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微流控装置中药物的衰减全反射-傅里叶变换红外光谱成像

Attenuated total reflection-Fourier transform infrared spectroscopic imaging of pharmaceuticals in microfluidic devices.

作者信息

Ewing Andrew V, Clarke Graham S, Kazarian Sergei G

机构信息

Department of Chemical Engineering, Imperial College London , London SW7 2AZ, United Kingdom.

Bristol-Myers Squibb , Reeds Lane, Moreton, Wirral, Merseyside CH46 1QW, United Kingdom.

出版信息

Biomicrofluidics. 2016 Apr 20;10(2):024125. doi: 10.1063/1.4946867. eCollection 2016 Mar.

DOI:10.1063/1.4946867
PMID:27158293
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4841796/
Abstract

The poor aqueous solubility of many active pharmaceutical ingredients presents challenges for effective drug delivery. In this study, the combination of attenuated total reflection (ATR)-FTIR spectroscopic imaging with specifically designed polydimethylsiloxane microfluidic devices to study drug release from pharmaceutical formulations has been developed. First, the high-throughput analysis of the dissolution of micro-formulations studied under flowing conditions has been introduced using a model formulation of ibuprofen and polyethylene glycol. The behaviour and release of the drug was monitored in situ under different pH conditions. In contrast to the neutral solution, where both the drug and excipient dissolved at a similar rate, structural change from the molecularly dispersed to a crystalline form of ibuprofen was characterised in the obtained spectroscopic images and the corresponding ATR-FTIR spectra for the experiments carried out in the acidic medium. Further investigations into the behaviour of the drug after its release from formulations (i.e., dissolved drug) were also undertaken. Different solutions of sodium ibuprofen dissolved in a neutral medium were studied upon contact with acidic conditions. The phase transition from a dissolved species of sodium ibuprofen to the formation of solid crystalline ibuprofen was revealed in the microfluidic channels. This innovative approach could offer a promising platform for high-throughput analysis of a range of micro-formulations, which are of current interest due to the advent of 3D printed pharmaceutical and microparticulate delivery systems. Furthermore, the ability to study dissolved drug in solution under flowing conditions can be useful for the studies of the diffusion of drugs into tissues or live cells.

摘要

许多活性药物成分的水溶性较差,这给有效的药物递送带来了挑战。在本研究中,已开发出将衰减全反射(ATR)-傅里叶变换红外光谱成像与专门设计的聚二甲基硅氧烷微流控装置相结合的方法,用于研究药物制剂中的药物释放。首先,使用布洛芬和聚乙二醇的模型制剂,引入了在流动条件下对微制剂溶解情况的高通量分析。在不同pH条件下原位监测药物的行为和释放情况。与中性溶液不同,在中性溶液中药物和赋形剂以相似的速率溶解,而在酸性介质中进行的实验所获得的光谱图像和相应的ATR-傅里叶变换红外光谱中,表征了布洛芬从分子分散形式到结晶形式的结构变化。还对药物从制剂中释放后(即溶解的药物)的行为进行了进一步研究。研究了溶解在中性介质中的不同布洛芬钠溶液与酸性条件接触后的情况。在微流控通道中揭示了从溶解的布洛芬钠物种到形成固体结晶布洛芬的相变。这种创新方法可为一系列微制剂的高通量分析提供一个有前景的平台,由于3D打印药物和微粒递送系统的出现,这些微制剂目前备受关注。此外,在流动条件下研究溶液中溶解药物的能力对于研究药物向组织或活细胞中的扩散可能是有用的。