Integration of paper-based analytical devices with digital microfluidics for colorimetric detection of creatinine

IF 3.6 3区 化学 Q2 CHEMISTRY, ANALYTICAL Analyst Pub Date : 2024-10-08 DOI:10.1039/d4an00688g
Larissa Garcia Velasco, Danielly Santos Rocha, Richard P. S. de Campos, Wendell Karlos Tomazelli Coltro
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Abstract

Digital microfluidics (DMF) is a platform that enables the automated manipulation of individual droplets of sizes ranging from nano- to microliter and can be coupled with numerous techniques, including colorimetry. However, although DMF electrode architecture is highly versatile, its integration with different analytical methods often requires either changes in sample access, top plate design, or the integration of supplementary equipment into the system. As an alternative to overcome these challenges, this study proposes a simple integration between paper-based analytical devices (PADs) and DMF for automated and eco-friendly sample processing aiming at the colorimetric detection of creatinine (an important biomarker for kidney disease) in artificial urine. Optimized and selective Jaffé reaction was performed on the device, and reaction products were delivered to the PAD, which was subsequently analyzed with a bench scanner. The optimal operational parameters on DMF were 45 s reaction time with circular mixing and capture of the image after 5 min. Under optimized conditions, a linear behavior was obtained for creatinine concentrations ranging from 2 to 32 mg dL-1, with limits of detection and quantitation equal to 1.4 mg dL-1 and 3.1 mg dL-1, respectively. For the concentration range tested, the relative standard deviation varied from 2.5 to 11.0%, considering four measurements per concentration. Creatinine-spiked synthetic urine samples were subjected to analysis via DMF-PAD and the spectrophotometric reference method. The concentrations of CR determined using both analytical techniques were close to the theoretical values, with the resultant standard deviations of 2-9% and 1-4% for DMF-PAD and spectrophotometry, respectively. Furthermore, the recovery values were within the acceptable range, with DMF-PAD yielding 96-108% and spectrophotometry producing 95-102%. Finally, the greenness levels of DMF-PAD and spectrophotometric methods were evaluated using the Analytical Greenness Metric software, in which 0.71 and 0.51 scores were obtained, respectively. This indicates that the proposed method presents a higher greenness level, mainly due to its miniaturized characteristic using a smaller volume of reagent and sample and the possibility of automation, thus reducing user exposure to potentially toxic substances. Therefore, the DMF-PADs demonstrated great potential for application in the clinical analysis of creatinine, aiding in routine tests by introducing an automated, simple, and environmentally friendly process.
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将纸质分析装置与数字微流控技术相结合,用于肌酐的比色检测
数字微流控(DMF)是一种能够自动操作大小从纳米到微升不等的单个液滴的平台,可与包括比色法在内的多种技术相结合。然而,尽管 DMF 电极结构具有很强的通用性,但要将其与不同的分析方法集成,往往需要改变样品存取方式、顶板设计或将辅助设备集成到系统中。为了克服这些挑战,本研究提出了一种纸质分析设备(PAD)与 DMF 之间的简单集成,用于自动化和环保型样品处理,目的是对人工尿液中的肌酐(肾脏疾病的重要生物标志物)进行比色检测。在该装置上进行了优化的选择性贾菲反应,反应产物被输送到 PAD,随后用台式扫描仪进行分析。DMF 的最佳操作参数为 45 秒反应时间,循环混合,5 分钟后捕捉图像。在优化条件下,肌酐浓度从 2 毫克 dL-1 到 32 毫克 dL-1 之间呈线性关系,检出限和定量限分别为 1.4 毫克 dL-1 和 3.1 毫克 dL-1。在测试的浓度范围内,考虑到对每个浓度进行四次测量,相对标准偏差在 2.5% 到 11.0% 之间。添加了肌酸酐的合成尿样通过 DMF-PAD 和分光光度参照法进行分析。使用这两种分析技术测定的 CR 浓度均接近理论值,DMF-PAD 和分光光度法的标准偏差分别为 2-9% 和 1-4%。此外,回收率也在可接受的范围内,DMF-PAD 的回收率为 96-108%,分光光度法的回收率为 95-102%。最后,使用分析绿色度量软件对 DMF-PAD 和分光光度法的绿色度进行了评估,结果分别为 0.71 和 0.51。这表明拟议方法的绿色程度较高,主要原因是该方法具有微型化的特点,使用的试剂和样品量较少,而且可以实现自动化,从而减少使用者接触潜在有毒物质的机会。因此,DMF-PAD 在肌酐的临床分析中显示出巨大的应用潜力,通过引入自动化、简单和环保的流程,有助于常规检测。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Analyst
Analyst 化学-分析化学
CiteScore
7.80
自引率
4.80%
发文量
636
审稿时长
1.9 months
期刊介绍: The home of premier fundamental discoveries, inventions and applications in the analytical and bioanalytical sciences
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