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Identification of Human Serum Peptides in Fourier Transform Ion Cyclotron Resonance Precision Profiles

机译:傅立叶变换离子回旋加速器共振精密谱中人血清肽的鉴定

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The continuous efforts to find new prognostic or diagnostic biomarkers have stimulated the use of mass spectrometry (MS) profiles in a clinical setting. In the early days (about one decade ago), a single low-resolution mass spectrum derived from an individual’s body fluid was used for comparative studies. However, a peptide profile of a complex mixture is most informative when recorded on an ultrahigh resolution instrument such as a Fourier transform ion cyclotron resonance (FTICR) mass spectrometer. In this study we show the benefits of the ultrahigh resolving power and the high mass accuracy and precision provided by an FTICR mass spectrometer equipped with a 15-tesla magnet. The ultrahigh-resolution data not only allow assignment of fragment ions with high charge states (4+, 5+) but also enhance confidence of human serum peptide identifications from tandem MS experiments. This is exemplified with collision-induced dissociation (CID) and electron transfer dissociation (ETD) data of middle-down-sized endogenous or protein-breakdown peptides that are of interest in biomarker discovery studies.
机译:寻找新的预后或诊断生物标志物的不断努力刺激了在临床环境中质谱(MS)谱的使用。在早期(大约十年前),从个人体液获得的单个低分辨率质谱用于比较研究。但是,当在超高分辨率仪器(例如傅立叶变换离子回旋共振(FTICR)质谱仪)上进行记录时,复杂混合物的肽谱最为有用。在这项研究中,我们展示了配备15特斯拉磁体的FTICR质谱仪具有超高分辨能力以及高质量精度和精密度的优势。超高分辨率数据不仅允许分配具有高电荷态(4 +,5 +)的碎片离子,而且还增强了串联MS实验中人血清肽鉴定的可信度。生物标志物发现研究中感兴趣的中等大小的内源性或蛋白质分解肽的碰撞诱导解离(CID)和电子转移解离(ETD)数据就是例证。

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