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使用反相微乳液聚合合成负载多聚磷酸盐的纳米颗粒用于持续递送至胃肠道。

Synthesis of Polyphosphate-Loaded Nanoparticles Using Inverse Miniemulsion Polymerization for Sustained Delivery to the Gastrointestinal Tract.

作者信息

Borges Fernando T P, Papavasiliou Georgia, Teymour Fouad

机构信息

Department of Chemical and Biological Engineering, Illinois Institute of Technology, Chicago, IL 60616, USA.

Department of Biomedical Engineering, Illinois Institute of Technology, Chicago, IL 60616, USA.

出版信息

Macromol React Eng. 2019 Apr;13(2). doi: 10.1002/mren.201800068. Epub 2019 Feb 18.

Abstract

Polyphosphate salts, such as sodium hexametaphosphate (PPi), are effective in the attenuation of collagenase and biofilm production and prevention of anastomotic leak in mice models. However, systemic administration of polyphosphate solutions to the gut presents a series of difficulties such as uncontrolled delivery to target and off-site tissues. In this article a process to produce PPi-loaded poly(ethylene glycol) diacrylate (PEGDA) hydrogel nanoparticles through miniemulsion polymerization is developed. The effects of using a polyphosphate salt, as compared to a monophosphate salt, is investigated through cloud point measurements, which is then translated to a change in the required HLB of the miniemulsion system. A parametric study is developed and yields a way to control particle swelling ratio and mean diameter based on the surfactant and/or initiator concentration, among other parameters. Finally, release kinetics of two different crosslink density particles shows a sustained and tunable release of the encapsulated polyphosphate.

摘要

多磷酸盐,如六偏磷酸钠(PPi),在小鼠模型中对胶原酶的抑制、生物膜生成的抑制以及吻合口漏的预防方面是有效的。然而,将多磷酸盐溶液全身给药至肠道存在一系列困难,例如向靶组织和非靶组织的递送不受控制。在本文中,开发了一种通过微乳液聚合制备负载PPi的聚(乙二醇)二丙烯酸酯(PEGDA)水凝胶纳米颗粒的方法。通过浊点测量研究了使用多磷酸盐与单磷酸盐相比的效果,然后将其转化为微乳液体系所需HLB的变化。开展了一项参数研究,并得出了一种基于表面活性剂和/或引发剂浓度等参数来控制颗粒溶胀率和平均直径的方法。最后,两种不同交联密度颗粒的释放动力学显示了包封的多磷酸盐的持续且可调节的释放。

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