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一种结合 LC-MS/MS 和 LC-MS 的多方法,用于定量人血清中的碘甲状腺原氨酸。

A combined LC-MS/MS and LC-MS multi-method for the quantification of iodothyronines in human blood serum.

机构信息

Institut für Experimentelle Endokrinologie, Charité-Universitätsmedizin Berlin, Augustenburger Platz 1, 13353, Berlin, Germany.

Department of Analytical Chemistry, A. Menarini Research & Business Service GmbH, Glienicker Weg 125, 12489, Berlin, Germany.

出版信息

Anal Bioanal Chem. 2019 Aug;411(21):5605-5616. doi: 10.1007/s00216-019-01941-9. Epub 2019 Jun 15.

Abstract

We report here a novel approach for the extraction and analysis of thyroid hormones (TH) and their metabolites (THM) from human serum samples. Our method features a compact, 96-well micro-titre plate-based pre-analytic extraction/clean-up workflow combined with an isotope dilution LC-MS/MS-MS analytical method. In particular, these features make possible the detection of iodothyronines at their endogenous concentrations in serum differing by a factor of ca. 10, with potential to semi-automate the pre-analytics. The method was validated by the assessment of linearity, lower limits of quantification and detection (LLOQ and LLOD respectively), intra- and inter-day accuracy, precision, process efficiency (PE), matrix effect (ME) and relative recovery (RE). Calibration curves were linear in the concentration range in sample matrix from 0.1-250 nM for T, rT, T and 3-TAM and from 0.005-1 nM for 3,5-T and 3,3'-T. Using a 200-μL sample volume, the analyte dependant LLOQ were in the range 0.005 (3,5-T) to 0.25 (T) nM and LLOD were between 0.002 (3,5-T) and 0.052 nM (T). We applied the LC-MS/MS-MS method to the analysis of a cross section of patients with disorders of the thyroid hormone axis. T, T and rT concentrations (± standard deviation) were 120 ± 18, 1.9 ± 0.4 and 0.45 ± 0.09 nM respectively. 3,3'-T concentrations (± standard deviation) were 0.079 ± 0.022 nM; 3,5-T concentrations were below the LLOQ and/or LLOD in all but a single sample (0.013 nM). This method expands the analytical spectrum to endogenous thyroid hormone metabolites such as 3,5-T which exert biological actions and rT which may act as surrogate markers for disturbed thyroid hormone metabolism. Graphical abstract.

摘要

我们在此报告一种从人血清样本中提取和分析甲状腺激素 (TH) 和其代谢物 (THM) 的新方法。我们的方法具有紧凑的、基于 96 孔微量滴定板的预分析提取/净化工作流程,结合同位素稀释 LC-MS/MS-MS 分析方法。特别是,这些特点使得有可能以血清中内源性浓度的 10 倍差异检测碘甲状腺原氨酸,并且有可能半自动化预分析。该方法通过评估线性、定量下限和检测下限 (LLOQ 和 LLOD 分别)、日内和日间精密度、过程效率 (PE)、基质效应 (ME) 和相对回收率 (RE) 进行验证。校准曲线在样品基质中的浓度范围内呈线性,范围为 0.1-250 nM 用于 T、rT、T 和 3-TAM,0.005-1 nM 用于 3,5-T 和 3,3'-T。使用 200μL 样品体积,分析物依赖的 LLOQ 在 0.005(3,5-T)至 0.25(T)nM 范围内,LLOQ 在 0.002(3,5-T)至 0.052 nM(T)范围内。我们将 LC-MS/MS-MS 方法应用于甲状腺激素轴紊乱患者的横断面分析。T、T 和 rT 浓度(±标准偏差)分别为 120±18、1.9±0.4 和 0.45±0.09 nM。3,3'-T 浓度(±标准偏差)为 0.079±0.022 nM;3,5-T 浓度在除单个样本(0.013 nM)之外的所有样本中均低于 LLOQ 和/或 LLOD。该方法扩展了分析谱,包括 3,5-T 等内源性甲状腺激素代谢物,这些代谢物具有生物作用,rT 可能作为甲状腺激素代谢紊乱的替代标志物。

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