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一种用于测量水凝胶中小分子扩散的微流控方法。

A microfluidic method to measure small molecule diffusion in hydrogels.

机构信息

Department of Chemical Engineering, Bucknell University, Lewisburg, PA 17837, USA.

Department of Chemical Engineering, Bucknell University, Lewisburg, PA 17837, USA.

出版信息

Mater Sci Eng C Mater Biol Appl. 2014 Feb 1;35:322-34. doi: 10.1016/j.msec.2013.10.035. Epub 2013 Nov 11.

Abstract

Drug release from a fluid-contacting biomaterial is simulated using a microfluidic device with a channel defined by solute-loaded hydrogel; as water is pumped through the channel, solute transfers from the hydrogel into the water. Optical analysis of in-situ hydrogels, characterization of the microfluidic device effluent, and NMR methods were used to find diffusion coefficients of several dyes (model drugs) in poly(ethylene glycol) diacrylate (PEG-DA) hydrogels. Diffusion coefficients for methylene blue and sulforhodamine 101 in PEG-DA calculated using the three methods are in good agreement; both dyes are mobile in the hydrogel and elute from the hydrogel at the aqueous channel interface. However, the dye acid blue 22 deviates from typical diffusion behavior and does not release as expected from the hydrogel. Importantly, only the microfluidic method is capable of detecting this behavior. Characterizing solute diffusion with a combination of NMR, optical and effluent methods offer greater insight into molecular diffusion in hydrogels than employing each technique individually. The NMR method made precise measurements for solute diffusion in all cases. The microfluidic optical method was effective for visualizing diffusion of the optically active solutes. The optical and effluent methods show potential to be used to screen solutes to determine if they elute from a hydrogel in contact with flowing fluid. Our data suggest that when designing a drug delivery device, analyzing the diffusion from the molecular level to the device level is important to establish a complete picture of drug elution, and microfluidic methods to study such diffusion can play a key role.

摘要

使用一种带有溶质负载水凝胶的通道的微流控设备模拟流体接触生物材料的药物释放;当水被泵入通道时,溶质从水凝胶转移到水中。对原位水凝胶进行光学分析、对微流控设备流出物进行特性分析以及使用 NMR 方法,以找到几种染料(模型药物)在聚乙二醇二丙烯酸酯(PEG-DA)水凝胶中的扩散系数。使用这三种方法计算的亚甲蓝和磺基罗丹明 101 在 PEG-DA 中的扩散系数非常吻合;这两种染料在水凝胶中均具有流动性,并从水凝胶在水通道界面处洗脱。然而,酸性蓝 22 染料偏离典型的扩散行为,并未按预期从水凝胶中释放。重要的是,只有微流控方法能够检测到这种行为。结合 NMR、光学和流出物方法来表征溶质扩散,可以比单独使用每种技术更深入地了解水凝胶中的分子扩散。NMR 方法在所有情况下都能对溶质扩散进行精确测量。微流控光学方法有效地可视化了光活性溶质的扩散。光学和流出物方法具有用于筛选溶质以确定它们是否从与流动流体接触的水凝胶中洗脱的潜力。我们的数据表明,在设计药物输送装置时,从分子水平到装置水平分析扩散对于建立药物洗脱的完整图景很重要,并且研究这种扩散的微流控方法可以发挥关键作用。

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