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利用红外基质辅助激光解吸电喷雾电离质谱进行高通量完整蛋白质分析在药物发现中的应用。

High-Throughput Intact Protein Analysis for Drug Discovery Using Infrared Matrix-Assisted Laser Desorption Electrospray Ionization Mass Spectrometry.

机构信息

AbbVie Inc, 1 North Waukegan Rd., North Chicago, Illinois 60064, United States.

出版信息

Anal Chem. 2022 Oct 4;94(39):13566-13574. doi: 10.1021/acs.analchem.2c03211. Epub 2022 Sep 21.

DOI:10.1021/acs.analchem.2c03211
PMID:36129783
Abstract

Mass spectrometry (MS) is the primary analytical tool used to characterize proteins within the biopharmaceutical industry. Electrospray ionization (ESI) coupled to liquid chromatography (LC) is the current gold standard for intact protein analysis. However, inherent speed limitations of LC/MS prevent analysis of large sample numbers (>1000) in a day. Infrared matrix-assisted laser desorption electrospray ionization (IR-MALDESI-MS), an ambient ionization MS technology, has recently been established as a platform for high-throughput small molecule analysis. Here, we report the applications of such a system for the analysis of intact proteins commonly performed within the drug discovery process. A wide molecular weight range of proteins 10-150 kDa was detected on the system with improved tolerance to salts and buffers compared to ESI. With high concentrations and model proteins, a sample rate of up to 22 Hz was obtained. For proteins at low concentrations and in buffers used in commonly employed assays, robust data at a sample rate of 1.5 Hz were achieved, which is ∼22× faster than current technologies used for high-throughput ESI-MS-based protein assays. In addition, two multiplexed plate-based high-throughput sample cleanup methods were coupled to IR-MALDESI-MS to enable analysis of samples containing excessive amounts of salts and buffers without fully compromising productivity. Example experiments, which leverage the speed of the IR-MALDESI-MS system to monitor NISTmAb reduction, protein autophosphorylation, and compound binding kinetics in near real time, are demonstrated.

摘要

质谱(MS)是生物制药行业中用于鉴定蛋白质的主要分析工具。电喷雾电离(ESI)与液相色谱(LC)的联用是目前分析完整蛋白质的金标准。然而,LC/MS 的固有速度限制使其无法在一天内分析大量 (>1000) 个样本。红外基质辅助激光解吸电喷雾电离(IR-MALDESI-MS)是一种新兴的大气离子化 MS 技术,最近已被确立为高通量小分子分析的平台。在这里,我们报告了该系统在药物发现过程中常用于分析完整蛋白质的应用。与 ESI 相比,该系统能够检测到 10-150 kDa 分子量范围内的广泛蛋白质,并且对盐和缓冲液的耐受性更好。对于高浓度和模型蛋白质,可获得高达 22 Hz 的采样率。对于低浓度的蛋白质和常用测定中使用的缓冲液,可实现 1.5 Hz 的稳健数据采集,这比目前用于高通量 ESI-MS 基蛋白质测定的技术快约 22 倍。此外,两种基于板的多重高通量样品净化方法与 IR-MALDESI-MS 联用,可在不降低生产力的情况下分析含有大量盐和缓冲液的样品。本文还展示了利用 IR-MALDESI-MS 系统的速度进行的实验,这些实验实时监测了 NISTmAb 还原、蛋白质自磷酸化和化合物结合动力学。

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