Uromodulin and α(1)-antitrypsin urinary peptide analysis to differentiate glomerular kidney diseases.

نویسندگان

  • Maribel Navarro-Muñoz
  • Meritxell Ibernon
  • Josep Bonet
  • Vanessa Pérez
  • Mari Cruz Pastor
  • Beatriz Bayés
  • Juan Casado-Vela
  • Maruja Navarro
  • Jordi Ara
  • Anna Espinal
  • Lourdes Fluvià
  • Assumpta Serra
  • Dolores López
  • Ramón Romero
چکیده

BACKGROUND/AIMS Glomerular kidney disease (GKD) is suspected in patients based on proteinuria, but its diagnosis relies primarily on renal biopsy. We used urine peptide profiling as a noninvasive means to link GKD-associated changes to each glomerular entity. METHODS Urinary peptide profiles of 60 biopsy-proven glomerular patients and 14 controls were analyzed by combining magnetic bead peptide enrichment, MALDI-TOF MS analysis, and ClinProTools v2.0 to select differential peptides. Tentative identification of the differential peptides was carried out by HPLC-MS/MS. RESULTS The HPLC-MS/MS results suggest that uromodulin (UMOD; m/z: 1682, 1898 and 1913) and α(1)-antitrypsin (A1AT; m/z: 1945, 2392 and 2505) are differentially expressed urinary peptides that distinguish between GKD patients and healthy subjects. Low UMOD and high A1AT peptide abundance was observed in 80-92% of patients with GKD. Proliferative forms of GKD were distinguished from nonproliferative forms, based on a combination of UMOD and A1AT peptides. Nonproliferative forms correlated with higher A1AT peptide levels - focal segmental glomerulosclerosis was linked more closely to high levels of the m/z 1945 peptide than minimal change disease. CONCLUSION We describe a workflow - urinary peptide profiling coupled with histological findings - that can be used to distinguish GKD accurately and noninvasively, particularly its nonproliferative forms.

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عنوان ژورنال:
  • Kidney & blood pressure research

دوره 35 5  شماره 

صفحات  -

تاریخ انتشار 2012