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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Complexation hydrogels for intestinal delivery of interferon beta and calcitonin
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Complexation hydrogels for intestinal delivery of interferon beta and calcitonin

机译:用于肠内干扰素β和降钙素递送的络合水凝胶

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摘要

Recent studies have suggested that complexation hydrogels poly(methacrylic acid-g-ethylene glycol) (henceforth designated as P(MAA-g-EG)) exhibit high insulin incorporation efficiency. rapid insulin release in the intestine based on their pH-dependent complexation properties, enzyme-inhibiting effects and mucoadhesive characteristics. Therefore, they are promising carriers for insulin delivery via an oral route. As we designed these hydrogels as carriers suitable for oral administration of various peptide/protein drugs, in this study we aimed at investigating the applicability of P(MAA-g-EG) hydrogels to improving the intestinal absorption of various peptide/protein drugs. High loading efficiency into hydrogels was observed for insulin, calcitonin, and interferon beta. In addition, polymer microparticles loaded with calcitonin and interferon beta exhibited complexation/decomplexation and pH-sensitive release behavior. The molecular weight and chemical structure appeared to affect the efficiency of loading and release depending on the peptides and proteins. Furthermore, a drastic reduction of plasma calcium concentration accompanied by calcium absorption and a dose-dependent enhancement of plasma interferon beta concentration were observed after the administration of particles loaded with calcitonin or interferon beta into closed rat ileal segments. These findings indicate that P(MAA-g-EG) hydrogels are promising carriers for administration of various peptides; and proteins via an oral route.
机译:最近的研究表明,络合水凝胶聚(甲基丙烯酸-g-乙二醇)(以下称为P(MAA-g-EG))表现出很高的胰岛素掺入效率。根据其pH依赖的络合特性,酶抑制作用和粘膜粘附特性​​,可在肠道中快速释放胰岛素。因此,它们是有望通过口服途径输送胰岛素的载体。由于我们将这些水凝胶设计为适合口服各种肽/蛋白质药物的载体,因此在本研究中,我们旨在研究P(MAA-g-EG)水凝胶对改善各种肽/蛋白质药物的肠道吸收的适用性。对于胰岛素,降钙素和干扰素β,观察到在水凝胶中的高负载效率。此外,负载降钙素和干扰素β的聚合物微粒表现出络合/分解和pH敏感的释放行为。分子量和化学结构似乎影响加载和释放的效率,具体取决于肽和蛋白质。此外,在封闭的大鼠回肠段中施用降钙素或干扰素β颗粒后,可观察到血浆钙浓度急剧下降并伴有钙吸收,血浆中干扰素β浓度呈剂量依赖性增加。这些发现表明,P(MAA-g-EG)水凝胶是用于各种肽的有前途的载体。和蛋白质通过口服途径。

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