Clinical Pharmacokinetics of Daprodustat: Results of an Absorption, Distribution, and Excretion Study With Intravenous Microtracer and Concomitant Oral Doses for Bioavailability Determination

Clinical Pharmacokinetics of Daprodustat: Results of an Absorption, Distribution, and Excretion Study With Intravenous Microtracer and Concomitant Oral Doses for Bioavailability Determination

Daprodustat, an oral hypoxia‐inducible factor prolyl hydroxylase inhibitor, is being investigated for treatment of anemia in chronic kidney disease. This phase 1, nonrandomized, 2‐period, crossover study in 6 healthy men characterized the absorption, distribution, and excretion of daprodustat when a...

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Veröffentlicht in:Clinical pharmacology in drug development 2021-12, Vol.10 (12), p.1419-1431
Hauptverfasser: Mahar, Kelly M., Caltabiano, Stephen, Andrews, Susan, Ramanjineyulu, Bandi, Chen, Liangfu, Young, Graeme, Pereira, Adrian, Lindsay, Alistair C., van den Berg, Frans, Cobitz, Alexander R.
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anemia
Bioavailability
chronic kidney disease
daprodustat
hypoxia‐inducible factor
Life Sciences & Biomedicine
mass balance
Metabolites
Original
Pharmacokinetics
Pharmacology & Pharmacy
Science & Technology
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container_end_page 1431
container_issue 12
container_start_page 1419
container_title Clinical pharmacology in drug development
container_volume 10
creator Mahar, Kelly M.
Caltabiano, Stephen
Andrews, Susan
Ramanjineyulu, Bandi
Chen, Liangfu
Young, Graeme
Pereira, Adrian
Lindsay, Alistair C.
van den Berg, Frans
Cobitz, Alexander R.
description Daprodustat, an oral hypoxia‐inducible factor prolyl hydroxylase inhibitor, is being investigated for treatment of anemia in chronic kidney disease. This phase 1, nonrandomized, 2‐period, crossover study in 6 healthy men characterized the absorption, distribution, and excretion of daprodustat when administered as oral and intravenous (IV) doses of unlabeled and radiolabeled daprodustat ([14C]‐GSK1278863). Tolerability and pharmacokinetic properties of daprodustat, and its 6 metabolites in the systemic circulation, were also evaluated. The mean recovery of radiolabeled daprodustat was ≈95% by day 5, with the majority in feces and minor renal elimination, indicating that daprodustat and metabolites are primarily eliminated via hepatobiliary and fecal routes. Approximately 40% of total circulating radioactivity in plasma following both IV and oral administration was daprodustat; thus, 60% was attributed to metabolites. It was estimated that ≈80% of daprodustat was absorbed across the gastrointestinal tract, and ≈18% cleared by hepatic extraction. Pharmacokinetics were essentially dose proportional, with moderate (≈66%) oral tablet bioavailability. Following IV administration, daprodustat plasma clearance (19.3 L/h) and volume of distribution (14.6 L) were low, suggesting low tissue distribution outside systemic circulation with likely low penetration into tissues. Daprodustat was generally well tolerated, with no deaths or serious or significant adverse events reported.
doi_str_mv 10.1002/cpdd.1029
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source Wiley Online Library Journals Frontfile Complete
subjects anemia
Bioavailability
chronic kidney disease
daprodustat
hypoxia‐inducible factor
Life Sciences & Biomedicine
mass balance
Metabolites
Original
Pharmacokinetics
Pharmacology & Pharmacy
Science & Technology
title Clinical Pharmacokinetics of Daprodustat: Results of an Absorption, Distribution, and Excretion Study With Intravenous Microtracer and Concomitant Oral Doses for Bioavailability Determination
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