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迈向即时诊断代谢指纹分析:利用微流控预处理样品的红外光谱定量测定血浆肌酐。

Toward point-of-care diagnostic metabolic fingerprinting: quantification of plasma creatinine by infrared spectroscopy of microfluidic-preprocessed samples.

机构信息

National Research Council of Canada, Institute for Biodiagnostics, 435 Ellice Avenue, Winnipeg, Manitoba, Canada R3B 1Y6.

出版信息

Analyst. 2009 Jun;134(6):1224-31. doi: 10.1039/b821442e. Epub 2009 Mar 11.

Abstract

Infrared (IR) spectroscopy has previously been established as a means to accurately quantify several serum and urine metabolites, based upon spectroscopy of dry films. The same technique has also provided the basis to develop certain diagnostic tests, developed in the 'metabolomics' spirit. Here, we report on the further development of an integrated microfluidic-IR technology and technique, customized with the aim of dramatically extending the capabilities of IR spectroscopy in both analytical and diagnostic (metabolomic) applications. By exploiting the laminar fluid diffusion interface (LFDI), serum specimens are processed to yield product streams that are better suited for metabolic fingerprinting; metabolites are captured within the aqueous product stream, while proteins (which otherwise dominate the spectra of films dried from serum) are present in much reduced concentration. Spectroscopy of films dried from the aqueous stream then provides enhanced diagnostic and analytical sensitivity. The manuscript introduces an LFDI card design that is customized for integration with IR spectroscopy, and details the development of a quantitative assay for serum creatinine--based upon LFDI-processed serum samples--that is substantially more accurate (standard error of calibration, SEC = 43 micromol/L) than the corresponding assay based upon unprocessed serum specimens (SEC = 138 micromol/L). Preliminary results of diffusion modeling are reported, and the prospects for further optimization of the technique, guided by accurate modeling, are discussed.

摘要

红外(IR)光谱学以前已经确立为一种通过对干燥膜进行光谱分析来准确量化几种血清和尿液代谢物的方法。该技术还为某些诊断测试提供了基础,这些测试是在“代谢组学”精神的指导下开发的。在这里,我们报告了集成微流控-IR 技术和技术的进一步发展,该技术经过定制,旨在极大地扩展 IR 光谱在分析和诊断(代谢组学)应用中的功能。通过利用层流流体扩散界面(LFDI),对血清标本进行处理,产生更适合代谢指纹分析的产物流;代谢物被捕获在水产物流中,而蛋白质(否则会主导从血清中干燥的膜的光谱)的浓度则大大降低。然后对从水相流中干燥的膜进行光谱分析,可提高诊断和分析的灵敏度。本文介绍了一种 LFDI 卡设计,该设计经过定制可与 IR 光谱集成,并详细介绍了基于 LFDI 处理的血清样本开发的血清肌酐定量测定法,该方法比基于未处理血清样本的相应测定法(SEC = 138 μmol/L)更准确(校准标准误差,SEC = 43 μmol/L)。报告了扩散建模的初步结果,并讨论了通过准确建模进一步优化该技术的前景。

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