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Phosphate-Loaded Hydrogel Nanoparticles for Sepsis Prevention Prepared via Inverse Miniemulsion Polymerization

机译:通过逆微乳液聚合制备用于预防败血症的磷酸负载水凝胶纳米颗粒

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Local depletion of intestinal phosphate triggers changes in bacterial phenotypes that adversely affect the health of the host. This article describes a process for encapsulating phosphates in crosslinked poly(ethylene glycol) diacrylate (PEGDA) nanoparticles using inverse miniemulsion polymerization as a drug delivery approach for sustained release of phosphates to the intestinal epithelium. The effects of crosslinker, PEGDA co-monomer, N-vinyl pyrrolidone, (NVP) and surfactant concentrations on the nanoparticle size distribution, swelling ratio and monomer conversion are investigated. Increased surfactant and PEGDA concentrations result in smaller particle size and swelling ratio. A copolymerization model of crosslinking is used to predict conversion and gelation dynamics as a function of polymerization conditions. The model assumes that bulk polymerization can be used to approximate inverse miniemulsion polymerization with an aqueous-phase initiator. The initiator efficiency is used as an adjustable parameter to simulate the conversion dynamics, thus accounting for radical confinement effects and interaction with emulsifier molecules.
机译:肠道磷酸盐的局部消耗会触发细菌表型的变化,从而对宿主的健康产生不利影响。本文介绍了一种使用逆向微乳液聚合将磷酸盐封装在交联的聚(乙二醇)二丙烯酸酯(PEGDA)纳米颗粒中的方法,该方法是将磷酸盐持续释放至肠上皮的药物递送方法。研究了交联剂,PEGDA共聚单体,N-乙烯基吡咯烷酮(NVP)和表面活性剂浓度对纳米粒度分布,溶胀率和单体转化率的影响。表面活性剂和PEGDA浓度的增加导致较小的粒径和溶胀率。交联的共聚模型用于预测转化率和胶凝动力学作为聚合条件的函数。该模型假定本体聚合可用于近似于水相引发剂的逆细乳液聚合。引发剂效率用作模拟转化动力学的可调参数,因此可以说明自由基的限制作用以及与乳化剂分子的相互作用。

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