Liquid microjunction surface sampling of acetaminophen, terfenadine and their metabolites in thin tissue sections

Vilmos Kertesz; Nithya Paranthaman; Paul Moench; Alexandre Catoire; Jimmy Flarakos; Gary J. Van Berkel

doi:10.4155/bio.14.130

Liquid microjunction surface sampling of acetaminophen, terfenadine and their metabolites in thin tissue sections

Vilmos Kertesz
, Nithya Paranthaman
, Paul Moench
, Alexandre Catoire
, Jimmy Flarakos
, Gary J. Van Berkel

Bioanalytical Mass Spectrometry

Research output: Contribution to journal › Article › peer-review

16 Scopus citations

Abstract

Background: The aim of this work was to evaluate the analytical performance of a fully automated droplet-based surface-sampling system for determining the distribution of the drugs acetaminophen and terfenadine, and their metabolites, in rat thin tissue sections. Results: The rank order of acetaminophen concentration observed in tissues was stomach > small intestine > liver, while the concentrations of its glucuronide and sulfate metabolites were greatest in the liver and small intestine. Terfenadine was most concentrated in the liver and kidney, while its major metabolite, fexofenadine, was found in the liver and small intestine. Conclusion: The spatial distributions of both drugs and their respective metabolites observed in this work were consistent with previous studies using radiolabeled drugs.

Original language	English
Pages (from-to)	2599-2606
Number of pages	8
Journal	Bioanalysis
Volume	6
Issue number	19
DOIs	https://doi.org/10.4155/bio.14.130
State	Published - Oct 1 2014

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abstract = "Background: The aim of this work was to evaluate the analytical performance of a fully automated droplet-based surface-sampling system for determining the distribution of the drugs acetaminophen and terfenadine, and their metabolites, in rat thin tissue sections. Results: The rank order of acetaminophen concentration observed in tissues was stomach > small intestine > liver, while the concentrations of its glucuronide and sulfate metabolites were greatest in the liver and small intestine. Terfenadine was most concentrated in the liver and kidney, while its major metabolite, fexofenadine, was found in the liver and small intestine. Conclusion: The spatial distributions of both drugs and their respective metabolites observed in this work were consistent with previous studies using radiolabeled drugs.",

author = "Vilmos Kertesz and Nithya Paranthaman and Paul Moench and Alexandre Catoire and Jimmy Flarakos and \{Van Berkel\}, \{Gary J.\}",

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T1 - Liquid microjunction surface sampling of acetaminophen, terfenadine and their metabolites in thin tissue sections

AU - Kertesz, Vilmos

AU - Paranthaman, Nithya

AU - Moench, Paul

AU - Catoire, Alexandre

AU - Flarakos, Jimmy

AU - Van Berkel, Gary J.

PY - 2014/10/1

Y1 - 2014/10/1

N2 - Background: The aim of this work was to evaluate the analytical performance of a fully automated droplet-based surface-sampling system for determining the distribution of the drugs acetaminophen and terfenadine, and their metabolites, in rat thin tissue sections. Results: The rank order of acetaminophen concentration observed in tissues was stomach > small intestine > liver, while the concentrations of its glucuronide and sulfate metabolites were greatest in the liver and small intestine. Terfenadine was most concentrated in the liver and kidney, while its major metabolite, fexofenadine, was found in the liver and small intestine. Conclusion: The spatial distributions of both drugs and their respective metabolites observed in this work were consistent with previous studies using radiolabeled drugs.

AB - Background: The aim of this work was to evaluate the analytical performance of a fully automated droplet-based surface-sampling system for determining the distribution of the drugs acetaminophen and terfenadine, and their metabolites, in rat thin tissue sections. Results: The rank order of acetaminophen concentration observed in tissues was stomach > small intestine > liver, while the concentrations of its glucuronide and sulfate metabolites were greatest in the liver and small intestine. Terfenadine was most concentrated in the liver and kidney, while its major metabolite, fexofenadine, was found in the liver and small intestine. Conclusion: The spatial distributions of both drugs and their respective metabolites observed in this work were consistent with previous studies using radiolabeled drugs.

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Liquid microjunction surface sampling of acetaminophen, terfenadine and their metabolites in thin tissue sections

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