Authors
Richard JH Smith, Jessy Alexander, Paul N Barlow, Marina Botto, Thomas L Cassavant, H Terence Cook, Santiago Rodriguez De Córdoba, Gregory S Hageman, T Sakari Jokiranta, William J Kimberling, John D Lambris, Lynne D Lanning, Vicki Levidiotis, Christoph Licht, Hans U Lutz, Seppo Meri, Matthew C Pickering, Richard J Quigg, Angelique L Rops, David J Salant, Sanjeev Sethi, Joshua M Thurman, Hope F Tully, Sean P Tully, Johan Van Der Vlag, Patrick D Walker, Reinhard Würzner, Peter F Zipfel
Publication date
2007/9/1
Journal
Journal of the American Society of Nephrology
Volume
18
Issue
9
Pages
2447-2456
Publisher
American Society of Nephrology
Description
The development of clinical treatment protocols usually relies on evidence-based guidelines that focus on randomized, controlled trials. For rare renal diseases, such stringent requirements can represent a significant challenge. Dense deposit disease (DDD; also known as membranoproliferative glomerulonephritis type II) is a prototypical rare disease. It affects only two to three people per million and leads to renal failure within 10 yr in 50% of affected children. On the basis of pathophysiology, this article presents a diagnostic and treatment algorithm for patients with DDD. Diagnostic tests should assess the alternative pathway of complement for abnormalities. Treatment options include aggressive BP control and reduction of proteinuria, and on the basis of pathophysiology, animal data, and human studies, plasma infusion or exchange, rituximab, sulodexide, and eculizumab are additional options. Criteria for …
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Scholar articles
RJH Smith, J Alexander, PN Barlow, M Botto… - Journal of the American Society of Nephrology, 2007