Evaluation of the Potential for Drug Interactions With Patiromer in Healthy Volunteers

Lawrence J Lesko; Elliot Offman; Christine Taylor Brew; Dahlia Garza; Wade Benton; Martha R Mayo; Alain Romero; Charles Du Mond; Matthew R Weir

doi:10.1177/1074248417691135

Evaluation of the Potential for Drug Interactions With Patiromer in Healthy Volunteers

J Cardiovasc Pharmacol Ther. 2017 Sep;22(5):434-446. doi: 10.1177/1074248417691135. Epub 2017 Feb 13.

Authors

Lawrence J Lesko¹, Elliot Offman², Christine Taylor Brew³, Dahlia Garza⁴, Wade Benton⁵, Martha R Mayo⁴, Alain Romero⁶, Charles Du Mond⁷, Matthew R Weir⁸

Affiliations

¹ 1 Center for Pharmacometrics and Systems Pharmacology, University of Florida College of Pharmacy, Orlando, FL, USA.
² 2 Clinical Pharmacology and Pharmacometrics, Celerion, Montreal, Quebec, Canada.
³ 3 Research Biology, Relypsa, Inc, Redwood City, CA, USA.
⁴ 4 Clinical Development, Relypsa, Inc, Redwood City, CA, USA.
⁵ 5 Consultant, Relypsa, Inc, Redwood City, CA, USA.
⁶ 6 Medical and Scientific Affairs, Relypsa, Inc, Redwood City, CA, USA.
⁷ 7 Biometrics, Relypsa, Inc, Redwood City, CA, USA.
⁸ 8 Division of Nephrology, Department of Medicine, University of Maryland School of Medicine, Baltimore, MD, USA.

Abstract

Introduction: Patiromer is a potassium-binding polymer that is not systemically absorbed; however, it may bind coadministered oral drugs in the gastrointestinal tract, potentially reducing their absorption.

Methods: Twelve randomized, open-label, 3-period, 3-sequence crossover studies were conducted in healthy volunteers to evaluate the effect of patiromer (perpetrator drug) on absorption and single-dose pharmacokinetics (PK) of drugs (victims) that might be commonly used with patiromer. Subjects received victim drug alone, victim drug administered together with patiromer 25.2 g (highest approved dose), and victim drug administered 3 hours before patiromer 25.2 g. The primary PK endpoints were area under the curve (AUC), extrapolated to infinity (AUC_0-∞), and maximum concentration ( C_max). Results were reported as 90% confidence intervals (CIs) about the geometric mean AUC_0-∞ and C_max ratios with prespecified equivalence limits of 80% to 125%.

Results: Overall, 370 subjects were enrolled, with 365 receiving ≥1 dose of patiromer; 351 subjects completed the studies and all required treatments. When coadministered with patiromer, the 90% CIs for AUC_0-∞ remained within 80% to 125% for 9 drugs (amlodipine, cinacalcet, clopidogrel, furosemide, lithium, metoprolol, trimethoprim, verapamil, and warfarin). The AUC_0-∞ point estimate ratios for levothyroxine and metformin with patiromer coadministration were ≥80%, with the lower bounds of the 90% CIs at 76.8% and 72.8%, respectively. For ciprofloxacin, the point estimate for AUC_0-∞ was 71.5% (90% CI: 65.3-78.4). For 8 of 12 drugs, point estimates for C_max were ≥80% with patiromer coadministration; for ciprofloxacin, clopidogrel, metformin, and metoprolol, the point estimates were <80%. When patiromer was administered 3 hours after each victim drug, the 90% CIs for AUC_0-∞ and C_max for each drug were within the prespecified 80% to 125% limits.

Conclusion: For 9 of the 12 drugs coadministered with patiromer, there were no clinically significant drug-drug interactions. For 3 drugs (ciprofloxacin, levothyroxine, and metformin), a 3-hour separation between patiromer and their administration resulted in no clinically significant drug-drug interactions.

Keywords: absorption; dose separation; drug–drug interactions; hyperkalemia; patiromer; potassium-binder.

Publication types

Randomized Controlled Trial

MeSH terms

Adolescent
Adult
Area Under Curve
Cross-Over Studies
Drug Interactions
Female
Healthy Volunteers
Humans
Male
Middle Aged
Polymers / adverse effects*
Polymers / pharmacokinetics
Young Adult

Substances

Polymers
patiromer