A quantitative method for the analysis of total and unbound concentrations of amoxicillin, ampicillin, ceftazidime, ceftriaxone, ertapenem, fosfomycin and penicillin G in human plasma with liquid chromatography–tandem mass spectrometry assay

IF 1.8 4区 医学 Q4 BIOCHEMICAL RESEARCH METHODS
Marlotte A. A. van der Veer, Marloes van der Meer-Vos, Timo R. de Haan, Linda G. W. Franken, Yuma. A. Bijleveld, Ron A. A. Mathôt
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引用次数: 0

Abstract

Monitoring antibiotic plasma levels is critical in populations with altered pharmacokinetics, such as critically ill patients in neonatal or adult intensive care units. This study aimed to develop and validate a rapid, reproducible and sensitive liquid chromatography–tandem mass spectrometry assay (LC–MS/MS) for measuring total and unbound concentrations of amoxicillin, ampicillin, ceftazidime, ceftriaxone, ertapenem, fosfomycin and penicillin G in human plasma. The method required 20 and 250 μl sample volumes for measuring total and unbound concentrations, respectively. Sample preparation involved protein precipitation and the addition of an internal standard. Ultrafiltration separated unbound drugs. Method validation covered selectivity, carryover, linearity, accuracy, precision, dilution effects, matrix effects and stability. The LC–MS/MS was performed within a run time of 7.5 min. Calibration curves were linear for ceftazidime and ertapenem (ranges 0.1–50 and 0.05–100 mg/l, respectively) and quadratic for other analytes (0.1–50 mg/l, except for ampicillin: 0.1–20 mg/l; R2 > 0.990). Accuracy was within ±15% of the nominal concentration, and precision did not exceed ±15% (relative standard deviation). Samples showed no significant degradation at the tested temperatures and time points. Clinical applicability was demonstrated in a critically ill neonate. This method with minimal sample volume and short analysis time enables the measurement of total and unbound concentrations of selected antibiotics, and is suitable for routine clinical care and studies.

Abstract Image

利用液相色谱-串联质谱法定量分析人体血浆中阿莫西林、氨苄西林、头孢他啶、头孢曲松、厄他培南、磷霉素和青霉素 G 的总浓度和未结合浓度。
对于药代动力学发生改变的人群,如新生儿或成人重症监护室的重症患者,监测抗生素血浆水平至关重要。本研究旨在开发并验证一种快速、可重复、灵敏的液相色谱-串联质谱测定法(LC-MS/MS),用于测量人血浆中阿莫西林、氨苄西林、头孢他啶、头孢曲松、厄他培南、磷霉素和青霉素 G 的总浓度和未结合浓度。该方法测量总浓度和未结合浓度分别需要 20 和 250 μl 样品体积。样品制备包括蛋白质沉淀和添加内标。超滤分离未结合的药物。方法验证包括选择性、携带、线性、准确性、精密度、稀释效应、基质效应和稳定性。LC-MS/MS 的运行时间为 7.5 分钟。头孢他啶和厄他培南的校准曲线呈线性(范围分别为 0.1-50 毫克/升和 0.05-100 毫克/升),其他分析物的校准曲线呈二次曲线(0.1-50 毫克/升,氨苄西林除外:0.1-20 毫克/升;R2 > 0.990)。准确度在标称浓度的 ±15% 以内,精密度不超过 ±15%(相对标准偏差)。在测试温度和时间点上,样品没有出现明显降解。临床适用性已在一名重症新生儿身上得到证实。该方法样品量少、分析时间短,可测量选定抗生素的总浓度和未结合浓度,适用于常规临床护理和研究。
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来源期刊
Biomedical Chromatography
Biomedical Chromatography 生物-分析化学
CiteScore
3.60
自引率
5.60%
发文量
268
审稿时长
2.3 months
期刊介绍: Biomedical Chromatography is devoted to the publication of original papers on the applications of chromatography and allied techniques in the biological and medical sciences. Research papers and review articles cover the methods and techniques relevant to the separation, identification and determination of substances in biochemistry, biotechnology, molecular biology, cell biology, clinical chemistry, pharmacology and related disciplines. These include the analysis of body fluids, cells and tissues, purification of biologically important compounds, pharmaco-kinetics and sequencing methods using HPLC, GC, HPLC-MS, TLC, paper chromatography, affinity chromatography, gel filtration, electrophoresis and related techniques.
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