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image/svg+xml Jakob Voss, based on art designer at PLoS, modified by Wikipedia users Nina and Beao Closed Access logo, derived from PLoS Open Access logo. This version with transparent background. http://commons.wikimedia.org/wiki/File:Closed_Access_logo_transparent.svg Jakob Voss, based on art designer at PLoS, modified by Wikipedia users Nina and Beao Clinical Pharmacolog...arrow_drop_down
image/svg+xml Jakob Voss, based on art designer at PLoS, modified by Wikipedia users Nina and Beao Closed Access logo, derived from PLoS Open Access logo. This version with transparent background. http://commons.wikimedia.org/wiki/File:Closed_Access_logo_transparent.svg Jakob Voss, based on art designer at PLoS, modified by Wikipedia users Nina and Beao
Clinical Pharmacology in Drug Development
Article . 2014 . Peer-reviewed
License: Wiley Online Library User Agreement
Data sources: Crossref
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Vorapaxar, an oral PAR‐1 receptor antagonist, does not affect the pharmacokinetics of rosiglitazone

Authors: Teddy, Kosoglou; Bharath, Kumar; Paul, Statkevich; James E, Schiller; Bhavna, Kantesaria; Mary E, Hanson; Christine McCrary, Sisk; +1 Authors

Vorapaxar, an oral PAR‐1 receptor antagonist, does not affect the pharmacokinetics of rosiglitazone

Abstract

AbstractPurposeTo evaluate the potential effects of vorapaxar on the pharmacokinetics and safety of rosiglitazone.MethodsThis was an open‐label, two‐period, two‐treatment, fixed‐sequence study in 18 healthy subjects. On Day 1, Period 1, subjects received a single dose of rosiglitazone 8 mg. In Period 2, subjects received vorapaxar 40 mg on Day 1, vorapaxar 7.5 mg once‐daily on Days 2–7, and a single dose of rosiglitazone 8 mg on Day 7. Rosiglitazone and N‐desmethylrosiglitazone pharmacokinetics were assessed alone (Period 1) and after coadministration with vorapaxar (Period 2). Vorapaxar and its M20 metabolite pharmacokinetics were assessed on Day 7, Period 2. Safety and tolerability were assessed throughout the study.ResultsCoadministration of rosiglitazone with vorapaxar had no effect on rosiglitazone or N‐desmethylrosiglitazone pharmacokinetics. The ratio of geometric means (GMR) and 90% confidence intervals (CI) of the coadministration versus monotherapy for Cmax (GMR 95; 90% CI 88, 103) and AUC0–24 h (GMR 103; 90% CI 98, 108) were within the 80–125% bioequivalence criteria. The metabolite‐to‐parent exposure ratio with and without vorapaxar was unaltered. Coadministration of vorapaxar with rosiglitazone was generally well tolerated.ConclusionCoadministration of vorapaxar with rosiglitazone or drugs metabolized via CYP2C8 is unlikely to cause a significant pharmacokinetic interaction.

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Keywords

Adult, Male, Adolescent, Metabolic Clearance Rate, Pyridines, Middle Aged, Healthy Volunteers, Cytochrome P-450 CYP2C8, Lactones, Cytochrome P-450 CYP2C8 Inhibitors, Area Under Curve, North Dakota, Humans, Hypoglycemic Agents, Drug Interactions, Female, Receptor, PAR-1, Biotransformation, Platelet Aggregation Inhibitors, Half-Life

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selected citations
These citations are derived from selected sources.
This is an alternative to the "Influence" indicator, which also reflects the overall/total impact of an article in the research community at large, based on the underlying citation network (diachronically).
BIP!Citations provided by BIP!
popularity
This indicator reflects the "current" impact/attention (the "hype") of an article in the research community at large, based on the underlying citation network.
BIP!Popularity provided by BIP!
influence
This indicator reflects the overall/total impact of an article in the research community at large, based on the underlying citation network (diachronically).
BIP!Influence provided by BIP!
impulse
This indicator reflects the initial momentum of an article directly after its publication, based on the underlying citation network.
BIP!Impulse provided by BIP!
1
Average
Average
Average
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