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通过高速电子捕获解离傅里叶变换离子回旋共振质谱法对肽和蛋白质进行表征。

Peptide and protein characterization by high-rate electron capture dissociation Fourier transform ion cyclotron resonance mass spectrometry.

作者信息

Tsybin Youri O, Ramström Margareta, Witt Matthias, Baykut Gökhan, Håkansson Per

机构信息

Division of Ion Physics, Angström Laboratory, Uppsala University, Box 534, SE-751 21, Uppsala, Sweden.

出版信息

J Mass Spectrom. 2004 Jul;39(7):719-29. doi: 10.1002/jms.658.

Abstract

The analytical utility of the electron capture dissociation (ECD) technique, developed by McLafferty and co-workers, has substantially improved peptide and protein characterization using Fourier transform ion cyclotron resonance mass spectrometry (FTICR-MS). The limitations of the first ECD implementations on commercial instruments were eliminated by the employment of low-energy electron-injection systems based on indirectly heated dispenser cathodes. In particular, the ECD rate and reliability were greatly increased, enabling the combination of ECD/FTICR-MS with on-line liquid separation techniques. Further technique development allowed the combination of two rapid fragmentation techniques, high-rate ECD and infrared multiphoton dissociation (IRMPD), in a single experimental configuration. Simultaneous and consecutive irradiations of trapped ions with electrons and photons extended the possibilities for ion activation/dissociation and led to improved peptide and protein characterization. The application of high-rate ECD/FTICR-MS has demonstrated its power and unique capabilities in top-down sequencing of peptides and proteins, including characterization of post-translational modifications, improved sequencing of peptides with multiple disulfide bridges and secondary fragmentation (w-ion formation). Analysis of peptide mixtures has been accomplished using high-rate ECD in bottom-up mass spectrometry based on mixture separation by liquid chromatography and capillary electrophoresis. This paper summarizes the current impact of high-rate ECD/FTICR-MS for top-down and bottom-up mass spectrometry of peptides and proteins.

摘要

由麦克拉弗蒂及其同事开发的电子捕获解离(ECD)技术的分析效用,极大地改进了使用傅里叶变换离子回旋共振质谱(FTICR-MS)对肽和蛋白质的表征。基于间接加热的 dispenser 阴极的低能量电子注入系统的应用消除了商业仪器上首次实施 ECD 时的局限性。特别是,ECD 速率和可靠性大幅提高,使得 ECD/FTICR-MS 能够与在线液相分离技术相结合。进一步的技术发展允许在单一实验配置中结合两种快速碎片化技术,即高速 ECD 和红外多光子解离(IRMPD)。用电子和光子对捕获离子进行同时和连续照射扩展了离子活化/解离的可能性,并改进了对肽和蛋白质的表征。高速 ECD/FTICR-MS 的应用已在肽和蛋白质的自上而下测序中展示了其强大功能和独特能力,包括翻译后修饰的表征、具有多个二硫键的肽的改进测序以及二级碎片化(w 离子形成)。基于液相色谱和毛细管电泳的混合物分离,在自下而上的质谱分析中使用高速 ECD 完成了对肽混合物的分析。本文总结了高速 ECD/FTICR-MS 对肽和蛋白质的自上而下和自下而上质谱分析的当前影响。

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