Volume 47, Issue 7 p. 825-833

Regadenoson Pharmacokinetics and Tolerability in Subjects With Impaired Renal Function

Dr Toufigh Gordi PhD

Corresponding Author

Dr Toufigh Gordi PhD

Depomed, Inc, Menlo Park, California

Address for correspondence: Toufigh Gordi, PhD, Depomed, Inc, 1360 O'Brien Dr, Menlo Park, CA 94025; e-mail: [email protected].Search for more papers by this author
Dr Brent Blackburn PhD

Dr Brent Blackburn PhD

CVT, Inc, Palo Alto, California

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Dr Hsiao Lieu MD

Dr Hsiao Lieu MD

Portola Pharmaceuticals, Inc, Palo Alto, California

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First published: 07 March 2013
Citations: 51

Abstract

The authors have investigated the pharmacokinetics and tolerability of regadenoson, a selective A2A adenosine receptor agonist for use in drug-stressed myocardial perfusion imaging in subjects with varying degrees of renal function. Sixteen subjects with different creatinine clearance values (range: 15–132 mL/min) received a single intravenous bolus dose of 400 μg regadenoson. A population pharmacokinetic model was developed to describe the pharmacokinetics of regadenoson in these subjects. Regadenoson elimination half-life was prolonged with decreasing renal function. However, maximum plasma concentrations, number, or severity of adverse events did not differ significantly between the subjects. Heart rate increased in all subjects after regadenoson injection but returned to normal within 150 minutes. There were no blood pressure pattern differences with respect to renal function. Results from this study do not indicate that dose adjustments are necessary when subjects with decreased renal function are administered the clinically relevant dose of 400 μg regadenoson.