材料科学
牛血清白蛋白
萃取(化学)
色谱法
药物输送
控制释放
涂层
化学工程
生物医学工程
复合材料
纳米技术
化学
医学
工程类
作者
Michael G. Potroz,Raghavendra C. Mundargi,J. J. J. Gillissen,Ee‐Lin Tan,Sigalit Meker,Jae Whan Park,Haram Jung,Soo-Hyun Park,Daeho Cho,Sa Ik Bang,Nam‐Joon Cho
标识
DOI:10.1002/adfm.201700270
摘要
Efficient oral administration of protein‐based therapeutics faces significant challenges due to degradation from the highly acidic conditions present in the stomach and proteases present in the digestive tract. Herein, investigations into spike‐covered sunflower sporopollenin exine capsules (SECs) for oral protein delivery using bovine serum albumin (BSA) as a model drug are reported and provide significant insights into the optimization of SEC extraction, SEC loading, and controlled release. The phosphoric‐acid‐based SEC extraction process is optimized. Compound loading is shown to be driven by the evacuation of air bubbles from SEC cavities through the porous SEC shell wall, and vacuum loading is shown to be the optimal loading method. Three initial BSA‐loading proportions are evaluated, leading to a practical loading efficiency of 22.3 ± 1.5 wt% and the determination that the theoretical maximum loading is 46.4 ± 2.5 wt%. Finally, an oral delivery formulation for targeted intestinal delivery is developed by tableting BSA‐loaded SECs and enteric coating. BSA release is inhibited for 2 h in simulated gastric conditions followed by 100% release within 8 h in simulated intestinal conditions. Collectively, these results indicate that sunflower SECs provide a versatile platform for the oral delivery of therapeutics.
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