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4D-diaXLMS:用于交联质谱的蛋白质组学全范围四维数据非依赖性采集工作流程。

4D-diaXLMS: Proteome-wide Four-Dimensional Data-Independent Acquisition Workflow for Cross-Linking Mass Spectrometry.

机构信息

The Institute for Advanced Studies, Wuhan University, Wuhan, Hubei 430072, China.

出版信息

Anal Chem. 2023 Sep 19;95(37):14077-14085. doi: 10.1021/acs.analchem.3c02824. Epub 2023 Sep 10.

Abstract

Cross-linking mass spectrometry (XL-MS) is a powerful tool for examining protein structures and interactions. Nevertheless, analysis of low-abundance cross-linked peptides is often limited in the data-dependent acquisition (DDA) mode due to its semistochastic nature. To address this issue, we introduced a workflow called 4D-diaXLMS, representing the first-ever application of four-dimensional data-independent acquisition for proteome-wide cross-linking analysis. Cross-linking studies of the HeLa cell proteome were evaluated using the classical cross-linker disuccinimidyl suberate as an example. Compared with the DDA analysis, 4D-diaXLMS exhibited marked improvement in the identification coverage of cross-linked peptides, with a total increase of 36% in single-shot analysis across all 16 SCX fractions. This advantage was further amplified when reducing the fraction number to 8 and 4, resulting in 125 and 149% improvements, respectively. Using 4D-diaXLMS, up to 83% of the cross-linked peptides were repeatedly identified in three replicates, more than twice the 38% in the DDA mode. Furthermore, 4D-diaXLMS showed good performance in the quantitative analysis of yeast cross-linked peptides even in a 15-fold excess amount of HeLa cell matrix, with a low coefficient of variation and high quantitative accuracies in all concentrations. Overall, 4D-diaXLMS was proven to have high coverage, good reproducibility, and accurate quantification for in-depth XL-MS analysis in complex samples, demonstrating its immense potential for advances in the field.

摘要

交联质谱(XL-MS)是一种用于研究蛋白质结构和相互作用的强大工具。然而,由于其半随机性质,低丰度交联肽的分析在数据依赖采集(DDA)模式下通常受到限制。为了解决这个问题,我们引入了一种称为 4D-diaXLMS 的工作流程,这代表了用于蛋白质组范围交联分析的四维数据独立采集的首次应用。使用经典交联剂二琥珀酰亚胺琥珀酸酯作为示例,评估了 HeLa 细胞蛋白质组的交联研究。与 DDA 分析相比,4D-diaXLMS 显著提高了交联肽的鉴定覆盖率,在所有 16 个 SCX 馏分的单次分析中总增加了 36%。当减少馏分数到 8 和 4 时,这一优势进一步放大,分别增加了 125%和 149%。使用 4D-diaXLMS,高达 83%的交联肽在三个重复中被重复鉴定,是 DDA 模式下 38%的两倍多。此外,4D-diaXLMS 在定量分析酵母交联肽方面表现良好,即使在 HeLa 细胞基质的 15 倍过量情况下,所有浓度的变异系数都很低,定量准确性也很高。总的来说,4D-diaXLMS 被证明在复杂样品的深入 XL-MS 分析中具有高覆盖率、良好的重现性和准确的定量,为该领域的进展展示了巨大的潜力。

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