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Avoiding Misannotation of In-Source Fragmentation Products as Cellular Metabolites in Liquid Chromatography-Mass Spectrometry-Based Metabolomics

机译:避免基于液相色谱-质谱联用的代谢组学中源分解产物作为细胞代谢物的误判

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Liquid chromatographymass spectrometry (LC-MS) technology allows for rapid quantitation of cellular metabolites, with metabolites identified by mass spectrometry and chromatographic retention time. Recently, with the development of rapid scanning high-resolution high accuracy mass spectrometers and the desire for high throughput screening, minimal or no chromatographic separation has become increasingly popular. When analyzing complex cellular extracts, however, the lack of chromatographic separation could potentially result in misannotation of structurally related metabolites. Here, we show that, even using electrospray ionization, a soft ionization method, in-source fragmentation generates unwanted byproducts of identical mass to common metabolites. For example, nucleotide-triphosphates generate nucleotide-diphosphates, and hexose-phosphates generate triose-phosphates. We evaluated yeast intracellular metabolite extracts and found more than 20 cases of in-source fragments that mimic common metabolites. Accordingly, chromatographic separation is required for accurate quantitation of many common cellular metabolites.
机译:液相色谱质谱(LC-MS)技术可对细胞代谢产物进行快速定量,并通过质谱和色谱保留时间鉴定代谢产物。近来,随着快速扫描高分辨率高精度质谱仪的发展以及对高通量筛选的期望,最小或没有色谱分离已变得越来越流行。但是,当分析复杂的细胞提取物时,缺乏色谱分离可能会导致结构相关代谢物的错误注释。在这里,我们表明,即使使用电喷雾电离,一种软电离方法,源内裂解也会产生与常见代谢物质量相同的有害副产物。例如,核苷酸三磷酸产生核苷酸二磷酸,而己糖磷酸产生磷酸三糖。我们评估了酵母细胞内代谢产物的提取物,发现了20多个模拟常见代谢产物的源片段。因此,需要进行色谱分离才能准确定量许多常见的细胞代谢物。

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