Effect of Calcium Channel or ß-Blockade on the Progression of Diabetic Nephropathy in African Americans

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Hypertension. 1997;29:744-750

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Compound via MeSH
Substance via MeSH
ATENOLOL
VERAPAMIL HYDROCHLORIDE
Medline Plus Health Information
Diabetes
Diabetic Kidney Problems
High Blood Pressure

Effect of Calcium Channel or ß-Blockade on the Progression of Diabetic Nephropathy in African Americans

George L. Bakris; Amy Mangrum; J. Brian Copley; Nancy Vicknair; Rebecca Sadler

the Department of Medicine, Division of Nephrology, Ochsner Clinic, New Orleans, La (G.L.B., J.B.C., N.V., R.S.), and Rush University Hypertension Center, Rush-Presbyterian/St Luke's Medical Center, Chicago, Ill (G.L.B., A.M.).

Correspondence to George L. Bakris, MD, FACP, Rush University Hypertension Center, Rush-Presbyterian/St Luke's Medical Center, 1725 W Harrison, Suite 117, Chicago, IL 60612. E-mail gbakris@rpslmc.edu

ß-Blockers are known to slow the progression of diabeticnephropathy by lowering arterial pressure. Moreover, in individualswith diabetic nephropathy, antihypertensive agents that providesustained reductions in proteinuria slow the rate of declinein renal function compared with agents without this antiproteinuriceffect. To examine whether differential effects on proteinuriaaffect the progression of diabetic nephropathy, we conducteda randomized study that compared the effects of a heart rate–loweringcalcium channel blocker, sustained-release verapamil, with thoseof a ß-blocker, atenolol, on the progression of diabeticrenal disease. The primary end point of the study was a changein creatinine clearance slope. Thirty-four African Americanswith the following inclusion criteria were randomized to oneof the two groups: serum creatinine greater than 1.4 mg/dL,proteinuria greater than 1500 mg/d, longer than a 5-year historyof both non–insulin-dependent diabetes mellitus and hypertension,and exclusion of other renal diseases. Goal blood pressure wasless than 140/90 mm Hg. All subjects received loop diureticsas second line agents to help achieve the blood pressure goal.Twenty-four-hour urinary protein and sodium excretions as wellas creatinine clearance were measured at 6-month intervals.Blood pressure was measured every 3 months. After a mean follow-upof 54±6 months, the calcium channel blocker group demonstratedboth a slower rate of decline in creatinine clearance (-1.7±0.9versus -3.7±1.4 mL/min per year per 1.73 m², P<.01)and a greater reduction in proteinuria compared with the atenololgroup. Additionally, a greater proportion of the atenolol grouphad a 50% or more increase in serum creatinine compared withthe verapamil group (32±9% versus 16±7%, P<.05).These between-group differences could not be explained by differencesin blood pressure control. These data support the concept thatantihypertensive agents that persistently maintain reductionsin both arterial pressure and proteinuria slow the progressionof diabetic renal disease in African Americans to a greaterextent than those agents without these effects.

Key Words: blacks • diabetic nephropathies • calcium channel blockers • verapamil • atenolol • adrenergic beta-antagonists

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				J. T. Wright Jr, G. Bakris, T. Greene, L. Y. Agodoa, L. J. Appel, J. Charleston, D. Cheek, J. G. Douglas-Baltimore, J. Gassman, R. Glassock, et al. Effect of Blood Pressure Lowering and Antihypertensive Drug Class on Progression of Hypertensive Kidney Disease: Results From the AASK Trial JAMA, November 20, 2002; 288(19): 2421 - 2431. [Abstract] [Full Text] [PDF]

				P. Swales and B. Williams Review: Calcium channel blockade in combination with angiotensin-converting enzyme inhibition or angiotensin II (AT1-receptor) antagonism in hypertensive diabetics and patients with renal disease and hypertension Journal of Renin-Angiotensin-Aldosterone System, June 1, 2002; 3(2): 79 - 89. [Abstract] [PDF]

				C. Arauz-Pacheco, M. A. Parrott, and P. Raskin The Treatment of Hypertension in Adult Patients With Diabetes Diabetes Care, January 1, 2002; 25(1): 134 - 147. [Full Text] [PDF]

				G. L. Bakris A Practical Approach to Achieving Recommended Blood Pressure Goals in Diabetic Patients Arch Intern Med, December 10, 2001; 161(22): 2661 - 2667. [Abstract] [Full Text] [PDF]

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				B. Nielsen and A. Flyvbjerg Calcium channel blockers - the effect on renal changes in clinical and experimental diabetes: an overview Nephrol. Dial. Transplant., May 1, 2000; 15(5): 581 - 585. [Full Text] [PDF]

				D. R. Abernethy and J. B. Schwartz Calcium-Antagonist Drugs N. Engl. J. Med., November 4, 1999; 341(19): 1447 - 1457. [Full Text] [PDF]

				C.R. Gibbs, D.G. Beevers, and G.Y.H. Lip The management of hypertensive disease in Black patients QJM, April 1, 1999; 92(4): 187 - 192. [Abstract] [Full Text] [PDF]

				M. Hemmelder, D. de Zeeuw, and P. de Jong Antiproteinuric efficacy of verapamil in comparison to trandolapril in non-diabetic renal disease Nephrol. Dial. Transplant., January 1, 1999; 14(1): 98 - 104. [Abstract] [PDF]