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一种用于在线衍生化并应用于体内神经化学监测的微流控芯片。

A microfluidic chip for on-line derivatization and application to in vivo neurochemical monitoring.

作者信息

Valenta Alec C, D'Amico Cara I, Dugan Colleen E, Grinias James P, Kennedy Robert T

机构信息

Department of Chemistry, University of Michigan, 930 N. University Avenue, Ann Arbor, Michigan 48109, USA.

出版信息

Analyst. 2021 Feb 7;146(3):825-834. doi: 10.1039/d0an01729a. Epub 2020 Dec 21.

Abstract

Microfluidic chips can perform a broad range of automated fluid manipulation operations for chemical analysis including on-line reactions. Derivatization reactions carried out on-chip reduce manual sample preparation and improve experimental throughput. In this work we develop a chip for on-line benzoyl chloride derivatization coupled to microdialysis, an in vivo sampling technique. Benzoyl chloride derivatization is useful for the analysis of small molecule neurochemicals in complex biological matrices using HPLC-MS/MS. The addition of one or more benzoyl groups to small, polar compounds containing amines, phenols, thiols, and certain alcohols improves reversed phase chromatographic retention, electrospray ionization efficiency, and analyte stability. The current derivatization protocol requires a three-step manual sample preparation, which ultimately limits the utility of this method for rapid sample collection and large sample sets. A glass microfluidic chip was developed for derivatizing microdialysis fractions on-line as they exit the probe for collection and off-line analysis with HPLC-MS/MS. Calibration curves for 21 neurochemicals prepared using the on-chip method showed linearity (R > 0.99), limits of detection (0.1-500 nM), and peak area RSDs (4-14%) comparable to manual derivatization. Method temporal resolution was investigated both in vitro and in vivo showing rapid rise times for all analytes, which was limited by fraction length (3 min) rather than the device. The platform was applied to basal measurements in the striatum of awake rats where 19 of 21 neurochemicals were above the limit of detection. For a typical 2 h study, a minimum of 120 pipetting steps are eliminated per animal. Such a device provides a useful tool for the analysis of small molecules in biological matrices which may extend beyond microdialysis to other sampling techniques.

摘要

微流控芯片可对化学分析执行广泛的自动化流体处理操作,包括在线反应。芯片上进行的衍生化反应减少了手动样品制备并提高了实验通量。在本工作中,我们开发了一种用于在线苯甲酰氯衍生化并与微透析(一种体内采样技术)相结合的芯片。苯甲酰氯衍生化对于使用高效液相色谱-串联质谱法(HPLC-MS/MS)分析复杂生物基质中的小分子神经化学物质很有用。向含有胺、酚、硫醇和某些醇的小极性化合物中添加一个或多个苯甲酰基可改善反相色谱保留、电喷雾电离效率和分析物稳定性。当前的衍生化方案需要三步手动样品制备,这最终限制了该方法在快速样品采集和大量样品集方面的实用性。开发了一种玻璃微流控芯片,用于在微透析馏分离开探针进行收集并通过HPLC-MS/MS进行离线分析时在线衍生化。使用芯片上方法制备的21种神经化学物质的校准曲线显示出线性(R>0.99)、检测限(0.1 - 500 nM)和峰面积相对标准偏差(4 - 14%),与手动衍生化相当。在体外和体内研究了方法的时间分辨率,结果表明所有分析物的上升时间都很快,这受馏分长度(3分钟)而非设备限制。该平台应用于清醒大鼠纹状体的基础测量,其中21种神经化学物质中有19种高于检测限。对于一个典型的2小时研究,每只动物至少可省去120个移液步骤。这样的设备为分析生物基质中的小分子提供了一个有用的工具,其应用可能不仅限于微透析,还可扩展到其他采样技术。

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