Distribution of Pathologic Findings in Individuals with Nephrotic Proteinuria According to Serum Albumin

doi:10.1093/ndt/gfm833

NDT Advance Access published online on December 8, 2007
Nephrology Dialysis Transplantation, doi:10.1093/ndt/gfm833

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Distribution of Pathologic Findings in Individuals with Nephrotic Proteinuria According to Serum Albumin

Karn Gupta, Samy S. Iskandar, Pirouz Daeihagh, Heather L. Ratliff and Anthony J. Bleyer

Section on Nephrology, Wake Forest University School of Medicine, Medical Center Boulevard, Winston Salem, NC, USA

Correspondence and offprint requests to: Anthony J. Bleyer, Section on Nephrology, Wake Forest University School of Medicine, Medical Center Boulevard, Winston Salem, NC 27103, USA. Tel: +1-336-716-4513; Fax: +1-336-716-4318; E-mail: ableyer{at}wfubmc.edu

Abstract

Background. Previous studies of the nephrotic syndrome havenot carefully examined the relationship between serum albuminand the distribution of pathologic diagnoses found at the timeof biopsy. The spectrum of pathologic findings in individualswith nephrotic proteinuria and a normal serum albumin has notbeen determined. Knowledge regarding the spectrum of findingsin nephrotic proteinuria according to serum albumin levels mayhelp nephrologists in the clinical decision making of when toperform a renal biopsy and in determining proper managementof these patients.

Methods. Pathologic reports of native kidney biopsies performedfor idiopathic proteinuria >3 g/24 h were reviewed. Clinicalcharacteristics and biopsy findings were compared for individualswith serum albumin <30 g/L (Group I), 30 to <35 g/L (GroupII) and $≥$ 35 g/L (Group III).

Results. There were 57 patients in Group I, 20 in Group II and35 in Group III. The proportion of individuals with focal andsegmental glomerulosclerosis (FSGS) increased according to group:26% in Group I, 45% in Group II and 74% in Group III. Of 35patients in Group III, 34 had FSGS or advanced nephrosclerosisfrom another cause. Seven of 17 Group III patients with follow-uprequired dialysis after a mean interval of 6 years. Few of thesepatients received immunosuppressive therapy.

Conclusions. As serum albumin increases in the nephrotic syndrome,the proportion of patients with FSGS increases. Patients withnephrotic proteinuria and a serum albumin >35 g/L sufferfrom FSGS, nephrosclerosis and have poor renal survival. Whenevaluating nephrotic patients, nephrologists should use thisknowledge about the spectrum of disease in the clinical decisionmaking of when to perform a biopsy and in providing the patientmore precise information regarding risks, benefits and alternativesof the kidney biopsy procedure.

Keywords: focal and segmental glomerulosclerosis; idiopathic nephrotic syndrome; proteinuria; renal biopsy; spectrum of disease

Received for publication: 22. 2.07
Accepted in revised form: 25.10.07

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