Literature DB >> 25895746

A multidrug, antiproteinuric approach to alport syndrome: a ten-year cohort study.

Erica Daina1, Paolo Cravedi1,2, Mirella Alpa3, Dario Roccatello3, Sara Gamba1, Annalisa Perna1, Flavio Gaspari1, Giuseppe Remuzzi1,4, Piero Ruggenenti1,4.   

Abstract

BACKGROUND/AIMS: Combined ACE inhibitor, angiotensin-receptor-blocker, non-dihydropyridine calcium-channel-blocker, and statin therapy (Remission Clinic) reduced proteinuria and halted progression in non-diabetic nephropathies, but their efficacy in Alport syndrome (AS) nephropathy is unknown.
METHODS: From February 2004 to September 2007, we included nine albuminuric AS adults with creatinine clearance >20 ml/min/1.73 m(2) in a single-center, open-label, prospective, off-on-off academic study. After the 1-month wash-out from RAS inhibition (Run-in), patients entered the 4-month, add-on, treatment period with benazepril (10-20 mg/day), valsartan (80-160 mg/day), diltiazem (60-120 mg/day), and fluvastatin (40-80 mg/day) followed by the 1-month wash-out (Recovery). The primary outcome was albuminuria at month 4. After recovery, patients were kept on the Remission Clinic protocol and followed until July 2014 (Extension).
RESULTS: The median (IQR) albuminuria progressively declined from 657.7 (292.7-1,089.6) μg/min at baseline to 71.4 (21.7-504.9) μg/min at treatment end (p = 0.009) and raised to 404.3 (167.9-446.8) μg/min after recovery. Albumin and IgG fractional clearances significantly (p ≤ 0.005) decreased from 66.9 (53.6-80.8) to 9.4 (4.6-26.0) and from 5.1 (3.0-8.4) to 1.1 (0.6-3.2), and then recovered toward baseline. Blood pressure and lipids significantly decreased on treatment, without changes in inulin-measured GFR or para-aminohippuric-measured RPF. After recovery, one patient refused to enter the extension, one with severe renal insufficiency at baseline reached ESRD, and seven retained normal serum creatinine until the end of the study. At the final visit, three were microalbuminuric and one was normoalbuminuric. Treatment was well tolerated.
CONCLUSION: The Remission Clinic approach safely ameliorated albuminuria, blood pressure, lipids, and glomerular selectivity in AS patients and halted long-term progression in those without renal insufficiency to start with.
© 2015 S. Karger AG, Basel.

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Year:  2015        PMID: 25895746      PMCID: PMC4451141          DOI: 10.1159/000381480

Source DB:  PubMed          Journal:  Nephron        ISSN: 1660-8151            Impact factor:   2.847


  15 in total

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Authors:  Kasper Rossing; Per K Christensen; Berit R Jensen; Hans-Henrik Parving
Journal:  Diabetes Care       Date:  2002-01       Impact factor: 19.112

Review 2.  Systemic and glomerular hypertension in progressive renal disease.

Authors:  S Anderson
Journal:  Kidney Int Suppl       Date:  1988-09       Impact factor: 10.545

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Authors:  A Remuzzi; S Puntorieri; C Battaglia; T Bertani; G Remuzzi
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Review 4.  Progression, remission, regression of chronic renal diseases.

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5.  Comparison of the effects of angiotensin-converting enzyme inhibition and angiotensin II receptor blockade on the evolution of spontaneous glomerular injury in male MWF/Ztm rats.

Authors:  A Remuzzi; B Malanchini; C Battaglia; T Bertani; G Remuzzi
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7.  A controlled, prospective study of the effects of atorvastatin on proteinuria and progression of kidney disease.

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9.  Preemptive ramipril therapy delays renal failure and reduces renal fibrosis in COL4A3-knockout mice with Alport syndrome.

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10.  Effects of combined ACE inhibitor and angiotensin II antagonist treatment in human chronic nephropathies.

Authors:  Ruth Campbell; Fabio Sangalli; Elena Perticucci; Claudio Aros; Cecilia Viscarra; Annalisa Perna; Andrea Remuzzi; Federico Bertocchi; Luca Fagiani; Giuseppe Remuzzi; Piero Ruggenenti
Journal:  Kidney Int       Date:  2003-03       Impact factor: 10.612

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2.  Achieving remission of proteinuria in childhood CKD.

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