Development and Validation of a Sensitive Liquid Chromatography-Tandem Mass Spectrometry Method for Therapeutic Drug Monitoring of Ceftolozane and Tazobactam in Human Plasma Microsamples.

IF 2.8 4区医学 Q2 MEDICAL LABORATORY TECHNOLOGY

Therapeutic Drug Monitoring Pub Date : 2024-08-06 DOI:10.1097/FTD.0000000000001236

Matteo Conti, Beatrice Giorgi, Milo Gatti, Pierluigi Viale, Federico Pea

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引用次数: 0

Abstract

Background: Ceftolozane/tazobactam (C-T) is a novel beta-lactam/beta-lactamase inhibitor combination approved for the treatment of various infections caused by difficult-to-treat Pseudomonas aeruginosa. In critically ill patients, C-T may exhibit significant pharmacokinetic variability, both between individuals and within individuals, warranting therapeutic drug monitoring for clinical purposes. We aim to develop and validate a novel and sensitive analytical method for concurrently determining C and T in human plasma microsamples (3 μL).

Methods: The method was developed using liquid chromatography-tandem mass spectrometry (LC-MS/MS) with positive electrospray ionization and multiple reaction monitoring (MRM) detection modes, employing specific mass transitions for both drugs. Sample preparation was simple, and the chromatographic run lasted only 4 minutes. Validation was conducted according to European Medicines Agency (EMA) guidelines, encompassing specificity, sensitivity, linearity, precision, accuracy, matrix effect, extraction recovery, limit of quantification, and drug stability. The validated method was applied to measure C and T in 32 plasma samples collected from critically ill patients with multidrug-resistant, gram-negative, bacterial infections.

Results: The method ensured accurate (BIAS% 2.1-9.6 for C and -2.2 to 15.2 for T) and precise intraday CV% for C: 6.7-5.5; for T: 1.3-8.9; interday CV% for C 6.0-10.8; for T 4.1-10.2) measurements of C-T over a wide concentration range (0.2-200.0 mg/L for C and 0.1-100.0 mg/L for T). Overall, the recovery at quality control concentration levels was high for both C and T (mean values: 90-91 for C and 89-92 for T). Analyte stability was satisfactory in both human plasma and extracts under various storage conditions. The clinical applicability of the assay was confirmed by the reliably quantifying C and T in clinical plasma samples.

Conclusions: The developed and validated LC-MS/MS method is sensitive and suitable for monitoring C and T in human plasma microsamples.

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开发并验证用于人体血浆微量样本中头孢妥仑和他唑巴坦治疗药物监测的灵敏液相色谱-串联质谱法

背景：头孢唑烷/他唑巴坦（C-T）是一种新型β-内酰胺/β-内酰胺酶抑制剂复方制剂，已被批准用于治疗难以治疗的铜绿假单胞菌引起的各种感染。在重症患者中，C-T 在个体之间和个体内部都可能表现出显著的药代动力学变异，因此需要进行临床治疗药物监测。我们旨在开发并验证一种新颖灵敏的分析方法，用于同时测定人体血浆微量样本（3 μL）中的 C 和 T：该方法采用液相色谱-串联质谱法（LC-MS/MS），采用正电离和多反应监测（MRM）检测模式，利用两种药物的特定质量跃迁。样品制备简单，色谱运行仅需 4 分钟。根据欧洲药品管理局（EMA）的指导方针进行了验证，包括特异性、灵敏度、线性、精密度、准确度、基质效应、提取回收率、定量限和药物稳定性。验证后的方法被用于检测 32 份血浆样本中的 C 和 T，这些样本来自多重耐药革兰氏阴性细菌感染的重症患者：结果：该方法确保了准确性（C 的 BIAS% 为 2.1-9.6，T 为 -2.2-15.2 ）和精确性，C 的日内 CV% 为 6.7-5.5，T 为 1.3-8.9：在较宽的浓度范围（C 为 0.2-200.0 毫克/升，T 为 0.1-100.0 毫克/升）内，对 C-T 进行了精确测量（C 的日内 CV%为 6.7-5.5，T 的日内 CV%为 1.3-8.9，C 的日间 CV%为 6.0-10.8，T 的日间 CV%为 4.1-10.2）。总体而言，C 和 T 在质控浓度水平下的回收率都很高（平均值：C 为 90-91，T 为 89-92）。在各种储存条件下，人血浆和提取物中分析物的稳定性均令人满意。临床血浆样本中 C 和 T 的可靠定量证实了该检测方法的临床适用性：结论：所开发和验证的 LC-MS/MS 方法灵敏度高，适用于监测人体血浆微量样本中的 C 和 T。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Therapeutic Drug Monitoring 医学-毒理学

CiteScore

5.00

自引率

8.00%

发文量

213

审稿时长

4-8 weeks

期刊介绍： Therapeutic Drug Monitoring is a peer-reviewed, multidisciplinary journal directed to an audience of pharmacologists, clinical chemists, laboratorians, pharmacists, drug researchers and toxicologists. It fosters the exchange of knowledge among the various disciplines–clinical pharmacology, pathology, toxicology, analytical chemistry–that share a common interest in Therapeutic Drug Monitoring. The journal presents studies detailing the various factors that affect the rate and extent drugs are absorbed, metabolized, and excreted. Regular features include review articles on specific classes of drugs, original articles, case reports, technical notes, and continuing education articles.

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