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首页> 外文期刊>Talanta: The International Journal of Pure and Applied Analytical Chemistry >Integration of stable isotope labeling derivatization and magnetic dispersive solid phase extraction for measurement of neurosteroids by in vivo microdialysis and UHPLC-MS/MS
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Integration of stable isotope labeling derivatization and magnetic dispersive solid phase extraction for measurement of neurosteroids by in vivo microdialysis and UHPLC-MS/MS

机译:稳定同位素标记衍生化和磁性色散固相萃取在体内微透析和UHPLC-MS / MS测量神经激素的磁性色散固相提取

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摘要

In this work, a novel strategy of stable isotope labeling derivatization (SILD) combined with magnetic dispersive solid-phase extraction (MDSPE), has been proposed for simultaneous monitoring of neurosteroids changes linked to Parkinson's disease (PD) by in vivo microdialysis. The developed method was based on ultra-high performance liquid chromatography tandem mass spectrometry (UHPLC-MS/MS) detection using multiple-reaction monitoring (MRM) mode. In this study, a new pair of stable isotope labeling reagents d(0)-/d(3)-3-N-methyl-2'-carboxyl Rhodamine 6G (d(0)-/d(3)-MCR6G), were designed and synthesized for derivatizing neurosteroids in rat blood microdialysates and neurosteroid standards, respectively. d(3)-MCR6G labeled neurosteroids standards were used as internal standard for the following pretreatment and UHPLC-MS/MS quantification to minimize the deviations caused by complex matrix and ion suppression effects in mass spectrometry analysis. Under the optimized derivatization and extraction conditions, good linearities of eight neurosteroids were obtained with correlation coefficients R-2 values > 0.98. The limits of detection (LODs) and quantitation (LOQs) ranged from 0.06 to 0.12 pg/mL and 0.30-0.40 pg/mL, respectively. Taken together, the established method exhibited high sensitivity and selectivity, excellent accuracy, convenience and high efficiency. It was applied for the simultaneous and dynamic measurement of multiple neurosteroids in normal and PD rat blood microdialysates. This method would be expected to be potentially useful for the monitoring and drug treatment of PD and related neurological disorders in the future.
机译:在这项工作中,已经提出了一种与磁性色散固相萃取(MDSPE)结合的稳定同位素标记衍生化(Sild)的新策略,用于同时监测与帕金森病(PD)的神经活体改变通过体内微透析。使用多反应监测(MRM)模式,开发方法基于超高效液相色谱串联质谱(UHPLC-MS / MS)检测。在该研究中,一对新的稳定同位素标记试剂D(0) - / D(3)-3-n-甲基-2'-羧基罗丹明6g(d(0) - / d(3)-MCR6G),设计和合成,分别用于衍生化大鼠血液微透明酸盐和神经活体标准的神经硬化。 D(3)-MCR6G标记的神经硬化物标准物作为下列预处理和UHPLC-MS / MS定量的内标,以最小化由质谱分析中复杂基质和离子抑制效应引起的偏差。在优化的衍生化和提取条件下,使用相关系数R-2值R-2值,得到八个神经硬化的良好线性。检测限(LOD)和定量(LOQs)的极限分别为0.06至0.12pg / ml和0.30-0.40pg / ml。在一起,已建立的方法表现出高灵敏度和选择性,优异的准确性,方便,效率高。应用于正常和Pd大鼠血微透过的多种神经激素的同时和动态测量。预计该方法将可能在未来对Pd和相关神经障碍的监测和药物治疗有用。

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  • 作者单位

    Qufu Normal Univ Coll Chem &

    Chem Engn Key Lab Pharmaceut Intermediates &

    Anal Nat Med Qufu 273165 Shandong Peoples R China;

    Qufu Normal Univ Coll Chem &

    Chem Engn Key Lab Pharmaceut Intermediates &

    Anal Nat Med Qufu 273165 Shandong Peoples R China;

    Qufu Normal Univ Coll Chem &

    Chem Engn Key Lab Pharmaceut Intermediates &

    Anal Nat Med Qufu 273165 Shandong Peoples R China;

    Qufu Normal Univ Coll Chem &

    Chem Engn Key Lab Pharmaceut Intermediates &

    Anal Nat Med Qufu 273165 Shandong Peoples R China;

    Qufu Normal Univ Coll Chem &

    Chem Engn Key Lab Pharmaceut Intermediates &

    Anal Nat Med Qufu 273165 Shandong Peoples R China;

    Qufu Normal Univ Coll Chem &

    Chem Engn Key Lab Pharmaceut Intermediates &

    Anal Nat Med Qufu 273165 Shandong Peoples R China;

    Peking Univ Key Lab Bioorgan Chem &

    Mol Engn Beijing Natl Lab Mol Sci Minist Educ Inst Analyt Chem Coll Chem &

    Mol Engn Beijing 100871 Peoples R China;

    Peking Univ Key Lab Bioorgan Chem &

    Mol Engn Beijing Natl Lab Mol Sci Minist Educ Inst Analyt Chem Coll Chem &

    Mol Engn Beijing 100871 Peoples R China;

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

    Neurosteroids; Isotope-coded derivatization; Magnetic separation; Triple quadrupole mass spectrometry; In vivo microdialysis technique; Parkinson's disease;

    机译:神经活体;同位素编码衍生化;磁分离;三重四极杆质谱;在体内微透析技术;帕金森病;

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