Single dose oral ranolazine pharmacokinetics in patients receiving maintenance hemodialysis

Authors

Bridget A. Scoville, St. Alexius Medical Center
Jonathan H. Segal, University of Michigan Medical School
Noha N. Salama, Faculty of Pharmacy
Michael Heung, University of Michigan Medical School
Barry E. Bleske, UNM College of Pharmacy
Rachel F. Eyler, University of Connecticut
Bruce A. Mueller, University of Michigan, Ann Arbor

Document Type

Article

Publication Title

Renal Failure

Abstract

Purpose: Ranolazine is a novel anti-angina treatment approved in the United States for chronic stable angina. Ranolazine pharmacokinetics have not been studied previously in patients who receive maintenance hemodialysis. This study describes the pharmacokinetics of ranolazine and three major metabolites (CVT-2738, CVT-2512, CVT-2514) in patients receiving thrice weekly hemodialysis. Methods: Eight participants receiving maintenance hemodialysis completed this prospective, open-label study (study identifier NCT01435174 at Clinicaltrials.gov). Three participants received a single tablet of ranolazine 500 mg (followed by an interim analysis), and five received 2 tablets of ranolazine 500 mg. Blood samples were collected over 65 h to determine the pharmacokinetic characteristics during and between hemodialysis sessions. Non-compartmental analysis was used to determine the individual pharmacokinetic parameters. Results: Ranolazine off-hemodialysis elimination phase half-lives were 3.6 and 3.9 h for 500 mg and 1000 mg doses, respectively. The time to maximum concentration ranged from 2 to 18 hours and the average maximum concentration was 0.65 ± 0.27 mcg/mL and 1.18 ± 0.48 mcg/mL for ranolazine 500 mg and 1000 mg dose, respectively. The mean hemodialysis percent reduction ratio for the ranolazine 500 mg dose was 52.3 ± 8.1% and for the ranolazine 1000 mg dose was 69.2 ± 37.6%. Conclusions: Data on ranolazine dosing in patients receiving maintenance hemodialysis is almost non-existent. Given the extent of pharmacokinetic variability observed with the 500 mg and 1000 mg oral doses of ranolazine, neither can be recommended as a starting dose in patients receiving maintenance hemodialysis. Guided by the information gained form this study about the extent of hemodialytic drug clearance, further multi-dose clinical trials of ranolazine are needed to optimize therapeutic outcomes in this patient population.

First Page

118

Last Page

125

DOI

10.1080/0886022X.2019.1585371

Publication Date

1-1-2019

Recommended Citation

Scoville, Bridget A.; Segal, Jonathan H.; Salama, Noha N.; Heung, Michael; Bleske, Barry E.; Eyler, Rachel F.; and Mueller, Bruce A., "Single dose oral ranolazine pharmacokinetics in patients receiving maintenance hemodialysis" (2019). Pharmaceutical and Administrative Sciences Faculty Publications. 230. https://doi.org/10.1080/0886022X.2019.1585371
https://collections.uhsp.edu/pharm-admin-sciences_pubs/230