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向日葵孢粉素外壁胶囊上可设计的羧甲基茯苓聚糖/金属离子结构作为生物活性大分子的递送载体

Designable Carboxymethylpachymaran/Metal Ion Architecture on Sunflower Sporopollenin Exine Capsules as Delivery Vehicles for Bioactive Macromolecules.

作者信息

Deng Ziyu, Pei Yaqiong, Wang Shishuai, Zhou Bin, Hou Xinyao, Li Jing, Li Bin, Liang Hongshan

机构信息

College of Food Science and Technology, Key Laboratory of Environment Correlative Dietology (Huazhong Agricultural University), Ministry of Education, Huazhong Agricultural University, Wuhan 430070, China; China.

College of Culinary and Food Engineering, Wuhan Business University, Wuhan 430056, China.

出版信息

J Agric Food Chem. 2020 Nov 25;68(47):13990-14000. doi: 10.1021/acs.jafc.0c05169. Epub 2020 Nov 11.

Abstract

There are multiple obstacles in the gastrointestinal tract (GIT) for oral administration of bioactive macromolecules. Here, we engineered an oral delivery vehicle (sporopollenin exine capsules with carboxymethylpachymaran (CMP)/metal ion modification) with targeted release based on food-grade ingredients and processing operations. Then, the interaction and binding mechanisms between CMP and metal ions in the vehicle were investigated. By using β-galactosidase (β-Gal) as a model protein, the systems were characterized for the surface morphology and monitored by the release profile of β-Gal. Notably, the CMP/metal ion systems not only markedly decreased the CMP dosage but also achieved a valid long-term release compared with the previously reported CMP system. Among all the systems, the CMP/3% AlCl system showed the best ability to control the release with the maximum residual activity of β-Gal at nearly 72% after 24 h of treatment. Subsequently, the interaction mechanism between CMP and metal ions within the system was characterized by the perspectives of microstructure, rheological properties, and spectroscopy characteristics. The results indicated that the low pH conditions are conducive to the further cross-linking of CMP and metal ions, resulting in a high gel strength and thus a dense structure, which can impact the controlled release of β-Gal in the GIT. Overall, the system may be utilized in the administration of medical and functional foods, specifically for the delivery of bioactive proteins the oral route.

摘要

生物活性大分子口服给药时,胃肠道存在多种障碍。在此,我们基于食品级成分和加工操作设计了一种具有靶向释放功能的口服给药载体(羧甲基茯苓多糖(CMP)/金属离子修饰的孢粉素外壁胶囊)。然后,研究了载体中CMP与金属离子之间的相互作用和结合机制。以β-半乳糖苷酶(β-Gal)作为模型蛋白,对该系统进行表面形态表征,并通过β-Gal的释放曲线进行监测。值得注意的是,与先前报道的CMP系统相比,CMP/金属离子系统不仅显著降低了CMP用量,还实现了有效的长效释放。在所有系统中,CMP/3%AlCl系统显示出最佳的控释能力,处理24小时后β-Gal的最大残留活性接近72%。随后,从微观结构、流变学性质和光谱特征等角度对系统内CMP与金属离子之间的相互作用机制进行了表征。结果表明,低pH条件有利于CMP与金属离子进一步交联,形成高凝胶强度,从而形成致密结构,这会影响β-Gal在胃肠道中的控释。总体而言,该系统可用于医疗和功能性食品的给药,特别是用于口服途径的生物活性蛋白递送。

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