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Combination of Sustained Off-Resonance Irradiation and On-Resonance Excitation in FT-ICR

机译:FT-ICR中持续非共振辐射与共振激发的结合

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Fourier transform ion cyclotron resonance (FT-ICR) mass spectrometry is becoming more widely used among the mass spectrometric techniques and has excellent figures of merit. Ion activation and fragmentation via sustained off-resonance irradiation (SORI) collision-induced dissociation (CID) is commonly used in FT-ICR. However, one of the limitations of SORI-CID is that only low-energy processes are typically observed in the product ion spectra. Here we present another option for performing CID in FT-ICR, a combination of SORI and on-resonance excitation (RE), termed SORI-RE. In comparison to SORI, this method produces more abundant ions resulting from higher energy fragmentation pathways. The result is the observation of a significant abundance of both higher and lower energy fragmentation pathways in the same mass spectrum. The comparison of SORI, RE, and SORI-RE spectra may lead to mechanistic insights as the relative abundances of certain fragment ions change as a function of internal energy deposition. This technique is simple to incorporate in existing instruments, does not require hardware or software modification, and requires only an additional 20-40 ms acquisition time. The technique is illustrated for a peptide (YGGFL), two disaccharides differing in the position of the glycosidic linkage (2alpha-mannobiose, 3alpha-mannobiose), an oligosaccharide (Alditol XT), a small protein (ubiquitin), and an inorganic cation (UO_(2)~(+)). Examples of higher energy fragmentation path-ways enhanced by SORI-RE include the formation of immonium ions and oligosaccharide cross-ring cleavages.
机译:傅立叶变换离子回旋共振(FT-ICR)质谱在质谱技术中正变得越来越广泛,并且具有优异的品质因数。 FT-ICR通常使用通过持续非共振辐射(SORI)碰撞诱导的离解(CID)进行离子活化和破碎。但是,SORI-CID的局限性之一是在产物离子谱图中通常仅观察到低能过程。在这里,我们介绍了另一种在FT-ICR中执行CID的选项,即SORI和共振激励(RE)的组合,称为SORI-RE。与SORI相比,此方法由于较高的能量碎裂途径而产生了更多的离子。结果是在相同的质谱图中观察到大量的较高和较低的能量裂解途径。由于某些碎片离子的相对丰度随内部能量沉积的变化而变化,因此SORI,RE和SORI-RE光谱的比较可能会导致机理上的洞察。该技术很容易集成到现有仪器中,不需要硬件或软件的修改,并且仅需要额外的20-40 ms的采集时间。说明了该技术的一种肽(YGGFL),两个在糖苷键位置不同的二糖(2alpha-甘露二糖,3alpha-甘露二糖),低聚糖(Alditol XT),小蛋白(泛素)和无机阳离子( UO_(2)〜(+))。通过SORI-RE增强的高能碎裂途径的例子包括形成铵离子和寡糖交叉环裂解。

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