Diabetic Nephropathy Clinical Trial
Official title:
Eplerenone, ACE Inhibition and Albuminuria
The purpose of this study is to determine whether eplerenone is more effective than doubling the dose of ACE inhibitor in reducing urinary protein (albumin) loss in diabetes mellitus
In patients with proteinuric renal diseases renal function almost invariably deteriorates,
independent from the original renal disease. It has been demonstrated that the rapidity of
renal function deterioration is determined by blood pressure and proteinuria1. Treatment
modalities that lower proteinuria in general tend to attenuate the deterioration of renal
function. As such, ACE-inhibitors have been proven to be of particular value in the
treatment of patients with proteinuria, since these drugs consistently lower proteinuria.
More recently, similar antiproteinuric effects have been described for the angiotensin
receptor blockers (ARBs). Theoretically, ACE inhibitors may have advantages over ARBs
because they are supposed to increase bradykinin levels. Bradykinin has also been implicated
in the development of nephropathy in mice. About its role in human diabetic nephropathy few
if any data exist. The effect of ACE inhibition or ARBs is not complete, since addition of
either drug to the other may further improve albuminuria. This may be explained by
insufficient dosage of single drug therapy or because of an escape phenomenon. The latter
has been amply described for ACE inhibitors. Especially with chronic ACE inhibition
angiotensin II levels may be near normal. This may lead to persistent angiotensin II
effects, among which aldosterone stimulation.
Even though most investigators have emphasized the role of the renin-angiotensin system in
progressive renal injury, aldosterone has received little attention. However, its
profibrotic effects make aldosterone a potentially important player in the field, even more
so because the escape of aldosterone during treatment with ACE-inhibitors or ARBs. Moreover,
in addition to these theoretical considerations, evidence is emerging that mineralocorticoid
receptor blockade with spironolactone added to ACE-inhibitors or ARBs indeed has an
additive, favourable effect on proteinuria. These findings warrant a search for the value of
such agents in albuminuria and exploration of the mechanisms by which mineralocorticoid
blockade may exert its beneficial effects.
Primary aim:
1. To study whether the combination of eplerenone and a standard dose of ACE-inhibition has
an additive effect on albuminuria in patients with albuminuric nephropathy compared to ACE-I
alone, or double dose of ACE-inhibitor.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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