Pharmacokinetics of the Novel Atrial-Selective Antiarrhythmic Agent Vernakalant Hydrochloride Injection (RSD1235): Influence of CYP2D6 Expression and Other Factors

doi:10.1177/0091270008325148

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First published on October 16, 2008, doi:10.1177/0091270008325148

The Journal of Clinical Pharmacology 2009;49:17.

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©© 2008 American College of Clinical Pharmacology, Inc.
The Journal of Clinical Pharmacology, 10.1177/0091270008325148

Article

Pharmacokinetics of the Novel Atrial-Selective Antiarrhythmic Agent Vernakalant Hydrochloride Injection (RSD1235): Influence of CYP2D6 Expression and Other Factors

Zhongping L. Mao , Jeffery J. Wheeler ¹, Lilian Clohs ¹, Gregory N. Beatch ¹, and James Keirns ²^*

¹ Cardiome Pharma Corporation
² Astellas Pharma US Inc

^* To whom correspondence should be addressed. E-mail: jim.keirns{at}us.astellas.com.

Abstract
Vernakalant hydrochloride injection (RSD1235) is a relativelyatrial-selective antiarrhythmic agent that converts atrial fibrillationrapidly to sinus rhythm. The pharmacokinetics of vernakalantwere explored in healthy volunteers and in patients with atrialfibrillation or atrial flutter in 4 clinical studies. Key pharmacokineticparameters analyzed were the maximum plasma concentration andthe area under the plasma concentration–time curve. Vernakalantexhibited linear pharmacokinetics over the dose range of 0.1mg/kg to 5.0 mg/kg in healthy subjects, and generally showeddose proportionality in patients with atrial fibrillation oratrial flutter who received 1 or 2 vernakalant infusions. Vernakalantwas metabolized rapidly via 4-O-demethylation by cytochromeP450 (CYP)2D6 to its major metabolite RSD1385, which then circulatedpredominantly as an inactive glucuronide conjugate. In mostpatients, the maximum plasma concentration of RSD1385 glucuronideexceeded that of vernakalant. Unconjugated RSD1385 was foundat low levels in all patients demonstrating either a cytochromeP450 CYP2D6 "extensive metabolizer" or "poor metabolizer" phenotypeor genotype; however, CYP2D6 poor metabolizers had even lowerlevels of unconjugated RSD1385. The impact of CYP2D6 metabolizerstatus on vernakalant exposure was explored in patients withatrial fibrillation or atrial flutter who received a therapeuticregimen (3 mg/kg initially via 10-minute intravenous infusionfollowed by a second 2 mg/kg 10-minute infusion if atrial fibrillationpersisted after a 15-minute observation period). In the subsetthat received 2 vernakalant infusions, there was little differencein vernakalant maximum plasma concentration or area under theplasma concentration–time curve from the start of thefirst infusion to 90 minutes between CYP2D6 poor metabolizersand extensive metabolizers or between those who did or did notreceive concomitant CYP2D6-inhibitor medications. Gender, age,and renal function did not have a clinically significant influenceon the pharmacokinetics of vernakalant. These results suggestthat an assessment of CYP2D6 expression may not be needed whenvernakalant is administered acutely and intravenously to patientswith atrial fibrillation.
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