/冷冻保护剂体系进行冷冻干燥。通过扫描电子显微镜和原子力显微镜对冷冻干燥粉末的形态进行了表征,并通过卡尔费休法分析了残余水分含量。添加 HPβCD 的冻干粉末为易碎的多孔蛋糕(残余水分在 0.8%至 3%之间),在水中容易再分散,形成透明体系,通过 DLS 测定,胶束粒径仅有微小增加。