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脂质体双层包衣作为抗菌肽的包封基质:开发与表征

Dual Coating of Liposomes as Encapsulating Matrix of Antimicrobial Peptides: Development and Characterization.

作者信息

Gomaa Ahmed I, Martinent Cynthia, Hammami Riadh, Fliss Ismail, Subirade Muriel

机构信息

Department of Food Science, Laval University, Quebec City, QC, Canada.

Institute of Nutrition and Functional Foods, Quebec City, QC, Canada.

出版信息

Front Chem. 2017 Nov 17;5:103. doi: 10.3389/fchem.2017.00103. eCollection 2017.

Abstract

Antimicrobial peptides have been proposed as a potential biopreservatives in pharmaceutical research and agribusiness. However, many limitations hinder their utilization, such as their vulnerability to proteolytic digestion and their potential interaction with other food ingredients in complex food systems. One approach to overcome such problems is developing formulations entrapping and thereby protecting the antimicrobial peptides. Liposome encapsulation is a strategy that could be implemented to combine protection of the antimicrobial activity of the peptides from proteolytic enzymes and the controlled release of the encapsulated active ingredients. The objective of this study was to develop dual-coated food grade liposome formulations for oral administration of bacteriocins. The formulations were developed from anionic and cationic phospholipids as models of negatively and positively charged liposomes, respectively. Liposomes were prepared by the hydration of lipid films. Subsequently, the liposomes were coated with two layers comprising a biopolymer network (pectin) and whey proteins (WPI) in order to further improve their stability and enable the gradual release of the developed liposomes. Liposomes were characterized for their size, charge, molecular structure, morphology, encapsulation efficiency, and release. The results of FTIR, zeta potential, size distribution, and transmission electron microscopy (TEM) confirmed that the liposomes were efficiently coated. Ionic interactions were involved in the stabilization of the positively charged liposome formulations. Negatively charge liposome formulations were stabilized through weak interactions. The release study proved the efficiency of dual coating on the protection of liposomes against gastrointestinal digestion. This work is the first to study the encapsulation of antimicrobial peptides in dual-coated liposomes. Furthermore, the work successfully encapsulated MccJ25 in both negative and positive liposome models.

摘要

抗菌肽已被提议作为药物研究和农业综合企业中的一种潜在生物防腐剂。然而,许多限制因素阻碍了它们的应用,例如它们易受蛋白水解消化的影响以及在复杂食品体系中与其他食品成分的潜在相互作用。克服这些问题的一种方法是开发能够包裹并因此保护抗菌肽的制剂。脂质体包封是一种可以实施的策略,用于结合保护肽的抗菌活性免受蛋白水解酶的影响以及控制包封活性成分的释放。本研究的目的是开发用于口服细菌素的双层包衣食品级脂质体制剂。这些制剂分别由阴离子和阳离子磷脂制成,作为带负电荷和正电荷脂质体的模型。脂质体通过脂质膜水化制备。随后,脂质体用两层进行包衣,这两层包括生物聚合物网络(果胶)和乳清蛋白(乳清蛋白分离物),以进一步提高其稳定性并使所开发的脂质体能够逐渐释放。对脂质体的大小、电荷、分子结构、形态、包封效率和释放进行了表征。傅里叶变换红外光谱(FTIR)、zeta电位、大小分布和透射电子显微镜(TEM)的结果证实脂质体被有效地包衣。离子相互作用参与了带正电荷脂质体制剂的稳定。带负电荷的脂质体制剂通过弱相互作用得以稳定。释放研究证明了双层包衣在保护脂质体免受胃肠道消化方面的有效性。这项工作是首次研究抗菌肽在双层包衣脂质体中的包封。此外,这项工作成功地将MccJ25包封在阴性和阳性脂质体模型中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/41c4/5698301/e27a792f1563/fchem-05-00103-g0001.jpg

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