Selective Aldosterone Blockade with Eplerenone Reduces Albuminuria in Patients with Type 2 Diabetes

doi:10.2215/CJN.00240106

HOME

HELP

FEEDBACK

SUBSCRIPTIONS

Diabetes and the Kidney

Selective Aldosterone Blockade with Eplerenone Reduces Albuminuria in Patients with Type 2 Diabetes

Murray Epstein^*, Gordon H. Williams, Myron Weinberger, Andrew Lewin, Scott Krause^||, Robin Mukherjee^||, Rajiv Patni^||, and Bruce Beckerman^||

^* University of Miami School of Medicine, Miami, Florida; Harvard Medical School and Brigham and Women’s Hospital, Boston, Massachusetts; Indiana University School of Medicine, Indianapolis, Indiana; National Research Institute, Los Angeles, California; and ^{^||} Pfizer Inc., New York, New York

Address correspondence to: Dr. Murray Epstein, Nephrology Section, VA Medical Center, 1201 NW 16th Street, Miami, FL 33125. Phone: 305-575-3103; Fax: 305-575-3378; murraye{at}gate.net

Previous studies have shown that the selective aldosterone blockereplerenone, in doses of up to 200 mg/d, reduces albuminuriain patients with type 2 diabetes. This study was conducted toascertain whether lower doses of eplerenone (50 or 100 mg/d)co-administered with the angiotensin-converting enzyme (ACE)inhibitor enalapril would produce a similar antialbuminuriceffect while obviating the hyperkalemia observed previously.After open-label run-in with enalapril 20 mg/d, patients withdiabetes and a urinary albumin:creatinine ratio (UACR) $≥$ 50 mg/gwere randomly assigned to receive enalapril plus one of threedouble-blind daily treatments for 12 wk: placebo, eplerenone50 mg (EPL50), or eplerenone 100 mg (EPL100). After week 4,amlodipine 2.5 to 10 mg/d was allowed for BP control (systolic/diastolicBP $≤$ 130/80 mmHg). The primary study end points were the percentagechange from baseline at week 12 in UACR and the incidence ofhyperkalemia. Secondary end points included percentage changesfrom baseline in UACR at weeks 4 and 8 and changes from baselinein systolic and diastolic BP. Treatment with EPL50 or EPL100but not placebo significantly reduced albuminuria from baseline.By week 12, UACR was reduced by 7.4% in the placebo group, by41.0% in the EPL50 group, and by 48.4% in the EPL100 group (botheplerenone groups, P < 0.001 versus placebo). The incidencesof sustained and severe hyperkalemia were not significantlydifferent in any of the three treatment arms and did not differon the basis of quartile of estimated GFR (all NS). For thesecondary end points, both eplerenone treatment groups significantlyreduced albuminuria from baseline as early as week 4 (P <0.001), whereas placebo treatment (including enalapril) didnot result in any significant decreases in UACR. Systolic BPdecreased significantly in all treatment groups at all timepoints, but, generally, all treatment groups experienced similardecreases in BP. Co-administration of EPL50 or EPL100 with anACE inhibitor as compared with an ACE inhibitor alone significantlyreduces albuminuria in patients with diabetes without producingsignificant increases in hyperkalemia.

This article has been cited by other articles:

T. Berl
Maximizing inhibition of the renin-angiotensin system with high doses of converting enzyme inhibitors or angiotensin receptor blockers
Nephrol. Dial. Transplant., August 1, 2008; 23(8): 2443 - 2447.
[Full Text] [PDF]

G. Remuzzi, D. Cattaneo, and N. Perico
The Aggravating Mechanisms of Aldosterone on Kidney Fibrosis
J. Am. Soc. Nephrol., August 1, 2008; 19(8): 1459 - 1462.
[Abstract] [Full Text] [PDF]

L. M. Ruilope
Aldosterone, Hypertension, and Cardiovascular Disease: An Endless Story
Hypertension, August 1, 2008; 52(2): 207 - 208.
[Full Text] [PDF]

H.-H. Parving, F. Persson, J. B. Lewis, E. J. Lewis, N. K. Hollenberg, and the AVOID Study Investigators
Aliskiren Combined with Losartan in Type 2 Diabetes and Nephropathy
N. Engl. J. Med., June 5, 2008; 358(23): 2433 - 2446.
[Abstract] [Full Text] [PDF]

J. M. C. Connell, S. M. MacKenzie, E. M. Freel, R. Fraser, and E. Davies
A Lifetime of Aldosterone Excess: Long-Term Consequences of Altered Regulation of Aldosterone Production for Cardiovascular Function
Endocr. Rev., April 1, 2008; 29(2): 133 - 154.
[Abstract] [Full Text] [PDF]

D. A. Calhoun
Aldosterone and Cardiovascular Disease: Smoke and Fire
Circulation, December 12, 2006; 114(24): 2572 - 2574.
[Full Text] [PDF]

				G. Remuzzi, D. Cattaneo, and N. Perico The Aggravating Mechanisms of Aldosterone on Kidney Fibrosis J. Am. Soc. Nephrol., August 1, 2008; 19(8): 1459 - 1462. [Abstract] [Full Text] [PDF]

				L. M. Ruilope Aldosterone, Hypertension, and Cardiovascular Disease: An Endless Story Hypertension, August 1, 2008; 52(2): 207 - 208. [Full Text] [PDF]

				H.-H. Parving, F. Persson, J. B. Lewis, E. J. Lewis, N. K. Hollenberg, and the AVOID Study Investigators Aliskiren Combined with Losartan in Type 2 Diabetes and Nephropathy N. Engl. J. Med., June 5, 2008; 358(23): 2433 - 2446. [Abstract] [Full Text] [PDF]

				J. M. C. Connell, S. M. MacKenzie, E. M. Freel, R. Fraser, and E. Davies A Lifetime of Aldosterone Excess: Long-Term Consequences of Altered Regulation of Aldosterone Production for Cardiovascular Function Endocr. Rev., April 1, 2008; 29(2): 133 - 154. [Abstract] [Full Text] [PDF]

				D. A. Calhoun Aldosterone and Cardiovascular Disease: Smoke and Fire Circulation, December 12, 2006; 114(24): 2572 - 2574. [Full Text] [PDF]