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首页> 外文期刊>Expert opinion on drug delivery >One-step solid-oil-water emulsion for sustained bioactive ranibizumab release
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One-step solid-oil-water emulsion for sustained bioactive ranibizumab release

机译:用于持续生物活性RANIBIZIMAB释放的一步固水 - 水乳液

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Background: The advent of therapeutic proteins highlights the need for delivery systems that protect and extend the duration of its action. Ranibizumab-VEGF is one such drug used for treating wet AMD. This paper describes a facile method to sustain bioactive ranibizumab release from PLGA-based particles. Methods: Two emulsion techniques were explored namely: water-in-oil-in-water (WOW) and solid-in-oil-in-water (SOW) emulsion. The bioactivity of ranibizumab was evaluated by comparing its binding capability to VEGF, measured with ELISA to total protein measured by microBCA. Results: During the emulsion process, contact of ranibizumab with the water-oil interface is the main destabilizing factor and this can be prevented with the use of amphiphilic PVA and solid-state protein in WOW and SOW emulsion respectively. In vitro release of the ranibizumab-loaded particles indicated that a 15-day release could be achieved with SOW particles while the WOW particles generally suffered from a burst release. Released ranibizumab was capable of inhibiting endothelial cell growth indicating its retention of bioactivity. The suppression of burst release from the SOW particles was attributed to the relatively smooth surface morphology of the SOW microparticles. Conclusions: The use of SOW encapsulation in modulating ranibizumab release while maintaining their bioactivity has been highlighted.
机译:背景:治疗性蛋白质的出现突出了需要保护和延长其行动持续时间的递送系统的需求。 Ranibizumab-Vegf是一种用于治疗湿AMD的这种药物。本文描述了一种从PLGA的粒子维持生物活性Ranibizumab释放的容易方法。方法:探索了两种乳液技术:水 - 水包装水(陶瓷)和固体水溶液(母猪)乳液。通过将其结合能力与VEGF的结合能力进行比较,用ELISA与Microbca测量的总蛋白质进行比较来评估Ranibizumab的生物活性。结果:在乳液过程中,Ranibizumab与水 - 油界面的接触是主要的稳定因子,并且可以分别使用哇和播种乳液中的两亲性PVA和固态蛋白来防止这种方法。 ranibizumab的释放的体外释放表明,可以用母猪颗粒实现15天的释放,同时通常遭受爆发释放的陶瓷颗粒。释放的Ranibizumab能够抑制内皮细胞生长,表明其保留生物活性。从母猪颗粒抑制爆发释放归因于母猪微粒的相对光滑的表面形态。结论:在调制Ranibizumab发布时使用播种源的使用,同时突出了它们的生物活性。

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