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Calcifediol-loaded liposomes for local treatment of pulmonary bacterial infections.

机译:加载了降钙素二醇的脂质体,用于局部治疗肺部细菌感染。

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摘要

The influence of vitamin D3 and its metabolites calcifediol (25(OH)D) and calcitriol on immune regulation and inflammation is well described, and raises the question of potential benefit against bacterial infections. In the current study, 25(OH)D was encapsulated in liposomes to enable aerosolisation, and tested for the ability to prevent pulmonary infection by Pseudomonas aeruginosa. Prepared 25(OH)D-loaded liposomes were nanosized and monodisperse, with a negative surface charge and a 25(OH)D entrapment efficiency of approximately 23%. Jet nebulisation of liposomes was seen to yield an aerosol suitable for tracheo-bronchial deposition. Interestingly, 25(OH)D in either liposomes or ethanolic solution had no effect on the release of the proinflammatory cytokine KC from Pseudomonas-infected murine epithelial cells (LA-4); treatment of infected, human bronchial 16-HBE cells with 25(OH)D liposomes however resulted in a significant reduction in bacterial survival. Together with the importance of selecting an application-appropriate in vitro model, the current study illustrates the feasibility and practicality of employing liposomes as a means to achieve 25(OH)D lung deposition. 25(OH)D-loaded liposomes further demonstrated promising effects regarding prevention of Pseudomonas infection in human bronchial epithelial cells.
机译:维生素D3及其代谢产物骨化二醇(25(OH)D)和骨化三醇对免疫调节和炎症的影响已得到很好的描述,并提出了对抗细菌感染的潜在益处的问题。在当前的研究中,将25(OH)D封装在脂质体中以实现雾化,并测试了预防铜绿假单胞菌引起的肺部感染的能力。制备的负载25(OH)D的脂质体是纳米级的并且是单分散的,具有负表面电荷和大约23%的25(OH)D包封率。观察到脂质体的喷射雾化产生适合气管支气管沉积的气雾剂。有趣的是,脂质体或乙醇溶液中的25(OH)D对假单胞菌感染的鼠上皮细胞(LA-4)中促炎细胞因子KC的释放没有影响。然而,用25(OH)D脂质体处理感染的人支气管16-HBE细胞会导致细菌存活率显着降低。与选择适合应用的体外模型的重要性一起,当前的研究表明了采用脂质体作为实现25(OH)D肺沉积的手段的可行性和实用性。装载25(OH)D的脂质体进一步证明了在预防人支气管上皮细胞中假单胞菌感染方面的有希望的作用。

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