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胰岛素在作为口服给药载体的络合水凝胶中的体外释放行为及稳定性

In vitro release behavior and stability of insulin in complexation hydrogels as oral drug delivery carriers.

作者信息

Kim Bumsang, Peppas Nicholas A

机构信息

Biomaterials, Drug Delivery and Molecular Recognition Laboratories, Department of Chemical Engineering, 1 University Station Code C 0400, The University of Texas, Austin, TX 78712-0231, USA.

出版信息

Int J Pharm. 2003 Nov 6;266(1-2):29-37. doi: 10.1016/s0378-5173(03)00378-8.

Abstract

Novel pH-responsive complexation hydrogels containing pendent glucose (P(MAA-co-MEG)) or grafted PEG chains (P(MAA-g-EG)) were synthesized by photopolymerization. The feasibility of these hydrogels as oral protein delivery carriers was evaluated. The pH-responsive release behavior of insulin was analyzed from both P(MAA-co-MEG) and P(MAA-g-EG) hydrogels. In acidic media (pH 2.2), insulin release from the hydrogels was very slow. However, as the pH of the medium was changed to 6.5, a rapid release of insulin occurred. In both cases, the biological activity of insulin was retained. For P(MAA-co-MEG) hydrogels, the biological activity of insulin decreased when the pendent glucose content increased. In P(MAA-g-EG) hydrogels, when the grafted PEG molecular weight increased, the insulin biological activity decreased. Finally, hydrogels of P(MAA-co-MEG) prepared with an initial ratio of 1:4 MEG:MAA and P(MAA-g-EG) hydrogels containing PEG chains of molecular weights of 200 showed the greatest change in insulin release rate from acidic to basic pH solutions and the greatest protective effect for insulin in simulated GI tract conditions.

摘要

通过光聚合反应合成了含有侧链葡萄糖(P(MAA-co-MEG))或接枝PEG链(P(MAA-g-EG))的新型pH响应络合水凝胶。评估了这些水凝胶作为口服蛋白质递送载体的可行性。分析了胰岛素从P(MAA-co-MEG)和P(MAA-g-EG)水凝胶中的pH响应释放行为。在酸性介质(pH 2.2)中,胰岛素从水凝胶中的释放非常缓慢。然而,当介质的pH值变为6.5时,胰岛素迅速释放。在这两种情况下,胰岛素的生物活性均得以保留。对于P(MAA-co-MEG)水凝胶,当侧链葡萄糖含量增加时,胰岛素的生物活性降低。在P(MAA-g-EG)水凝胶中,当接枝PEG分子量增加时,胰岛素生物活性降低。最后,以1:4的MEG:MAA初始比例制备的P(MAA-co-MEG)水凝胶和含有分子量为200的PEG链的P(MAA-g-EG)水凝胶在从酸性到碱性pH溶液的胰岛素释放速率变化最大,并且在模拟胃肠道条件下对胰岛素具有最大的保护作用。

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