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A Clinical Drug‐Drug Interaction Study Assessing a Novel Drug Transporter Phenotyping Cocktail With Adefovir, Sitagliptin, Metformin, Pitavastatin, and Digoxin

A new probe drug cocktail containing substrates of important drug transporters was tested for mutual interactions in a clinical trial. The cocktail consisted of (predominant transporter; primary phenotyping metric): 10 mg adefovir‐dipivoxil (OAT1; renal clearance (CLR)), 100 mg sitagliptin (OAT3; CL...

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Published in:Clinical pharmacology and therapeutics 2019-12, Vol.106 (6), p.1398-1407
Main Authors: Trueck, Christina, Hsin, Chih‐hsuan, Scherf‐Clavel, Oliver, Schaeffeler, Elke, Lenssen, Rebekka, Gazzaz, Malaz, Gersie, Marleen, Taubert, Max, Quasdorff, Maria, Schwab, Matthias, Kinzig, Martina, Sörgel, Fritz, Stoffel, Marc S., Fuhr, Uwe
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cited_by cdi_FETCH-LOGICAL-c3214-a5868bd6b1dff3952becc8c0f252747c09e15c809f855499fb9c2d96129aedf3
cites cdi_FETCH-LOGICAL-c3214-a5868bd6b1dff3952becc8c0f252747c09e15c809f855499fb9c2d96129aedf3
container_end_page 1407
container_issue 6
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container_title Clinical pharmacology and therapeutics
container_volume 106
creator Trueck, Christina
Hsin, Chih‐hsuan
Scherf‐Clavel, Oliver
Schaeffeler, Elke
Lenssen, Rebekka
Gazzaz, Malaz
Gersie, Marleen
Taubert, Max
Quasdorff, Maria
Schwab, Matthias
Kinzig, Martina
Sörgel, Fritz
Stoffel, Marc S.
Fuhr, Uwe
description A new probe drug cocktail containing substrates of important drug transporters was tested for mutual interactions in a clinical trial. The cocktail consisted of (predominant transporter; primary phenotyping metric): 10 mg adefovir‐dipivoxil (OAT1; renal clearance (CLR)), 100 mg sitagliptin (OAT3; CLR), 500 mg metformin (several renal transporters; CLR), 2 mg pitavastatin (OATP1B1; clearance/F), and 0.5 mg digoxin (intestinal P‐gp, renal P‐gp, and OATP4C1; peak plasma concentration (Cmax) and CLR). Using a randomized six‐period, open change‐over design, single oral doses were administrated either concomitantly or separately to 24 healthy male and female volunteers. Phenotyping metrics were evaluated by noncompartmental analysis and compared between periods by the standard average bioequivalence approach (boundaries for ratios 0.80–1.25). Primary metrics supported the absence of relevant interactions, whereas secondary metrics suggested that mainly adefovir was a victim of minor drug‐drug interactions (DDIs). All drugs were well tolerated. This cocktail may be another useful tool to assess transporter‐based DDIs in vivo.
doi_str_mv 10.1002/cpt.1564
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title A Clinical Drug‐Drug Interaction Study Assessing a Novel Drug Transporter Phenotyping Cocktail With Adefovir, Sitagliptin, Metformin, Pitavastatin, and Digoxin
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