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Effects of Freeze-Thaw Cycles of Blood Samples on High-Coverage Quantitative Metabolomics

机译:血液样品冻融循环对高覆盖量性代谢皂炎的影响

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摘要

Blood metabolomics has been widely used for discovering potential metabolite biomarkers of various diseases. In this study, we report our investigation of the effects of freeze-thaw cycles (FTCs) of human serum samples on quantitative metabolomics using a differential chemical isotope labeling (CIL) LC-MS method. A total of 99 serum samples collected from healthy individuals (47 females and 52 males) were subjected to five FTCs, followed by C-12-/C-13-dansylation labeling LC-MS analysis. A total of 2790 peak pairs or metabolites were relatively quantified among the 495 comparative samples, including 150 positively identified metabolites, 235 high-confident putatively identified metabolites and 1949 mass-matched metabolites from database searches. Multivariate analysis of the metabolome data showed a clustering of the third to fifth FTC samples in contrast to the separation of the first and second FTC samples, indicating that the extent of FTC-induced metabolome changes became smaller after the third cycle. The changing patterns among the FTC-effected metabolites were found to be complex. Using sex as a biological factor for grouping, we observed a clear separation of males and females when the samples were subjected to the same number of FTCs. However, when the male- and female-samples with different numbers of FTCs were compared, the number of significant metabolites found in male-female comparison increased dramatically, indicating that FTC effects could lead to a large number of false positives in biomarker discovery. Finally, we proposed a method of detecting the FTC effects by reanalyzing the original samples after subjecting them to an additional FTC.
机译:血液代谢物已被广泛用于发现各种疾病的潜在代谢产物生物标志物。在这项研究中,我们通过差分化学同位素标记(CIL)LC-MS方法向人血清样品对人血清样品的冻融循环(FTCS)对定量代谢组学的影响进行调查。从健康个体(47个女性和52个男性)收集的总共99个血清样品进行了五种FTCS,然后进行了C-12- / C-13-丹酰化标记LC-MS分析。在495个比较样品中,总共2790个峰对或代谢物相对量化,其中包括150个正鉴定的代谢物,235高自信地鉴定代谢物和1949年从数据库搜索的大规模匹配代谢物。与第一和第二FTC样品的分离相比,新代谢数据的多变量分析显示第三至第五FTC样品的聚类,表明在第三周期之后FTC诱导的代谢物变化的程度变得更小。发现FTC效果代谢物中的变化模式是复杂的。用性作为分组的生物因素,当样品经受相同数量的FTCs时,我们观察到较清楚的雄性和女性分离。然而,当比较具有不同数量的FTCS的男性和雌性样本时,男性对比较中发现的显着代谢物的数量显着增加,表明FTC效应可能导致生物标志物发现中的大量误报。最后,我们提出了一种通过在将原始样本进行重新定位到额外的FTC之后重新分析原始样品来检测FTC效应的方法。

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  • 来源
    《Analytical chemistry》 |2020年第13期|共8页
  • 作者单位

    Zhejiang Univ Natl Clin Res Ctr Infect Dis Affiliated Hosp 1 State Key Lab Diag &

    Treatment Coll Med Collaborat Innovat Ctr Diag &

    Treatment Hangzhou 310003 Peoples R China;

    Univ Alberta Dept Chem Edmonton AB T6G 2G2 Canada;

    Univ Alberta Dept Chem Edmonton AB T6G 2G2 Canada;

    Zhejiang Univ Natl Clin Res Ctr Infect Dis Affiliated Hosp 1 State Key Lab Diag &

    Treatment Coll Med Collaborat Innovat Ctr Diag &

    Treatment Hangzhou 310003 Peoples R China;

    Zhejiang Univ Natl Clin Res Ctr Infect Dis Affiliated Hosp 1 State Key Lab Diag &

    Treatment Coll Med Collaborat Innovat Ctr Diag &

    Treatment Hangzhou 310003 Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
  • 关键词

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