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首页> 外文期刊>Journal of chromatography, B. Analytical technologies in the biomedical and life sciences >Simple LC-MS/MS method using core-shell ODS microparticles for the simultaneous quantitation of edoxaban and its major metabolites in human plasma
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Simple LC-MS/MS method using core-shell ODS microparticles for the simultaneous quantitation of edoxaban and its major metabolites in human plasma

机译:简单的LC-MS / MS方法使用核心壳ODS微粒用于同时定量Edoxaban及其在人血浆中的主要代谢物

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摘要

Edoxaban is mainly enzymatically converted to a 4-carboxylic acid form (4CA-EDX) and an N-desmethyl form (ND-EDX) in humans. This study aimed to establish a simple liquid chromatography-tandem mass spectrometry method using core-shell octadecyl silica (ODS) microparticles for the simultaneous quantitation of edoxaban and its two major metabolites in human plasma. Analytes extracted from plasma specimens by a one-step deproteinization were separated using a 2.6-mu m core-shell ODS microparticulate column and linear acetonitrile-ammonium acetate gradient elution at a flow rate of 0.25 mL/min with a run time of 7 min. The mass spectrometer was operated in the positive ion multiple reaction monitoring mode. Plasma samples collected from 20 patients with atrial fibrillation were analyzed by the present method. The chromatograms of drug-free human plasma had no interfering peaks. The calibration curves of edoxaban, 4CA-EDX, and ND-EDX were linear over the concentration ranges of 1.25-160, 0.47-60, and 0.12-15 ng/mL, respectively. Their pretreatment recoveries and matrix factors were 88.7-109.0% and 87.0-101.6%, respectively. The intra- and inter-day accuracy and imprecision values were 85.9-112.8% and within 13.3%, respectively. The plasma concentrations of edoxaban, 4CA-EDX, and ND-EDX in the patients had ranges of 17.8-102, 1.67-25.7, and 0.685-5.34 ng/mL, respectively. All the analytes were measurable within their calibration curves. In conclusion, this validated method for the simultaneous determination of edoxaban and its major metabolites was successfully applied to plasma specimens obtained from patients with atrial fibrillation.
机译:Edoxaban主要是酶促转化为4-羧酸形式(4CA-EDX)和在人中的N-去甲基形式(ND-EDX)。本研究旨在建立一种使用核 - 壳十二烷基二氧化硅(ODS)微粒的简单液相色谱 - 串联质谱法,用于同时定量Edoxaban及其两种人血浆中的两种主要代谢物。使用一阶段脱蛋白从等离子体样本中提取的分析物使用2.6-mu m核 - 壳体ODS微粒微粒柱和线性乙腈 - 乙酸铵梯度洗脱,其流速为0.25ml / min,运行时间为7分钟。质谱仪在正离子多反应监测模式下操作。通过本方法分析从20例心房颤动患者收集的血浆样本。无毒人血浆的色谱图没有干扰峰。 Edoxaban,4CA-EDX和ND-EDX的校准曲线分别在1.25-160,0.47-60和0.12-15ng / ml的浓度范围内线性。他们的预处理回收率和基质因子分别为88.7-109.0%和87.0-101.6%。日内和日间准确性和不精确值分别为85.9-112.8%,分别以内13.3%。患者中Edoxaban,4CA-EDX和ND-EDX的血浆浓度分别为17.8-102,1.67-25.7和0.685-5.34ng / ml。所有分析物在其校准曲线内都可以测量。总之,这种验证的同时测定Edoxaban及其主要代谢物的方法成功地应用于从心房颤动患者获得的血浆标本。

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