Original Article
Kidney International (2007) 71, 417–424. doi:10.1038/sj.ki.5002075; published online 10 January 2007
Effect of combining ACE inhibition with aldosterone blockade on proteinuria and renal damage in experimental nephrosis
A B Kramer1,2, E F van der Meulen1, I Hamming1, H van Goor1 and G Navis2
- 1Department of Pathology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands
- 2Department of Nephrology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands
Correspondence: GJ Navis, Department of Nephrology, University Medical Center Groningen, PO Box 30.001, Groningen 9700 RB, The Netherlands. E-mail: g.j.navis@int.umcg.nl
Received 4 January 2006; Revised 7 November 2006; Accepted 14 November 2006; Published online 10 January 2007.
Abstract
Aldosterone has pro-fibrotic properties and is a potential target for additional intervention in patients with chronic renal disease showing resistance to therapy during treatment with angiotensin-converting enzyme inhibitors (ACEi). Combining ACEi and aldosterone receptor blockade (aldoRB) in proteinuric renal disease reduces proteinuria, but effects on proteinuria-induced renal damage are unknown. We studied the effect of ACEi/aldoRB in adriamycin nephrosis (AN). Six weeks after injection of adriamycin in Wistar rats, randomized treatment with vehicle (VEH, n=8), aldoRB (n=12), ACEi (n=10), or a combination of ACEi/aldoRB (n=14) was given for 12 weeks. Healthy rats served as controls (n=6). Renal damage was quantified by markers of tubular injury (osteopontin (OPN) and kidney injury molecule-1 (Kim-1)), pre-fibrotic lesions (
-smooth muscle actin (SMA)), interstitial fibrosis (IF), and focal glomerulosclerosis (FGS). In AN animals, proteinuria was increased compared with controls. ACEi and ACEi/aldoRB significantly reduced proteinuria compared with VEH, whereas aldoRB monotherapy was without effect. Blood pressure was reduced in ACEi and ACEi/aldoRB compared with VEH and aldoRB. OPN and Kim-1 were increased in AN animals, but significantly reduced by ACEi/aldoRB. Treatment with ACEi and ACEi/aldoRB prevented an increase of SMA, IF, and FGS. In conclusion, ACEi/aldoRB effectively reduced proteinuria and markers of tubular injury and prevented renal damage in this rat model of chronic proteinuria-induced renal damage.
Keywords:
adosterone blockade, spironolactone, ACE-inhibition, proteinuria, focal glomerulosclerosis, interstitial fibrosis
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