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首页> 外文期刊>Rapid Communications in Mass Spectrometry: RCM >Metabolite identification by data-dependent accurate mass spectrometric analysis at resolving power of 60,000 in external calibration mode using an LTQ/Orbitrap
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Metabolite identification by data-dependent accurate mass spectrometric analysis at resolving power of 60,000 in external calibration mode using an LTQ/Orbitrap

机译:使用LTQ / Orbitrap在外部校准模式下通过数据相关的精确质谱分析鉴定代谢物,分辨能力为60,000

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Performance evaluation of accurate mass measurement by the LTQ/Orbitrap, at a resolving power of 60 000 and in external calibration mode, indicated that the Orbitrap is capable of providing high mass accuracy of <2ppm for over 24 h post-calibration. This, together with limited trade-off between sensitivity and resolving power plus a wide dynamic range for mass accuracy, suggested that the LTQ/Orbitrap is an ideal analytical tool for structural elucidation of metabolites. The application of the LTQ/Orbitrap to identification of human liver microsomal metabolites of carvedilol was evaluated, using parent mass list triggered data-dependent multiple-stage accurate mass analysis, at a resolving power of 60 000 in external calibration mode. A metabolite identification workflow was developed to utilize chemical formulas from high-resolution accurate mass measurements to confirm structures of product ions of a drug proposed by Mass Frontier, illustrated by identification of structures used to establish lineage of product ions of carvedilol, which later served as a template for identification of its metabolites. A total of 58 in vitro metabolites of carvedilol were detected using 5-ppm mass tolerance filters for theoretical m/z of protonated molecules of predicted metabolites in addition to product ions and neutral mass losses diagnostic of carvedilol. The chemical formulas with unsaturation numbers calculated from the accurate m/z of precursor and product ions can be used to assign, with a high degree of confidence, the structures of metabolites and the sites of metabolism. The mass accuracies obtained for all full scan MS and MS' spectra were <2 ppm. The majority of the metabolites identified agreed with those previously reported except for those that have not been reported before. For example, several glutathione conjugates of carvedilol were reported for the first time, which may explain the reported hepatotoxicity during clinical trials and recent clinical use. Copyright (C) 2007 John Wiley & Sons, Ltd.
机译:LTQ / Orbitrap在分辨率为60 000且在外部校准模式下对精确质量测量进行的性能评估表明,Orbitrap能够在校准后的24小时内提供<2ppm的高质量精度。这与灵敏度和分辨力之间的有限权衡以及质量精度的宽动态范围相结合,表明LTQ / Orbitrap是代谢物结构鉴定的理想分析工具。评估了LTQ / Orbitrap在鉴定卡维地洛人肝微粒体代谢产物中的应用,使用母体质量列表触发的数据相关的多阶段精确质量分析,在外部校准模式下的分辨力为60 000。开发了代谢物鉴定工作流程,以利用高分辨率精确质量测量中的化学式来确认Mass Frontier提出的药物的产物离子结构,通过鉴定用于建立卡维地洛产物离子谱系的结构举例说明,该结构后来被用作用于鉴定其代谢物的模板。除产物离子和卡维地洛的中性质量损失诊断外,使用5-ppm质量公差过滤器检测了总共58种卡维地洛的体外代谢物,用于预测代谢物的质子化分子的理论m / z。根据前体离子和产物离子的精确m / z计算出的具有不饱和数的化学式可用于高度可靠地分配代谢物的结构和代谢位点。所有全扫描MS和MS'质谱图的质量准确度均小于2 ppm。鉴定出的大多数代谢物与以前报道的代谢产物一致,但以前没有报道过。例如,首次报道了卡维地洛的几种谷胱甘肽结合物,这可以解释在临床试验和最近的临床使用中报道的肝毒性。版权所有(C)2007 John Wiley&Sons,Ltd.

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