UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study

MK-7246, an antagonist of the chemoattractant receptor on T helper type 2 (Th2) cells, is being developed for the treatment of respiratory diseases. In a first-in-human study, we investigated whether genetic polymorphisms contributed to the marked intersubject variability in the pharmacokinetics of...

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Autores principales: Wang, Y-H, Trucksis, M, McElwee, J J, Wong, P H, Maciolek, C, Thompson, C D, Prueksaritanont, T, Garrett, G C, Declercq, R, Vets, E, Willson, K J, Smith, R C, Klappenbach, J A, Opiteck, G J, Tsou, J A, Gibson, C, Laethem, T, Panorchan, P, Iwamoto, M, Shaw, P M, Wagner, J A, Harrelson, J C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2012
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3380185/
https://www.ncbi.nlm.nih.gov/pubmed/22669291
http://dx.doi.org/10.1038/clpt.2012.20
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author Wang, Y-H
Trucksis, M
McElwee, J J
Wong, P H
Maciolek, C
Thompson, C D
Prueksaritanont, T
Garrett, G C
Declercq, R
Vets, E
Willson, K J
Smith, R C
Klappenbach, J A
Opiteck, G J
Tsou, J A
Gibson, C
Laethem, T
Panorchan, P
Iwamoto, M
Shaw, P M
Wagner, J A
Harrelson, J C
author_facet Wang, Y-H
Trucksis, M
McElwee, J J
Wong, P H
Maciolek, C
Thompson, C D
Prueksaritanont, T
Garrett, G C
Declercq, R
Vets, E
Willson, K J
Smith, R C
Klappenbach, J A
Opiteck, G J
Tsou, J A
Gibson, C
Laethem, T
Panorchan, P
Iwamoto, M
Shaw, P M
Wagner, J A
Harrelson, J C
author_sort Wang, Y-H
collection PubMed
description MK-7246, an antagonist of the chemoattractant receptor on T helper type 2 (Th2) cells, is being developed for the treatment of respiratory diseases. In a first-in-human study, we investigated whether genetic polymorphisms contributed to the marked intersubject variability in the pharmacokinetics of MK-7246 and its glucuronide metabolite M3. Results from in vitro enzyme kinetic studies suggested that UGT2B17 is probably the major enzyme responsible for MK-7246 metabolism in both the liver and the intestine. As compared with those with the UGT2B17*1/*1 wild-type genotype, UGT2B17*2/*2 carriers, who possess no UGT2B17 protein, had 25- and 82-fold greater mean dose-normalized values of area under the plasma concentration–time curve (AUC) and peak concentration of MK-7246, respectively, and a 24-fold lower M3-to-MK-7246 AUC ratio. The apparent half-life of MK-7246 was not as variable between these two genotypes. Therefore, the highly variable pharmacokinetics of MK-7246 is attributable primarily to the impact of UGT2B17 genetic polymorphisms and extensive first-pass metabolism of MK-7246.
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spelling pubmed-33801852012-06-21 UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study Wang, Y-H Trucksis, M McElwee, J J Wong, P H Maciolek, C Thompson, C D Prueksaritanont, T Garrett, G C Declercq, R Vets, E Willson, K J Smith, R C Klappenbach, J A Opiteck, G J Tsou, J A Gibson, C Laethem, T Panorchan, P Iwamoto, M Shaw, P M Wagner, J A Harrelson, J C Clin Pharmacol Ther Articles MK-7246, an antagonist of the chemoattractant receptor on T helper type 2 (Th2) cells, is being developed for the treatment of respiratory diseases. In a first-in-human study, we investigated whether genetic polymorphisms contributed to the marked intersubject variability in the pharmacokinetics of MK-7246 and its glucuronide metabolite M3. Results from in vitro enzyme kinetic studies suggested that UGT2B17 is probably the major enzyme responsible for MK-7246 metabolism in both the liver and the intestine. As compared with those with the UGT2B17*1/*1 wild-type genotype, UGT2B17*2/*2 carriers, who possess no UGT2B17 protein, had 25- and 82-fold greater mean dose-normalized values of area under the plasma concentration–time curve (AUC) and peak concentration of MK-7246, respectively, and a 24-fold lower M3-to-MK-7246 AUC ratio. The apparent half-life of MK-7246 was not as variable between these two genotypes. Therefore, the highly variable pharmacokinetics of MK-7246 is attributable primarily to the impact of UGT2B17 genetic polymorphisms and extensive first-pass metabolism of MK-7246. Nature Publishing Group 2012-07 2012-06-06 /pmc/articles/PMC3380185/ /pubmed/22669291 http://dx.doi.org/10.1038/clpt.2012.20 Text en Copyright © 2012 American Society of Clinical Pharmacology and Therapeutics http://creativecommons.org/licenses/by-nc-nd/3.0/ This work is licensed under the Creative Commons Attribution-NonCommercial-No Derivative Works 3.0 Unported License. To view a copy of this license, visit http://creativecommons.org/licenses/by-nc-nd/3.0/
spellingShingle Articles
Wang, Y-H
Trucksis, M
McElwee, J J
Wong, P H
Maciolek, C
Thompson, C D
Prueksaritanont, T
Garrett, G C
Declercq, R
Vets, E
Willson, K J
Smith, R C
Klappenbach, J A
Opiteck, G J
Tsou, J A
Gibson, C
Laethem, T
Panorchan, P
Iwamoto, M
Shaw, P M
Wagner, J A
Harrelson, J C
UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study
title UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study
title_full UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study
title_fullStr UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study
title_full_unstemmed UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study
title_short UGT2B17 Genetic Polymorphisms Dramatically Affect the Pharmacokinetics of MK-7246 in Healthy Subjects in a First-in-Human Study
title_sort ugt2b17 genetic polymorphisms dramatically affect the pharmacokinetics of mk-7246 in healthy subjects in a first-in-human study
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3380185/
https://www.ncbi.nlm.nih.gov/pubmed/22669291
http://dx.doi.org/10.1038/clpt.2012.20
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