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Fourier Transform-Ion Mobility-Orbitrap Mass Spectrometer: A Next-Generation Instrument for Native Mass Spectrometry

机译:傅里叶变换 - 离子迁移率 - 锻造质谱仪:用于天然质谱法的下一代仪器

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摘要

A new instrument configuration for native ion mobility-mass spectrometry (IM-MS) is described. Macromolecule ions are generated by using a static ESI source coupled to an RF ion funnel, and these ions are then mobility and mass analyzed using a periodic focusing drift tube IM analyzer and an Orbitrap mass spectrometer. The instrument design retains the capabilities for first-principles determination of rotationally averaged ion neutral collision cross sections and high-resolution measurements in both mobility and mass analysis modes for intact protein complexes. Operation in the IM mode utilizes FT-IMS modes (originally described by Knorr (Knorr, F. J. et al. Anal. Chem. 1985, 57(2), 402-406)), which provides a means to overcome the inherent duty cycle mismatch for drift tube (DT)-IM and Orbitrap mass analysis. The performance of the native ESI-FT-DT-IM-Orbitrap MS instrument was evaluated using the protein complexes Gln K (MW 44 kDa) and streptavidin (MW 53 kDa) bound to small molecules (ADP and biotin, respectively) and transthyretin (MW 56 kDa) bound to thyroxine and zinc.
机译:描述了用于天然离子迁移质谱(IM-MS)的新仪器配置。通过使用耦合到RF离子漏斗的静态ESI源产生大分子离子,然后使用周期性聚焦漂移管IM分析仪和横向质谱仪分析这些离子和肿块。仪器设计保留了第一原理测定的旋转平均离子中性碰撞横截面和高分辨率测量的能力,以及用于完整蛋白质复合物的迁移率和质量分析模式。 IM模式下的操作利用FT-IMS模式(最初由KNORR(KNORR,FJ等人)。肛门。化学。1985,57(2),402-406))提供了一种克服固有占空比失配的方法用于漂移管(DT) - 氨基岩质量分析。使用蛋白质复合物Gln K(MW44KDA)和链霉抗生物素蛋白(分别分别)和Transthyretin( MW 56 kda)与甲状腺和锌结合。

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