Validation and clinical application of dried blood spot assay for quantitative assessment of edoxaban in healthy adults

Dried blood spot (DBS) is a sampling approach that offers several advantages over plasma and whole blood (WB) sampling, but several factors, such as hematocrit and temperature, can adversely affect quantitation. In an open-label, three-way crossover study in healthy subjects, we explored the correla...

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Bibliographic Details
Published inBioanalysis Vol. 12; no. 6; pp. 393 - 407
Main Authors He, Ling, Gajee, Roohi, Mangaraj, Raj, Waldron, Michael P, Brown, Karen S
Format Journal Article
LanguageEnglish
Published England Newlands Press Ltd 01.03.2020
Informa UK Limited
Newlands Press
Subjects
Acids
Anticoagulants
bioanalytical method validation
Blood
Chromatography
Clinical medicine
concordance
Cross-Over Studies
dried blood spot
Dried Blood Spot Testing
Dried Blood Spot Testing - methods
edoxaban
Factor Xa Inhibitors
Factor Xa Inhibitors - pharmacology
Factor Xa Inhibitors - therapeutic use
finger prick
Healthy Volunteers
Hematocrit
Humans
incurred sample analysis
Ions
Medical screening
Metabolites
Pharmacokinetics
Plasma
Pyridines
Pyridines - pharmacology
Pyridines - therapeutic use
Quantitation
Reproducibility of Results
Sampling
Thiazoles
Thiazoles - pharmacology
Thiazoles - therapeutic use
United States > US
bioanalytical method validation
finger prick
dried blood spot
edoxaban
concordance
incurred sample analysis
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ISSN1757-6180
1757-6199
DOI10.4155/bio-2019-0180

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Summary:Dried blood spot (DBS) is a sampling approach that offers several advantages over plasma and whole blood (WB) sampling, but several factors, such as hematocrit and temperature, can adversely affect quantitation. In an open-label, three-way crossover study in healthy subjects, we explored the correlation between DBS, WB and plasma samples, and between DBS samples from finger-prick and venipuncture blood for measuring edoxaban and its metabolite M-4 using LC–MS/MS. The methods were validated comprehensively. The incurred sample reanalysis experiments demonstrated quantitation reproducibility in all three matrices. Overall, there was a good correlation (near perfect concordance for edoxaban) among plasma, WB and DBS measurements. M-4 concentrations in DBS and WB were lower than in plasma. These results indicate using DBS may be used as an alternative methodology to measure edoxaban pharmacokinetics.
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ISSN:1757-6180
1757-6199
DOI:10.4155/bio-2019-0180