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基于数据非依赖采集/质谱联用(“HIAP-DIA”)的高通量、深度、血浆蛋白质组绝对定量分析。

High-throughput, in-depth and estimated absolute quantification of plasma proteome using data-independent acquisition/mass spectrometry ("HIAP-DIA").

机构信息

The Key Laboratory of Carbohydrate Chemistry & Biotechnology, Ministry of Education, School of Biotechnology, Jiangnan University, Wuxi, China.

College of Life Science, Northwest University, Xi'an, China.

出版信息

Proteomics. 2021 Mar;21(5):e2000264. doi: 10.1002/pmic.202000264. Epub 2021 Feb 23.

DOI:10.1002/pmic.202000264
PMID:33460299
Abstract

Mass spectrometry-based plasma proteomics has been demonstrated to be a useful tool capable of quantifying hundreds of proteins in a single LC-MS/MS experiment, for biomarker discovery or elucidation of disease mechanisms. We developed a novel data-independent acquisition (DIA)/MS-based workflow for high-throughput, in-depth and estimated absolute quantification of plasma proteins (termed HIAP-DIA), without depleting high-abundant proteins, in a single-shot experiment. In HIAP-DIA workflow, we generated an ultra-deep cumulative undepleted and depleted spectral library which contained 55,157 peptides and 5,328 proteins, optimized column length (50 cm) and gradient (90 min) of liquid chromatography instrumentation, optimized 50 DIA segments with average isolation window 17 Th, and selected reference proteins for estimated absolute quantification of all plasma proteins. A total of 606 proteins were quantified in triplicate, and 427 proteins were quantified with CV <20% in plasma proteome. R-squared value of overlapped 208 endogenous PQ500 estimated protein amounts from HIAP-DIA and absolute quantification with internal standards was 0.82, indicating high quantification accuracy of HIAP-DIA. As a pilot study, the HIAP-DIA approach described here was applied to a myelodysplastic syndromes (MDS) disease cohort. We achieved absolute quantification of 789 plasma proteins in 22 clinical plasma samples, spanning less than six orders of magnitude with quantification limit 10-20 ng/mL, and discovered 95 differentially expressed proteins providing insights into MDS pathophysiology.

摘要

基于质谱的血浆蛋白质组学已被证明是一种有用的工具,能够在单个 LC-MS/MS 实验中定量数百种蛋白质,用于发现生物标志物或阐明疾病机制。我们开发了一种新的基于数据非依赖性采集(DIA)/MS 的高通量、深度和估计绝对定量血浆蛋白质的工作流程(称为 HIAP-DIA),无需耗尽高丰度蛋白质,在单次实验中。在 HIAP-DIA 工作流程中,我们生成了一个超深度累积未耗尽和耗尽的光谱库,其中包含 55,157 个肽和 5,328 个蛋白质,优化了液相色谱仪器的柱长(50 cm)和梯度(90 min),优化了 50 个 DIA 段,平均分离窗口为 17 Th,并选择了参考蛋白质,用于估计所有血浆蛋白质的绝对定量。在三重重复中定量了 606 种蛋白质,在血浆蛋白质组中定量了 427 种蛋白质,CV <20%。HIAP-DIA 和内标绝对定量重叠的 208 种内源性 PQ500 估计蛋白质数量的 R 平方值为 0.82,表明 HIAP-DIA 的定量准确性很高。作为一项试点研究,这里描述的 HIAP-DIA 方法应用于骨髓增生异常综合征(MDS)疾病队列。我们在 22 个临床血浆样本中实现了 789 种血浆蛋白质的绝对定量,跨越了不到六个数量级,定量限为 10-20 ng/mL,发现了 95 种差异表达的蛋白质,为 MDS 病理生理学提供了新的见解。

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