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新型普罗布考纳米微囊的制备:扫描电子显微镜特征分析、浮力分析和抗氧化活性分析。

Novel nano-encapsulation of probucol in microgels: scanning electron micrograph characterizations, buoyancy profiling, and antioxidant assay analyses.

机构信息

a Biotechnology and Drug Development Research Laboratory, School of Pharmacy and Biomedical Sciences, Curtin Health Innovation Research Institute , Curtin University , Perth , Australia.

b Department of Pharmacology, Toxicology and Clinical Pharmacology, Faculty of Medicine , University of Novi Sad , Novi Sad , Serbia.

出版信息

Artif Cells Nanomed Biotechnol. 2018;46(sup3):S741-S747. doi: 10.1080/21691401.2018.1511571. Epub 2018 Sep 27.

Abstract

Smart polymers such as Eudragit (ED) have shown potential applications in oral drug delivery and targeted release. Probucol (PB) is a lipophilic drug used for hypercholesterolemia and possesses desirable antidiabetic effects such as antioxidant and cell protective effects. PB is highly hydrophobic and has poor bioavailability with significant inter- and intra-patient absorption, limiting its clinical applications in diabetes. This study aimed to design and analyse new PB-ED formulations with or without the absorption-enhancer chenodeoxycholic acid (CDCA). Sodium alginate-based microcapsules containing three different ED polymers (NM30D, RL30D and RS30D) were investigated with or without CDCA via scanning electron microscopy, energy dispersive X-ray spectroscopy (EDXR), confocal microscopy, osmotic stability, mechanical properties, buoyancy, release profiles (pH: 7.4), thermal stability and antioxidant effects. The effects of microcapsules on pancreatic β-cell survival, function, inflammatory profile and PB cellular uptake were analysed. All microcapsules showed uniform morphology and surface topography with CDCA being distributed evenly throughout the microcapsules. Osmotic stability was significantly improved in PB-NM30D and PB-RL30D microcapsules (p < .01 and p < .05, respectively), and PB-NM30D microcapsules displayed low buoyancy (p < .01). CDCA improved PB-NM30D effects on pancreatic β-cell function and bioenergetics, which suggests potential application of PB-NM30D-CDCA in PB delivery and diabetes treatment.

摘要

智能聚合物如 Eudragit(ED)已显示出在口服药物传递和靶向释放方面的潜在应用。普罗布考(PB)是一种用于高胆固醇血症的亲脂性药物,具有理想的抗糖尿病作用,如抗氧化和细胞保护作用。PB 具有很高的疏水性,生物利用度差,具有显著的个体间和个体内吸收,限制了其在糖尿病中的临床应用。本研究旨在设计和分析具有或不具有吸收增强剂胆酸(CDCA)的新 PB-ED 配方。通过扫描电子显微镜、能谱 X 射线光谱(EDXR)、共聚焦显微镜、渗透压稳定性、机械性能、浮力、释放曲线(pH:7.4)、热稳定性和抗氧化作用,研究了含有三种不同 ED 聚合物(NM30D、RL30D 和 RS30D)的基于海藻酸钠的微胶囊,以及含有或不含有 CDCA 的微胶囊。分析了微胶囊对胰岛 β 细胞存活、功能、炎症谱和 PB 细胞摄取的影响。所有微胶囊均表现出均匀的形态和表面形貌,CDCA 均匀分布在微胶囊中。PB-NM30D 和 PB-RL30D 微胶囊的渗透压稳定性显著提高(p<.01 和 p<.05),并且 PB-NM30D 微胶囊的浮力较低(p<.01)。CDCA 改善了 PB-NM30D 对胰岛 β 细胞功能和生物能量的影响,这表明 PB-NM30D-CDCA 在 PB 传递和糖尿病治疗中的潜在应用。

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