Angiotensin II Suppression in Humans by the Orally Active Renin Inhibitor Aliskiren (SPP100): Comparison With Enalapril

doi:10.1161/hy0102.102293

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Hypertension. 2002;39:e1-
doi: 10.1161/hy0102.102293

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(Hypertension. 2002;39:e1.)
© 2002 American Heart Association, Inc.

Hypertension Electronic Pages

Angiotensin II Suppression in Humans by the Orally Active Renin Inhibitor Aliskiren (SPP100)

Comparison With Enalapril

Juerg Nussberger; Grégoire Wuerzner; Chris Jensen; Hans R. Brunner

From the Division of Hypertension and Vascular Medicine, University Hospital Lausanne (J.N., G.W., H.R.B.) and Speedel Pharma (C.J.), Basel, Switzerland.

Correspondence to Juerg Nussberger, MD, Hypertension Division, CHUV, CH-1011 Lausanne, Switzerland. E-mail juerg.nussberger{at}chuv.hospvd.ch

Abstract

Renin is the main determinant of angiotensin (Ang) II levels.It, therefore, always appeared desirable to reduce Ang II levelsby direct inhibition of renin. So far, specific renin inhibitorslacked potency and/or oral availability. We tested the new orallyactive nonpeptidic renin inhibitor SPP100 (Aliskiren, an octanamidewith a 50% inhibitory concentration [IC50] in the low nanomolarrange) in 18 healthy volunteers on a constant 100 mmol/d sodiumdiet using a double-blind, 3-way crossover protocol. In 3 periodsof 8 days, separated by wash-outs of 6 days, each volunteerreceived 2 dosage levels of Aliskiren (low before high; 40 and80 or 160 and 640 mg/d) and randomized placebo or 20 mg enalapril.Aliskiren was well tolerated. Not surprisingly, blood pressureand heart rate remained unchanged in these normotensive subjects.There was a dose-dependent decrease in plasma renin activity,Ang I, and Ang II following single doses of Aliskiren startingwith 40 mg. Inhibition was still marked and significant afterrepeated dosing with maximal decreases in Ang II levels by 89%and 75% on Days 1 and 8, respectively, when the highest doseof Aliskiren was compared with placebo. At the same time, meanplasma active renin was increased 16- and 34-fold at the highestdose of Aliskiren. Plasma drug levels of Aliskiren were dose-dependentwith maximal concentrations reached between 3 to 6 hours afteradministration; steady state was reached between 5 and 8 daysafter multiple dosing. Less than 1% of dose was excreted inthe urine. Plasma and urinary aldosterone levels were decreasedafter doses of Aliskiren $>=$ 80 mg and after enalapril. Aliskirenat 160 and 640 mg enhanced natriuresis on Day 1 by +45% and+62%, respectively, compared with placebo (100%, ie, 87±11mmol/24h) and enalapril (+54%); kaliuresis remained unchanged.In conclusion, the renin inhibitor Aliskiren dose-dependentlydecreases Ang II levels in humans following oral administration.The effect is long-lasting and, at a dose of 160 mg, is equivalentto that of 20 mg enalapril. Aliskiren has the potential to becomethe first orally active renin inhibitor that provides a truealternative to ACE-inhibitors and Ang II receptor antagonistsin therapy for hypertension and other cardiovascular and renaldiseases.

Key Words: renin • angiotensin I • angiotensin-converting enzyme • aldosterone • blood pressure • hypertension, essential • hypertension, renovascular • heart failure

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