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下一代红外光谱学:基于 EC-QCL 的蛋白质中红外透射光谱学与平衡检测。

The Next Generation of IR Spectroscopy: EC-QCL-Based Mid-IR Transmission Spectroscopy of Proteins with Balanced Detection.

机构信息

Institute of Chemical Technologies and Analytics, Technische Universität Wien, Getreidemarkt 9, 1060 Vienna, Austria.

Vigo System S.A., 129/133 Poznańska St., 05-850 Oz̈arów, Mazowiecki, Poland.

出版信息

Anal Chem. 2020 Jul 21;92(14):9901-9907. doi: 10.1021/acs.analchem.0c01406. Epub 2020 Jul 13.

Abstract

We report a mid-IR transmission setup for the analysis of the protein amide I and amide II band in aqueous solutions that achieves a limit of detection as low as 0.0025 mg mL (outperforming our previous results and other state-of-the-art mid-IR-based techniques by almost an order of magnitude). This large improvement is made possible by combining the latest-generation external cavity-quantum cascade laser (EC-QCL) operated at room temperature with an optimized double-beam optical setup that adjusts the path length (26 μm) to ensure robust sample handling. For minimizing the noise introduced by the high-intensity laser light source, a thermoelectrically cooled mercury cadmium telluride balanced detection module was employed. In this way, noise levels better by a factor of up to 20 were achieved compared with single-channel measurements. Characteristic spectral features of proteins with different secondary structures were successfully identified at concentrations as low as 0.1 mg mL. Furthermore, a highly linear response was demonstrated for concentrations between 0.05 and 10 mg mL. The total acquisition time of the setup can be adapted to fulfill the required sensitivity of the protein measurements and to ensure maximum flexibility for future applications. The presented setup combines high sensitivity, large optical path lengths, and short measurement times and thus outperforms previous research type EC-QCL setups as well as commercially available instruments. This opens a wide range of future applications including protein-ligand interaction studies as well as qualitative and quantitative analyses of proteins in complex matrices such as those found in up- and downstream bioprocess monitoring and similar challenging applications which can not be readily met by conventional FT-IR spectroscopy.

摘要

我们报告了一种中红外传输设置,用于分析水溶液中的蛋白质酰胺 I 和酰胺 II 带,其检测限低至 0.0025mg/mL(优于我们之前的结果和其他最先进的中红外技术,几乎提高了一个数量级)。这种大幅改进是通过将最新一代室温运行的外腔量子级联激光器(EC-QCL)与优化的双光束光学设置相结合实现的,该设置调整光程(26μm)以确保稳健的样品处理。为了最小化高强度激光光源引入的噪声,采用了热电冷却的碲化汞镉平衡检测模块。通过这种方式,与单通道测量相比,噪声水平提高了多达 20 倍。在低至 0.1mg/mL 的浓度下,成功识别了具有不同二级结构的蛋白质的特征光谱特征。此外,在 0.05 至 10mg/mL 的浓度范围内,证明了高度线性的响应。该设置的总采集时间可以适应蛋白质测量所需的灵敏度,并确保未来应用的最大灵活性。所提出的设置结合了高灵敏度、大光程和短测量时间,因此优于以前的研究型 EC-QCL 装置以及商业上可用的仪器。这为未来的应用开辟了广泛的可能性,包括蛋白质-配体相互作用研究以及复杂基质中蛋白质的定性和定量分析,例如在上下游生物过程监测和类似具有挑战性的应用中发现的蛋白质,这些应用无法通过常规的傅里叶变换红外光谱法轻易满足。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d418/7376528/aafb805f0152/ac0c01406_0001.jpg

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