Renal disease in scleroderma: an update on evaluation, risk stratification, pathogenesis and management
- PMID: 22955019
- PMCID: PMC4048657
- DOI: 10.1097/BOR.0b013e3283588dcf
Renal disease in scleroderma: an update on evaluation, risk stratification, pathogenesis and management
Abstract
Purpose of review: Renal disease remains an important cause of morbidity and mortality in scleroderma. The spectrum of renal complications in systemic sclerosis includes scleroderma renal crisis (SRC), normotensive renal crisis, antineutrophil cytoplasmic antibodies-associated glomerulonephritis, penacillamine-associated renal disease, and reduced renal functional reserves manifested by proteinuria, microalbuminuria, or isolated reduction in glomerular filtration rate. The purpose of this review is to provide a concise and up-to-date review of the evaluation, risk stratification, pathogenesis, and management of scleroderma-associated renal disease.
Recent findings: Although SRC survival has significantly improved, mortality of this complication remains high outside of specialized centers. Recent data demonstrate strong associations between anti-RNA polymerase III antibodies and SRC. Subclinical renal impairment affects approximately 50% of scleroderma patients and may be associated with other vascular manifestations. Subclinical renal involvement rarely progresses to end-stage renal failure; however, recent studies suggest it may predict mortality in patients with other vasculopathic manifestations.
Summary: Testing for anti-RNA polymerase III antibodies should be incorporated into clinical care to identify patients at high risk for SRC. Recommendations from European League Against Rheumatism (EULAR), EULAR Scleroderma Trials and Research, and the Scleroderma Clinical Trials Consortium confirm angiotensin-converting enzyme inhibitors as first-line therapy for SRC, and give recommendations for second-line agents.
Conflict of interest statement
Dr V.K.S. has no relevant scientific disclosures related to this article. She is currently supported by award numbers KL2RR031974 and UL1RR031975 from the National Center for Research Resources.
Dr V.D.S. has no relevant scientific disclosures related to this article. She has received research funding in the past 2 years from the NIH (R01HL089758-01A1 and N01-AR-0-2251) and from Acterlion, United Therapeutics, Gilead, Roche and Celgene. She has received consulting income from United Therapeutics, Gilead, Roche and Sanofi, and is on the Speakers Bureau for Actelion and Gilead.
The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Center for Research Resources or the National Institutes of Health.
All authors were involved in drafting the article and revising it critically for important intellectual content. All authors approved the final version to be published. The authors have no conflicts of interest.
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