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Phospholipid complex based nanoemulsion system for oral insulin delivery: preparation in vitro and in vivo evaluations

机译:用于口服胰岛素递送的基于磷脂复合物的纳米乳剂系统:制备体外和体内评估

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摘要

>Purpose: The aim of this research was to develop a phospholipid complex based nanoemulsion system for oral insulin delivery.>Methods: Insulin-phospholipid complex (IPC) was firstly prepared by an anhydrous co-solvent lyophilization method, and then encapsulated into the oil phase of nanoemulsion to obtain the IPC-based nanoemulsion (IPC-NE). Both water-in-oil (W/O) IPC-NE and oil-in-water (O/W) IPC-NE were formulated and evaluated for comparison.>Results: The obtained W/O IPC-NE and O/W IPC-NE were both spherical in shape with a mean particle size of 18.6±0.79 nm and 27.3±1.25 nm, respectively. While both IPC-NEs exhibited enhanced Caco-2 cell monolayers permeability than IPC and insulin solution, W/O IPC-NE showed relatively greater protective effects against enzymatic degradation than O/W IPC-NE. Moreover, oral administration of W/O IPC-NE exhibited significant hypoglycemic effects, with 12.4-fold and 1.5-fold higher oral bioavailability compared with insulin solution and O/W IPC-NE, respectively.>Conclusion: IPC-NEs, especially the W/O IPC-NE showed promising efficiency in vitro and in vivo, thus could be a potential strategy for oral insulin delivery.
机译:>目的:本研究的目的是开发基于磷脂复合物的纳米乳剂,用于口服胰岛素的输送。>方法::胰岛素-磷脂复合物(IPC)首先由无水制备共溶剂冻干法,然后将其包封到纳米乳液的油相中,得到基于IPC的纳米乳液(IPC-NE)。制定并评估了油包水(W / O)IPC-NE和水包油(O / W)IPC-NE。>结果:获得的W / O IPC -NE和O / W IPC-NE均为球形,平均粒径分别为18.6±0.79 nm和27.3±1.25 nm。尽管两个IPC-NEs均比IPC和胰岛素溶液均显示出增强的Caco-2细胞单层通透性,但与O / W IPC-NE相比,W / O IPC-NE表现出相对更高的抗酶促降解作用。此外,口服W / O IPC-NE表现出明显的降血糖作用,与胰岛素溶液和O / W IPC-NE相比,口服生物利用度分别高12.4倍和1.5倍。>结论: IPC-NEs,特别是W / O IPC-NE在体外和体内均显示出有希望的效率,因此可能是口服胰岛素递送的潜在策略。

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