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首页> 外文期刊>Analytical and bioanalytical chemistry >Quantification of CYP2E1 in rat liver by UPLC-MS/MS-based targeted proteomics assay: a novel approach for enzyme activity assessment
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Quantification of CYP2E1 in rat liver by UPLC-MS/MS-based targeted proteomics assay: a novel approach for enzyme activity assessment

机译:UPLC-MS / MS的靶向蛋白质组学测定法量化大鼠肝脏CYP2E1:一种新型酶活性评估方法

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摘要

CYP2E1 is one of the most crucial isozymes of CYP450. It is responsible for metabolizing and activating a large number of toxicants and carcinogens, but the correlation between its abundance and activity has not been widely studied. With the flourishing of modern mass spectrometry technology, quantifying complex biological proteins and studying the relationship between their abundance and activity have become practicable. In our study, an accurate, sensitive, and stable LC-MS/MS-based method was developed and validated. The method can accurately quantify the abundance of CYP2E1 in the rat liver microsome and S9 fraction. The quantitative linearity of the method is between 2 and 320 ng/mL, and the run time is 16.5 minutes. Meanwhile, we used the probe substrate method (with chlorzoxazone as the substrate) as a reference to analyze the correlation between its activity and abundance. The result illustrated that the abundance of CYP2E1 by LC-MS/MS has a strong positive correlation with its activity. This is a relationship worth studying, which has not been reported before. We also explored the correlation between quantitative results by traditional methods (western blot and RT-PCR) and activity, and the positive correlation was not obvious. Therefore, when testing the correlation between metabolic enzyme abundance and activity, the LC-MS/MS-based method is confirmed to be more accurate than conventional methods. It will provide a meaningful way of researching the metabolic enzymes in drug interactions. Furthermore, we found that the S9 fraction can also be used for mass spectrometry quantitative analysis, which is helpful for promoting the practical application of targeted protein technology.
机译:CYP2E1是CYP450最关键的同工酶之一。它负责代谢和激活大量毒物和致癌剂,但其丰度和活性之间的相关性尚未被广泛研究。随着现代质谱技术的蓬勃发展,量化复杂的生物蛋白并研究其丰富和活性之间的关系已经变得可行。在我们的研究中,开发并验证了准确,敏感和稳定的LC-MS / MS的方法。该方法可以精确地量化大鼠肝微粒组和S9分数中的CYP2E1的丰度。该方法的定量线性度在2至320ng / ml之间,并且运行时间为16.5分钟。同时,我们使用探针底物法(用氯噻嗪酮作为基质)作为参考分析其活性和丰度之间的相关性。结果表明,LC-MS / MS的CYP2E1的丰度与其活性具有强烈的正相关。这是一种值得学习的关系,尚未以前则报告。我们还通过传统方法(Western Blot和RT-PCR)和活性来探讨定量结果之间的相关性,并且正相关并不明显。因此,当测试代谢酶丰度和活性之间的相关性时,基于LC-MS / MS的方法被证实比常规方法更准确。它将提供一种有意义的方法来研究药物相互作用中的代谢酶。此外,我们发现S9级分也可用于质谱定量分析,这有助于促进靶向蛋白质技术的实际应用。

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  • 作者单位

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Cent South Univ Xiangya Sch Pharmaceut Sci 172 Tongzipo Rd Changsha 410013 Hunan Peoples R China;

    Hunan Key Lab Bioanal Complex Matrix Samples C10 Bldg Lugu S&

    T Pk 28 Lutian Rd Changsha 410205 Hunan 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

    UPLC-MS; MS; Targeted proteomics assay; Enzyme activity;

    机译:UPLC-MS;MS;靶向蛋白质组学测定;酶活性;

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