A highly sensitive LC-MS-MS assay for analysis of midazolam and its major metabolite in human plasma: Applications to drug metabolism

Jabor VAP; Coelho EB; dos Santos NAG; Bonato PS; Lanchote VL

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A highly sensitive LC-MS-MS assay for analysis of midazolam and its major metabolite in human plasma: Applications to drug metabolism

机译：用于人血浆中咪达唑仑及其主要代谢物分析的高灵敏度LC-MS-MS分析方法：在药物代谢中的应用

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摘要

The present report describes a rapid, selective and a highly sensitive assay for midazolam (MDZ) and its major metabolite I-hydroxymidazolarn (l-OH-MDZ) in human plasma employing liquid chromatography-tandem mass spectrometry (LC-MS-MS) detection. The method involves liquid-liquid extraction sample clean-up, separation on a Purospher RP 18-e column and detection with an electrospray interface in the positive ion mode. The overall recoveries were about 100% and 80% for midazolam and 1-hydroxymidazolam, respectively. Accuracy, precision and linearity were acceptable for biological samples with quantitation limits of 0.1-100ngmL(-1) plasma for both analytes. The validated method was successfully applied to quantify plasma concentration of midazolam and 1-hydroxymidazolam in authentic samples from a healthy volunteer following a single 15 mg oral dose of midazolam (apparent total clearance: 3.47 L h(-1) kg(-1) and AUC(0-alpha)IOH-MDZ/MDZ: 0.338). (c) 2005 Elsevier B.V. All rights reserved.

机译：本报告介绍了使用液相色谱-串联质谱（LC-MS-MS）检测人血浆中的咪达唑仑（MDZ）及其主要代谢物I-羟基咪达唑仑（1-OH-MDZ）的快速，选择性和高灵敏度的测定方法。该方法包括液-液萃取样品净化，在Purospher RP 18-e色谱柱上分离以及在正离子模式下通过电喷雾界面进行检测。咪达唑仑和1-羟基咪达唑仑的总回收率分别约为100％和80％。两种样品的定量限为0.1-100ngmL（-1）的生物样品，其准确性，精密度和线性均可接受。经验证的方法已成功应用于从健康志愿者单次口服15 mg咪达唑仑（表观总清除率：3.47 L h（-1）kg（-1）和1.5 mg口服剂量的健康志愿者的真实样品中的咪达唑仑和1-羟基咪达唑仑的血浆浓度AUC（0-α）IOH-MDZ / MDZ：0.338）。（c）2005 Elsevier B.V.保留所有权利。

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《Journal of chromatography, B. Analytical technologies in the biomedical and life sciences》 |2005年第2期|共6页
作者
Jabor VAP; Coelho EB; dos Santos NAG; Bonato PS; Lanchote VL;
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正文语种 eng
中图分类分析化学;
关键词
midazolam; LC-MS-MS; plasma; pharmacokinetics; CYP3A4; TANDEM MASS-SPECTROMETRY; PERFORMANCE LIQUID-CHROMATOGRAPHY; IN-VITRO; CYP3A ACTIVITY; HUMAN SERUM; PROBE; 1-HYDROXYMIDAZOLAM; ENZYMES; 1'-HYDROXYMIDAZOLAM; 4-HYDROXYMIDAZOLAM;

机译：咪达唑仑;LC-MS-MS;血浆;药代动力学;CYP3A4;串联质谱;高效液相色谱;体外;CYP3A活性;人血清;探针;1-羟基咪唑啉;酶;4 -'-羟基;

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1. A highly sensitive LC-MS-MS assay for analysis of midazolam and its major metabolite in human plasma: Applications to drug metabolism [J] . Jabor VAP, Coelho EB, dos Santos NAG, Journal of chromatography, B. Analytical technologies in the biomedical and life sciences . 2005,第1a2期

机译：用于人血浆中咪达唑仑及其主要代谢物分析的高灵敏度LC-MS-MS分析方法：在药物代谢中的应用
2. Development a validated highly sensitive LC-MS/MS method for simultaneous quantification of Ledipasvir, sofosbuvir and its major metabolite GS-331007 in human plasma: Application to a human pharmacokinetic study [J] . Abdallah Ola M., Abdel-Megied Ahmed M., Gouda Amira S. Journal of Pharmaceutical and Biomedical Analysis: An International Journal on All Drug-Related Topics in Pharmaceutical, Biomedical and Clinical Analysis . 2017,第期

机译：开发验证的高敏感LC-MS / MS方法，用于同时定量LEDIPASVIR，SOFOSBUVIR及其主要代谢物GS-331007中的人血浆：应用于人类药代动力学研究
3. Sensitive assay for midazolam and its metabolite 1 '-hydroxymidazolam in human plasma by capillary high-performance liquid chromatography [J] . Eeckhoudt SL., Horsmans Y., De Winne AJ., Journal of Chromatography, Biomedical Applications . 1998,第1a2期

机译：毛细管高效液相色谱法测定人血浆中的咪达唑仑及其代谢物1'-羟基咪达唑仑
4. Development and validation of a sensitive LC-MS/MS method for analysis of midazolam and their metabolites in human plasma and urine [C] . Ganesh S. Moorthy, Praveen Srivastava, Vu T. Nguyen, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2013

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5. Stereoselective and nonstereoselective assay methods for metoprolol and its metabolites and their application to the evaluation of the influence of input rate on the metabolism and pharmacokinetics of metoprolol in humans. [D] . Mistry, Bipin M. 1999

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A highly sensitive LC-MS-MS assay for analysis of midazolam and its major metabolite in human plasma: Applications to drug metabolism

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