Label-free Quantitative Urinary Proteomics Identifies the Arginase Pathway As a New Player in Congenital Obstructive Nephropathy

Overview

Journal Mol Cell Proteomics

Specialties Biochemistry
Cell Biology
Molecular Biology

Date 2014 Sep 11

PMID 25205225

Citations 7

Authors

Chrystelle Lacroix

Cecile Caubet

Anne Gonzalez-de-Peredo

Benjamin Breuil

David Bouyssie

Alexandre Stella

Luc Garrigues

Caroline Le Gall

Anthony Raevel

Angelique Massoubre

Julie Klein

Stephane Decramer

Frederique Sabourdy

Flavio Bandin

Odile Burlet-Schiltz

Bernard Monsarrat

Joost-Peter Schanstra

Jean-Loup Bascands

Affiliations

Soon will be listed here.

Abstract

Obstructive nephropathy is a frequently encountered situation in newborns. In previous studies, the urinary peptidome has been analyzed for the identification of clinically useful biomarkers of obstructive nephropathy. However, the urinary proteome has not been explored yet and should allow additional insight into the pathophysiology of the disease. We have analyzed the urinary proteome of newborns (n = 5/group) with obstructive nephropathy using label free quantitative nanoLC-MS/MS allowing the identification and quantification of 970 urinary proteins. We next focused on proteins exclusively regulated in severe obstructive nephropathy and identified Arginase 1 as a potential candidate molecule involved in the development of obstructive nephropathy, located at the crossroad of pro- and antifibrotic pathways. The reduced urinary abundance of Arginase 1 in obstructive nephropathy was verified in independent clinical samples using both Western blot and MRM analysis. These data were confirmed in situ in kidneys obtained from a mouse obstructive nephropathy model. In addition, we also observed increased expression of Arginase 2 and increased total arginase activity in obstructed mouse kidneys. mRNA expression analysis of the related arginase pathways indicated that the pro-fibrotic arginase-related pathway is activated during obstructive nephropathy. Taken together we have identified a new actor in the development of obstructive nephropathy in newborns using quantitative urinary proteomics and shown its involvement in an in vivo model of disease. The present study demonstrates the relevance of such a quantitative urinary proteomics approach with clinical samples for a better understanding of the pathophysiology and for the discovery of potential therapeutic targets.

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