From “wet” matrices to “dry” blood spot sampling strategy: a versatile LC-MS/MS assay for simultaneous monitoring caffeine and its three primary metabolites in preterm infants
Author:
Dai Hao-Ran12ORCID, Guo Hong-Li1, Wang Wei-Jun12, Shen Xian3, Cheng Rui3, Xu Jing1, Hu Ya-Hui1, Ding Xuan-Sheng2, Chen Feng1ORCID
Affiliation:
1. Pharmaceutical Sciences Research Center , Department of Pharmacy , Children’s Hospital of Nanjing Medical University , Nanjing , P.R. China 2. School of Basic Medicine and Clinical Pharmacy , China Pharmaceutical University , Nanjing , P.R. China 3. Neonatal Intensive Care Unit , Children’s Hospital of Nanjing Medical University , Nanjing , P.R. China
Abstract
Abstract
Objectives
To update traditional “wet” matrices to dried blood spot (DBS) sampling, based on the liquid chromatography coupled with tandem mass spectrometry (LC-MS/MS) technique, and develop a method for simultaneous analyzing caffeine and its three primary metabolites (theobromine, paraxanthine, and theophylline), supporting routine therapeutic drug monitoring (TDM) for preterm infants.
Methods
DBS samples were prepared by a two-step quantitative sampling method, i.e., volumetric sampling of a quantitative 10 μL volume of peripheral blood and an 8 mm diameter whole punch extraction by a methanol/water (80/20, v/v) mixture containing 125 mM formic acid. Four paired stable isotope labeled internal standards and a collision energy defect strategy were applied for the method optimization. The method was fully validated following international guidelines and industrial recommendations on DBS analysis. Cross validation with previously developed plasma method was also proceeded. The validated method was then implemented on the TDM for preterm infants.
Results
The two-step quantitative sampling strategy and a high recovery extraction method were developed and optimized. The method validation results were all within the acceptable criteria. Satisfactory parallelism, concordance, and correlation were observed between DBS and plasma concentrations of the four analytes. The method was applied to provide routine TDM services to 20 preterm infants.
Conclusions
A versatile LC-MS/MS platform for simultaneous monitoring caffeine and its three primary metabolites was developed, fully validated, and successfully applied into the routine clinical TDM practices. Sampling method switching from “wet” matrices to “dry” DBS will facilitate and support the precision dosing of caffeine for preterm infants.
Funder
Specially Appointed Medical Expert Project of the Jiangsu Commission of Health Scientific Research Support Foundation for Top Young Scholars at the Children’s Hospital of Nanjing Medical University Special Fund for Clinical Research of the Wu Jieping Medical Foundation
Publisher
Walter de Gruyter GmbH
Subject
Biochemistry (medical),Clinical Biochemistry,General Medicine
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