Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
6160834 | Kidney International | 2014 | 5 Pages |
Abstract
The soluble urokinase receptor (suPAR) promotes proteinuria and induces focal segmental glomerulosclerosis (FSGS)-like lesions in mice. A serum suPAR concentration cutoff of 3000Â pg/ml has been proposed as a clinical biomarker for patients with FSGS. Interestingly, several studies in patients with glomerulopathy found an inverse correlation between the estimated glomerular filtration rate (eGFR) and suPAR. As patients with FSGS present at different eGFRs, we studied the relationship between eGFR and suPAR in a cohort of 476 non-FSGS patients and 54 patients with biopsy-proven idiopathic FSGS. In the non-FSGS patients, eGFR was the strongest significant determinant of suPAR. The proposed cutoff for suPAR in FSGS patients was exceeded in 17%, 39%, and 88% in patients with eGFRs of more than 60, 45-60, and 30-45Â ml/min per 1.73Â m2, respectively. In patients with eGFR of <30Â ml/min per 1.73Â m2, suPAR exceeded the cutoff in 95% of patients. Levels of suPAR in patients with idiopathic FSGS overlapped with non-FSGS controls and for any given eGFR did not discriminate FSGS cases from non-FSGS controls. In the overall cohort, there was a negative association between idiopathic FSGS and suPAR, and idiopathic FSGS was not an independent predictor of FSGS concentration over 3000Â pg/ml. Thus, this study does not support an absolute, eGFR-independent, suPAR concentration cutoff as a biomarker for underlying FSGS pathology and questions the validity of relative, eGFR-dependent suPAR cutoff values.
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Authors
Björn Meijers, Rutger J.H. Maas, Ben Sprangers, Kathleen Claes, Ruben Poesen, Bert Bammens, Maarten Naesens, Jeroen K.J. Deegens, Ruth Dietrich, Markus Storr, Jack F.M. Wetzels, Pieter Evenepoel, Dirk Kuypers,