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傅里叶变换离子回旋共振质谱高分辨分析:从无机盐簇到抗体偶联物及其他。

High Mass Analysis with a Fourier Transform Ion Cyclotron Resonance Mass Spectrometer: From Inorganic Salt Clusters to Antibody Conjugates and Beyond.

机构信息

Amgen Research, Amgen Inc, Thousand Oaks, California 91320, United States.

Department of Chemistry and Biochemistry, and Department of Biological Chemistry, University of California-Los Angeles, Los Angeles, California 90095, United States.

出版信息

J Am Soc Mass Spectrom. 2020 May 6;31(5):1155-1162. doi: 10.1021/jasms.0c00030. Epub 2020 Apr 2.

Abstract

Analysis of proteins and complexes under native mass spectrometric (MS) and solution conditions was typically performed using time-of-flight (ToF) analyzers, due to their routine high / transmission and detection capabilities. However, over recent years, the ability of Orbitrap-based mass spectrometers to transmit and detect a range of high molecular weight species is well documented. Herein, we describe how a 15 Tesla Fourier transform ion cyclotron resonance mass spectrometer (15 T FT-ICR MS) is more than capable of analyzing a wide range of ions in the high / scale (>5000), in both positive and negative instrument polarities, ranging from the inorganic cesium iodide salt clusters; a humanized IgG1 monoclonal antibody (mAb; 148.2 kDa); an IgG1-mertansine drug conjugate (148.5 kDa, drug-to-antibody ratio; DAR 2.26); an IgG1-siRNA conjugate (159.1 kDa; ribonucleic acid to antibody ratio; RAR 1); the membrane protein aquaporin-Z (97.2 kDa) liberated from a C8E4 detergent micelle; the empty MSP1D1-nanodisc (142.5 kDa) and the tetradecameric chaperone protein complex GroEL (806.2 kDa; GroEL dimer at 1.6 MDa). We also investigate different regions of the FT-ICR MS that impact ion transmission and desolvation. Finally, we demonstrate how the transmission of these species and resultant spectra are highly consistent with those previously generated on both quadrupole-ToF (Q-ToF) and Orbitrap instrumentation. This report serves as an impactful example of how FT-ICR mass analyzers are competitive to Q-ToFs and Orbitraps for high mass detection at high /.

摘要

在天然质谱(MS)和溶液条件下分析蛋白质和复合物,通常使用飞行时间(ToF)分析仪,因为它们具有常规的高传输和检测能力。然而,近年来,基于轨道阱的质谱仪传输和检测一系列高分子量物质的能力已得到充分证明。本文描述了 15 特斯拉傅里叶变换离子回旋共振质谱仪(15 T FT-ICR MS)如何能够在高分辨 (>5000)范围内分析多种离子,无论是正离子还是负离子,范围从无机碘化铯盐簇;一种人源化 IgG1 单克隆抗体(mAb;148.2 kDa);一种 IgG1-美登素药物偶联物(148.5 kDa,药物与抗体比;DAR 2.26);一种 IgG1-siRNA 偶联物(159.1 kDa;核酸与抗体比;RAR 1);从 C8E4 去污剂胶束中释放的水通道蛋白-Z(97.2 kDa);空 MSP1D1-纳米碟(142.5 kDa)和十四聚体伴侣蛋白复合物 GroEL(806.2 kDa;GroEL 二聚体为 1.6 MDa)。我们还研究了影响离子传输和去溶剂化的 FT-ICR MS 的不同区域。最后,我们证明了这些物质的传输及其产生的光谱与之前在四极杆-ToF(Q-ToF)和轨道阱仪器上生成的光谱高度一致。本报告有力地证明了 FT-ICR 质谱仪如何与 Q-ToF 和轨道阱竞争,以实现高分辨下的高分子量检测。

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