Mass spectrometry quantitation of immunosuppressive drugs in clinical specimens using online solid-phase extraction and accurate-mass full scan-single ion monitoring

IF 3.1 4区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY Journal of Mass Spectrometry and Advances in the Clinical Lab Pub Date : 2023-04-01 DOI:10.1016/j.jmsacl.2023.03.002
Priscilla S.-W. Yeung , Paige Miller , Tran Bao Lai-Nyugen , Phil Cheng , Amira Ibrahim , Run-Zhang Shi , Raffick A.R. Bowen , Ruben Yiqi Luo
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引用次数: 1

Abstract

Introduction

Therapeutic drug monitoring (TDM) of immunosuppressants is essential for optimal care of transplant patients. Immunoassays and liquid chromatography-mass spectrometry (LC-MS) are the most commonly used methods for TDM. However, immunoassays can suffer from interference from heterophile antibodies and structurally similar drugs and metabolites. Additionally, nominal-mass LC-MS assays can be difficult to optimize and are limited in the number of detectable compounds.

Objectives

The aim of this study was to implement a mass spectrometry-based test for immunosuppressant TDM using online solid-phase extraction (SPE) and accurate-mass full scan-single ion monitoring (FS-SIM) data acquisition mode.

Methods

LC-MS analysis was performed on a TLX-2 multi-channel HPLC with a Q-Exactive Plus mass spectrometer. TurboFlow online SPE was used for sample clean up. The accurate-mass MS was set to positive electrospray ionization mode with FS-SIM for quantitation of tacrolimus, sirolimus, everolimus, and cyclosporine A. MS2 fragmentation pattern was used for compound confirmation.

Results

The method was validated in terms of precision, analytical bias, limit of quantitation, linearity, carryover, sample stability, and interference. Quantitation of tacrolimus, sirolimus, everolimus, and cyclosporine A correlated well with results from an independent reference laboratory (r = 0.926–0.984).

Conclusions

Accurate-mass FS-SIM can be successfully utilized for immunosuppressant TDM with good correlation with results generated by standard methods. TurboFlow online SPE allows for a simple “protein crash and shoot” sample preparation protocol. Compared to traditional MRM, analyte quantitation by FS-SIM facilitates a streamlined assay optimization process.

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使用在线固相萃取和精确全扫描-单离子监测的临床标本免疫抑制药物质谱定量
引言免疫抑制剂的治疗药物监测(TDM)对于移植患者的最佳护理至关重要。免疫分析和液相色谱-质谱(LC-MS)是TDM最常用的方法。然而,免疫测定可能会受到嗜异抗体以及结构相似的药物和代谢产物的干扰。此外,标称质量LC-MS测定可能难以优化,并且可检测化合物的数量有限。目的本研究的目的是使用在线固相萃取(SPE)和精确的质谱全扫描单离子监测(FS-SIM)数据采集模式,对免疫抑制剂TDM进行基于质谱的检测。方法采用Q-Exactive Plus质谱仪在TLX-2多通道高效液相色谱上进行LC-MS分析。TurboFlow在线SPE用于样品清理。使用FS-SIM将精确质量MS设置为正电喷雾电离模式,用于他克莫司、西罗莫司、依维莫司和环孢菌素A的定量。MS2片段模式用于化合物确认。结果该方法在精密度、分析偏差、定量限、线性、携带量、样品稳定性和干扰等方面得到了验证。他克莫司、西罗莫司、依维莫司和环孢菌素A的定量与独立参考实验室的结果良好相关(r=0.926-0.984)。结论准确质量FS-SIM可成功用于免疫抑制剂TDM,与标准方法产生的结果良好相关性。TurboFlow在线SPE允许一个简单的“蛋白质碰撞和射击”样品制备协议。与传统的MRM相比,FS-SIM的分析物定量有助于简化分析优化过程。
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来源期刊
Journal of Mass Spectrometry and Advances in the Clinical Lab
Journal of Mass Spectrometry and Advances in the Clinical Lab Health Professions-Medical Laboratory Technology
CiteScore
4.30
自引率
18.20%
发文量
41
审稿时长
81 days
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