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Development of phosphorylated glucomannan-coated chitosan nanoparticles as nanocarriers for protein delivery

机译:磷酸化葡甘露聚糖涂层的壳聚糖纳米粒子作为蛋白质载体的纳米载体的开发。

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摘要

The aim of the present work was to develop a new nanoparticle carrier, adapted for the oral administration of proteins and their delivery to the immune system. Chitosan and phosphorylated glucomannan were chosen as major constituents of the nanoparticles. Chitosan nanoparticles were formed by ionic gelation and then coated with glucomannan. Two different protocols were adopted for the formation of the glucomannan coating: protocol I, in which chitosan nanoparticles were isolated before their coating; protocol II, in which chitosan nanoparticles were not isolated, but coated with glucomannan in the presence of free chitosan. The results showed that, under the selected formulation conditions, the sizes of the nanoparticles ranged between 170 and 300 nm and their zeta potential values were inverted from positive to negative by the glucomannan coating. The nanoparticles prepared by the two protocols could be freeze-dried, in the presence or absence of cryoprotective agents, preserving their original characteristics. The results of the stability study evidenced the positive role of the glucomannan coating in preventing the aggregation of the nanoparticles in buffered media. Finally, the association of the inmunomodulatory protein complex P1 to the chitosan-glucomannan nanoparticles was investigated. The results showed that the association was not dependent on the chitosan: sodium tripoliphosphate ratio, but it was significantly affected by the presence of sodium phosphate in the protein structure.
机译:本工作的目的是开发一种新的纳米颗粒载体,适用于蛋白质的口服给药及其向免疫系统的传递。选择壳聚糖和磷酸化葡甘露聚糖作为纳米颗粒的主要成分。通过离子凝胶形成壳聚糖纳米颗粒,然后用葡甘露聚糖包被。葡甘露聚糖涂层的形成采用两种不同的方案:方案I,其中壳聚糖纳米颗粒在涂层之前被分离;方案II,其中不分离壳聚糖纳米颗粒,而是在游离壳聚糖存在下用葡甘露聚糖包被。结果表明,在选定的配制条件下,纳米颗粒的大小在170至300 nm之间,并且其葡聚糖电位值通过葡甘露聚糖涂层从正反转为负。通过两种方案制备的纳米颗粒可以在存在或不存在冷冻保护剂的情况下冷冻干燥,保留其原始特性。稳定性研究的结果证明了葡甘露聚糖涂层在防止纳米颗粒在缓冲介质中聚集方面的积极作用。最后,研究了免疫调节蛋白复合物P1与壳聚糖-葡甘露聚糖纳米颗粒的缔合。结果表明,缔合关系不依赖于壳聚糖:三聚磷酸钠的比例,但受蛋白质结构中磷酸钠的存在影响很大。

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