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A facile fabrication of core-shell sodium alginate/gelatin beads for drug delivery systems

机译:用于药物递送系统的核 - 壳酸钠/明胶珠的容易制造

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摘要

To improve the durability and bioavailability of alginate, a one-step extrusion method was successfully applied to prepare alginate/gelatin core-shell beads. Gelatin cross-linked with glutaraldehyde was used as the core, while sodium alginate was used as the shell. To evaluate the effect of the sodium alginate shell on the in vitro drug release properties of the beads for biomedical applications, two drug models were used: water-soluble metformin hydrochloride and water-insoluble indomethacin. The structure and properties of different core-shell beads were characterized by Fourier transform infrared spectroscopy, scanning electron microscopy and swelling tests. The results showed that the beads consist of obvious inner core and outer skin layer which coats the surface stably. In addition, the core-shell structure improved the thermal stability of the beads and the entrapment efficiency reached 90% with a sodium alginate shell. As demonstrated, there is a gradual decrease in the swelling degree as the GTA or alginate concentration increases. For indomethacin, the cumulative release was 8.7% after 360min in HCl buffer. The anomalous transport mechanism was the predominant factor affecting the release behavior of the metformin hydrochloride-loaded beads and indomethacin loaded beads were controlled by case-II transport. This work suggests that the core-shell structure could improve the swelling properties and drug release behavior of the beads.
机译:为了提高藻酸盐的耐久性和生物利用度,成功地应用了一步挤出方法以制备藻酸盐/明胶核心壳珠。使用与戊二醛交联的明胶作为核心,而藻酸钠用作壳。为了评估藻酸钠壳对生物医学应用珠粒体外药物释放性能的影响,使用了两种药物模型:水溶性二甲双胍盐酸盐和水不溶性吲哚美辛。通过傅里叶变换红外光谱,扫描电子显微镜和溶胀试验表征了不同核壳珠子的结构和性质。结果表明,珠子由明显的内核和外部皮肤层组成,稳定地涂覆表面。此外,核心壳结构改善了珠子的热稳定性,并且血酸钠壳夹紧效率达到90%。如所示,随着GTA或海藻酸盐浓度的增加,溶胀度逐渐减小。对于吲哚美辛,HCl缓冲液360米后,累积释放为8.7%。异常传输机制是影响盐酸二甲双胍的盐酸二甲双胍的释放行为的主要因素,并且通过壳体-II运输来控制吲哚美辛的珠子。这项工作表明,核心壳结构可以改善珠子的肿胀性能和药物释放行为。

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