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Optimized Fragmentation Improves the Identification of Peptides Cross-Linked by MS-Cleavable Reagents

机译:优化的碎片改善了由MS可切割的试剂交联的肽的鉴定

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摘要

Cross-linking mass spectrometry is becoming increasingly popular, and current advances are widening the applicability of the technique so that it can be utilized by nonspecialist laboratories. Specifically, the use of novel mass spectrometry -cleavable (MS-cleavable) reagents dramatically reduces the complexity of the data by providing (i) characteristic reporter ions and (ii) the mass of the individual peptides rather than that of the cross-linked moiety. However, optimum acquisition strategies to obtain the best-quality data for such cross-linkers with higher energy C-trap dissociation (HCD) alone are yet to be achieved. Therefore, we have carefully investigated and optimized MS parameters to facilitate the identification of disuccinimidyl-sulfoxide-based cross-links on HCD-equipped mass spectrometers. From the comparison of nine different fragmentation energies, we chose several stepped-HCD fragmentation methods that were evaluated on a variety of cross-linked proteins. The optimal stepped-HCD method was then directly compared with previously described methods using an Orbitrap Fusion Lumos Tribrid instrument using a high complexity sample. The final results indicate that our stepped-HCD method is able to identify more cross-links than other methods, mitigating the need for multistage MS-enabled (MSn) instrumentation and alternative dissociation techniques. Data are available via ProteomeXchange with identifier PXDO11861.
机译:交联质谱变得越来越流行,电流进步正在扩大该技术的适用性,以便通过非专科学家实验室利用它。具体地,使用新颖的质谱 - 可生育(MS可切割的)试剂通过提供(I)特征报告器离子和(ii)单个肽的质量而不是交联部分的质量来显着降低数据的复杂性。然而,为了获得具有较高能量C-Trap解离(HCD)的这种交联剂的最佳质量数据的最佳采集策略尚未实现。因此,我们已经仔细研究和优化的MS参数,以促进在HCD的质谱仪上识别基于硫氨酰 - 硫氧化物的交联。从九个不同的碎片能量的比较来看,我们选择了几种在各种交联蛋白上评估的阶梯式HCD碎片方法。然后将最佳的步骤-HCD方法与使用高复杂性样品的使用斜拉瓣融合Lumos TribrId仪器的先前描述的方法直接进行比较。最终结果表明,我们的船舶HCD方法能够识别比其他方法更多的交叉链接,减轻了对能够多级MS的(MSN)仪器和替代解离技术的需求。数据可通过Proteomexchange提供标识符PXDO11861。

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