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包被凝集素的 PLGA 微球:热响应性释放及增强细胞相互作用的体外证据。

Lectin-coated PLGA microparticles: thermoresponsive release and in vitro evidence for enhanced cell interaction.

机构信息

Department of Pharmaceutical Technology and Biopharmaceutics, University of Vienna, Vienna, Austria.

出版信息

Int J Pharm. 2012 Oct 15;436(1-2):738-43. doi: 10.1016/j.ijpharm.2012.07.025. Epub 2012 Jul 25.

Abstract

PLGA-microparticles with 4.7 μm in diameter were prepared by the double emulsion technique and loaded with 1.7 μg fluorescein/mg PLGA mimicking a hydrophilic API. In an effort to further elucidate the release and bioadhesive characteristics of lectin-grafted formulations in vitro, the particles were coated with wheat germ agglutinin. The microparticles exhibited thermo-responsive release since no free fluorescein was detected at 4 °C or room temperature. At body temperature, however, more than 80% of the payload was released within 48 h. The adhesion of lectin-grafted particles to Caco-2 monolayers, which were applied as a model for the human intestinal epithelium, exceeded that of plain ones 1.5-fold as also observed by fluorescence microscopy. Furthermore, the amount of model drug bound and taken up into the cells was 5.8-fold higher after incubation for 4 h at 37 °C as compared to fluorescein in solution. According to fluorescence imaging a considerable amount of the total fluorescein payload was accumulated intracellularily after incubation for 5 h at 37 °C. These findings not only confirm the utility of bioadhesives of the second generation for improved absorption of low molecular weight hydrophilic compounds but also indicate storage stability of such suspensions at 4 °C and room temperature without any premature loss of API.

摘要

直径为 4.7μm 的 PLGA 微球通过复乳技术制备,并负载 1.7μg 荧光素/mg PLGA,模拟亲水性 API。为了进一步阐明体外糖结合制剂的释放和生物黏附特性,将颗粒用麦胚凝集素进行包被。微球表现出温度响应释放特性,因为在 4°C 或室温下未检测到游离荧光素。然而,在体温下,超过 80%的载药量在 48 小时内释放。与普通颗粒相比,用作为人肠道上皮模型的 Caco-2 单层黏附的糖结合颗粒的黏附性高出 1.5 倍,这也可以通过荧光显微镜观察到。此外,与溶液中的荧光素相比,孵育 4 小时后,结合并摄取到细胞中的模型药物量增加了 5.8 倍。根据荧光成像,在 37°C 孵育 5 小时后,相当一部分总荧光素载药量被细胞内积累。这些发现不仅证实了第二代生物黏附剂在改善低分子量亲水性化合物吸收方面的实用性,还表明在 4°C 和室温下储存此类混悬液具有稳定性,不会导致 API 的任何过早损失。

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