首页> 外文期刊>Clinical Chemistry: Journal of the American Association for Clinical Chemists >Speciation and Quantification of Thiols by Reversed-Phase Chromatography Coupled with On-Line Chemical Vapor Generation and Atomic Fluorescence Spectrometric Detection: Method Validation and Preliminary Application for Glutathione Measurements in Human Whole Blood
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Speciation and Quantification of Thiols by Reversed-Phase Chromatography Coupled with On-Line Chemical Vapor Generation and Atomic Fluorescence Spectrometric Detection: Method Validation and Preliminary Application for Glutathione Measurements in Human Whole Blood

机译:反相色谱结合在线化学蒸气发生和原子荧光光谱法检测硫醇的形态和定量:人全血中谷胱甘肽测定的方法验证和初步应用

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Background: We developed a sensitive, specific method for the low–molecular-mass thiols cysteine, cysteinylglycine, glutathione, and homocysteine and validated the method for measurement of glutathione in blood.Methods: The technique was based on reversed-phase chromatography (RPC) coupled on line with cold vapor generation atomic fluorescence spectrometry (CVGAFS). Thiols were derivatized before introduction on the column by use of a p -hydroxymercuribenzoate (PHMB) mercurial probe and separated as thiol-PHMB complexes on a Vydac C4 column. Postcolumn on-line reaction of derivatized thiols with bromine allowed rapid conversion of the thiol-PHMB complexes to inorganic mercury with recovery of 100 (2)% of the sample. HgII was selectively detected by atomic fluorescence spectrometry in an Ar/H2 miniaturized flame after sodium borohydride reduction to Hg.Results: The relationship between thiol-PHMB complex concentration and peak area (CVGAFS signal) was linear over the concentration range 0.01–1400 μmol/L (injected). The detection limits were 1, 1, 0.6, and 0.8 nmol/L for cysteine, cysteinylglycine, homocysteine, and glutathione in the injected sample, respectively. The CVs for thiols were 1.5%–2.2% for calibrator solutions and 2.1% and 3.0% for real samples. The RPC-CVGAFS method allowed speciation of glutathione (reduced and oxidized) in human whole blood from healthy donors and from the coronary sinus of patients with idiopathic dilated cardiomyopathy during and after chronotropic stress.Conclusion: The RPC-CVGAFS method could be used to measure reduced and oxidized glutathione in human whole blood as disease biomarkers.
机译:背景:我们开发了一种灵敏,特异的低分子硫醇半胱氨酸,半胱氨酰甘氨酸,谷胱甘肽和高半胱氨酸的测定方法,并验证了血液中谷胱甘肽的测定方法。方法:该技术基于反相色谱(RPC)与冷蒸气发生原子荧光光谱法(CVGAFS)在线耦合。硫醇在引入对羟基苯硫基苯甲酸(PHMB)汞离子探针之​​前被衍生化,并在Vydac C4色谱柱上以硫醇-PHMB配合物的形式分离。衍生的硫醇与溴的柱后在线反应可将硫醇-PHMB配合物快速转化为无机汞,回收率为样品的100(2)%。在硼氢化钠还原成Hg后,在Ar / H2微型火焰中通过原子荧光光谱法选择性地检测HgII。结果:在0.01-1400μmol/浓度范围内,硫醇-PHMB络合物浓度与峰面积(CVGAFS信号)之间的关系呈线性关系。 L(注入)。进样中半胱氨酸,半胱氨酰甘氨酸,高半胱氨酸和谷胱甘肽的检出限分别为1、1、0.6和0.8 nmol / L。校准溶液的硫醇CV为1.5%–2.2%,真实样品的CV为2.1%和3.0%。 RPC-CVGAFS方法可在变应性应激期间和之后从健康供体和特发性扩张型心肌病患者的冠状窦中提取人全血中的谷胱甘肽(还原和氧化)。结论:RPC-CVGAFS方法可用于测量还原和氧化人类全血中的谷胱甘肽作为疾病的生物标记。

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