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Pectin and Zinc Alginate: The Right Inner/Outer Polymer Combination for Core-Shell Drug Delivery Systems

机译:果胶和藻酸锌:适用于核-壳药物传递系统的内/外聚合物组合

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摘要

Core-shell beads loaded with betamethasone were developed using co-axial prilling as production technique and pectin plus alginate as polymeric carriers. During this study, many operative conditions were intensively investigated to find the best ones necessary to produce uniform core-shell particle systems in a reproducible way. Particularly, feed solutions’ composition, polymers mass ratios and the effect of the main process parameters on particles production, micromeritics, inner structure, drug loading and drug-release/swelling profiles in simulated biological fluids were studied. The optimized core-shell formulation F5 produced with a pectin core concentration of 4.0% and an alginate shell concentration of 2.0% (2:1 core:shell ratio) acted as a sustained drug delivery system. It was able to reduce the early release of the drug in the upper part of the gastro-intestinal tract for the presence of the zinc-alginate gastro-resistant outer layer and to specifically deliver it in the colon, thanks to the selectivity of amidated low methoxy pectin core for this district. Therefore, these particles may be proposed as colon targeted drug delivery systems useful for inflammatory bowel disease (IBD) therapy.
机译:负载倍他米松的核-壳珠子是使用同轴造粒技术生产的,果胶加藻酸盐作为聚合物载体的开发。在这项研究中,对许多操作条件进行了深入研究,以找到以可再现的方式生产均匀的核-壳颗粒系统所需的最佳条件。特别地,研究了进料溶液的组成,聚合物的质量比以及主要工艺参数对模拟生物流体中颗粒产生,微分子论,内部结构,载药量和药物释放/溶胀曲线的影响。果胶核心浓度为4.0%,藻酸盐壳浓度为2.0%(核壳比为2:1)生产的优化核壳配方F5可以作为持续的药物输送系统。由于存在酰胺化的低蛋白的选择性,它能够减少药物在胃肠道上部的早期释放,从而能够抵抗藻酸锌的胃外层,并能将其特异性地递送到结肠中。该区为甲氧基果胶芯。因此,这些颗粒可以被提议作为用于炎症性肠病(IBD)疗法的结肠靶向药物递送系统。

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