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首页> 外文期刊>Journal of chromatography, A: Including electrophoresis and other separation methods >Multifunctional isotopic standards based steroidomics strategy: Exploration of cancer screening model
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Multifunctional isotopic standards based steroidomics strategy: Exploration of cancer screening model

机译:基于多功能同位素标准的甾体组策略:癌症筛查模型的探索

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Quantitative determination of endogenous compounds in biological samples has still been challenged by the absence of authentic blank matrix. Alternative strategy of surrogate matrix for preparing reference samples are prevalent due to its low cost and high availability. However, the evaluation system of surrogate matrix is not perfect. Herein, a novel multifunctional isotopic standards based steroidomics strategy was developed. Isotope-labeled standards were used not only as internal standards but also for the evaluation the feasibility of surrogate matrix, which improved the accuracy of assessment and could provide a new prospect for the quantitative analysis of endogenous compounds. Based on this approach, a detailed optimization from LC separation, MS detection to extraction conditions for global steroids in the steroidogenesis was firstly carried out. Characteristics and regularities of steroids in LC-MS were summarized to make references for further targeted or untargeted steroidomics study. Then eighteen steroids were quantified with high accuracy and high sensitivity in plasma from four types of cancer patients and healthy subjects using 1% BSA in PBS as surrogate matrix. And multi-steroids indexes with the best discriminating ability for lung, colorectal, breast and gastric cancer in different genders were identified successfully with Student's t-test, PLS-DA and logistic regression- ROC curve analysis. Finally, efficient cancer screening workflow was established by integrating the amine submetabolomics and lipidomics data of our previous studies. Taken together, the integrated steroidomics strategy could shed a light on the guidance for further steroidome as well as other endogenous compounds analysis and may provide a powerful tool for cancer diagnosis. (C) 2019 Published by Elsevier B.V.
机译:通过不存在真实的空白基质,仍然挑战了生物样品中内源化合物的定量测定。由于其低成本和高可用性,用于制备参考样品的替代矩阵的替代策略是普遍的。然而,代理矩阵的评估系统并不完美。在此,开发了一种新型多功能同位素标准品标准术术策略。同位素标记的标准不仅是内部标准,还用于评估替代矩阵的可行性,这提高了评估的准确性,并可能为内源化合物的定量分析提供了新的前景。基于这种方法,首先进行了从LC分离,MS检测对类固醇中全球类固醇的提取条件的详细优化。总结了LC-MS中类固醇的特征和规律,以制备进一步有针对性或未明确的甾体组学研究的参考。然后在PBS中的四种类型的癌症患者和健康受试者的血浆中以高精度和高敏感性量化了18种类固醇,以PBS为替代基质,以1%BSA为蛋白质患者和健康受试者。与学生的T检验,PLS-DA和Logistic回归 - Roc曲线分析成功地鉴定了不同性别肺,结直肠癌,乳腺癌和胃癌的多种类固醇指标,并以不同的是不同的性别。最后,通过整合我们以前研究的胺潜鼠和脂质族数据来建立有效的癌症筛查工作流程。综合,综合甾体组策略可以在进一步的甾体和其他内源化合物分析的指导下揭示光线,并且可以为癌症诊断提供强大的工具。 (c)2019年由elestvier b.v发布。

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