Kuhlin Johanna, Sturkenboom Marieke G G, Ghimire Samiksha, Margineanu Ioana, van den Elsen Simone H J, Simbar Noviana, Akkerman Onno W, Jongedijk Erwin M, Koster Remco A, Bruchfeld Judith, Touw Daan J, Alffenaar Jan-Willem C
Unit of Infectious Diseases, Department of Medicine Solna, Karolinska Institutet, Stockholm, Sweden.
Department of Infectious Diseases, Karolinska University Hospital, Stockholm, Sweden.
Clin Mass Spectrom. 2018 Oct 19;14 Pt A:34-45. doi: 10.1016/j.clinms.2018.10.002. eCollection 2019 Sep.
Therapeutic drug monitoring (TDM) uses drug concentrations, primarily from plasma, to optimize drug dosing. Optimisation of drug dosing may improve treatment outcomes, reduce toxicity and reduce the risk of acquired drug resistance. The aim of this narrative review is to outline and discuss the challenges of developing multi-analyte assays for anti-tuberculosis (TB) drugs using liquid chromatography-tandem mass spectrometry (LC-MS/MS) by reviewing the existing literature in the field. Compared to other analytical methods, LC-MS/MS offers higher sensitivity and selectivity while requiring relatively low sample volumes. Additionally, multi-analyte assays are easier to perform since adequate separation and short run times are possible even when non-selective sample preparation techniques are used. However, challenges still exist, especially when optimizing LC separation techniques for assays that include analytes with differing chemical properties. Here, we have identified seven multi-analyte assays for first-line anti-TB drugs that use various solvents for sample preparation and mobile phase separation. Only two multi-analyte assays for second-line anti-TB drugs were identified (including either nine or 20 analytes), with each using different protein precipitation methods, mobile phases and columns. The 20 analyte assay did not include bedaquiline, delamanid, meropenem or imipenem. For these drugs, other assays with similar methodologies were identified that could be incorporated in the development of a future comprehensive multi-analyte assay. TDM is a powerful methodology for monitoring patient's individual treatments in TB programmes, but its implementation will require different approaches depending on available resources. Since TB is most-prevalent in low- and middle-income countries where resources are scarce, a patient-centred approach using sampling methods other than large volume blood draws, such as dried blood spots or saliva collection, could facilitate its adoption and use. Regardless of the methodology of collection and analysis, it will be critical that laboratory proficiency programmes are in place to ensure adequate quality control. It is our intent that the information contained in this review will contribute to the process of assembling comprehensive multiplexed assays for the dynamic monitoring of anti-TB drug treatment in affected individuals.
治疗药物监测(TDM)利用主要来自血浆的药物浓度来优化给药剂量。优化给药剂量可改善治疗效果、降低毒性并降低获得性耐药风险。本叙述性综述的目的是通过回顾该领域的现有文献,概述并讨论使用液相色谱 - 串联质谱(LC-MS/MS)开发抗结核(TB)药物多分析物检测方法所面临的挑战。与其他分析方法相比,LC-MS/MS具有更高的灵敏度和选择性,同时所需样品体积相对较小。此外,即使使用非选择性样品制备技术,多分析物检测也更易于执行,因为可以实现充分分离且运行时间较短。然而,挑战依然存在,尤其是在为包含具有不同化学性质分析物的检测优化LC分离技术时。在此,我们确定了七种用于一线抗结核药物的多分析物检测方法,这些方法使用各种溶剂进行样品制备和流动相分离。仅确定了两种用于二线抗结核药物的多分析物检测方法(包括九种或二十种分析物),每种方法使用不同的蛋白质沉淀方法、流动相和色谱柱。二十种分析物的检测方法未包括贝达喹啉、地拉曼尼、美罗培南或亚胺培南。对于这些药物,确定了其他具有相似方法的检测方法,可纳入未来全面多分析物检测方法的开发中。TDM是监测结核病项目中患者个体治疗的有力方法,但其实施将需要根据可用资源采用不同方法。由于结核病在资源稀缺的低收入和中等收入国家最为普遍,采用以患者为中心的方法,使用除大量采血以外的采样方法,如干血斑或唾液采集,可能有助于其采用和使用。无论采集和分析方法如何,至关重要的是要有实验室能力验证计划以确保充分的质量控制。我们希望本综述中包含的信息将有助于组装用于动态监测受影响个体抗结核药物治疗的全面多重检测方法的过程。
