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pH-Responsive poly(itaconic acid-co-N-vinylpyrrolidone) hydrogels with reduced ionic strength loading solutions offer improved oral delivery potential for high isoelectric point-exhibiting therapeutic proteins

机译:降低离子强度加载溶液的pH响应型聚衣康酸-共N乙烯基吡咯烷酮水凝胶为高等电点的治疗性蛋白提供了更高的口服递送潜力

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摘要

pH-Responsive hydrogels comprised of itaconic acid copolymerized with N-vinylpyrrolidone (P(IA-co-NVP)) were synthesized and tested as carriers for the oral delivery of high isoelectric point (pI) exhibiting therapeutic proteins. Swelling studies show that P(IA-co-NVP) hydrogels exhibit significantly greater and faster pH-responsive swelling than previously studied methacrylic acid-based hydrogels, achieving up to 68% greater equilibrium swelling and 10.4 times greater swelling in time-limited experiments. Using salmon calcitonin as a model high pI protein therapeutic, we show that P(IA-co-NVP) hydrogels exhibit significantly greater delivery potential than methacrylic acid-based hydrogels. Additionally, we show that utilizing a lower ionic strength solution during drug loading significantly improves drug delivery potential for high pI therapeutics. By using a 1.5 mM PBS buffer rather than the standard 150 mM PBS buffer during loading, up to 83 times as much calcitonin can be delivered in neutral conditions, with up to a 9.6 fold improvement in percent release. Using P(IA-co-NVP) hydrogel microparticles and a low ionic strength loading solution, up to 48 μg calcitonin/mg hydrogel can be delivered in small intestinal conditions. Based on expected absorption in the small intestine, this is sufficient delivery potential for achieving therapeutic dosage via a single, regularly-sized pill taken daily.
机译:合成了由衣康酸与N-乙烯基吡咯烷酮(P(IA-co-NVP)共聚)组成的pH响应水凝胶,并对其进行了测试,作为可口服递送高等电点(pI)的载体,以显示治疗性蛋白质。溶胀研究表明,P(IA-co-NVP)水凝胶比以前研究的基于甲基丙烯酸的水凝胶表现出明显更大和更快的pH响应溶胀,在限时实验中,溶胀达到68%,溶胀达到10.4倍。使用鲑鱼降钙素作为模型的高pI蛋白治疗剂,我们显示P(IA-co-NVP)水凝胶比基于甲基丙烯酸的水凝胶具有更大的输送潜力。此外,我们表明在药物加载过程中使用较低的离子强度溶液可显着提高高pI治疗药物的药物输送潜力。通过在加载过程中使用1.5 mM PBS缓冲液而不是标准150 mM PBS缓冲液,在中性条件下可递送多达83倍的降钙素,释放百分率最多可提高9.6倍。使用P(IA-co-NVP)水凝胶微粒和低离子强度负载溶液,可以在小肠条件下递送高达48μg降钙素/ mg水凝胶。基于在小肠中的预期吸收,这具有足够的输送潜力,可通过每天服用一个规则大小的药丸来达到治疗剂量。

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