Proteomic Analysis of Neutrophils in ANCA-associated Vasculitis Reveals a Dysregulation in Proteinase 3-associated Proteins Such As Annexin-A1 Involved in Apoptotic Cell Clearance

Overview

Journal Kidney Int

Publisher Elsevier

Specialty Nephrology

Date 2019 May 31

PMID 31142442

Citations 16

Authors

Judith Everts-Graber

Katherine R Martin

Nathalie Thieblemont

Julie Mocek

Arnaud Roccabianca

Philippe Chafey

Morgane Le Gall

Pascale Tacnet-Delorme

Chris P Reutelingsperger

Jean-Marc Naccache

Bernard Bonnotte

Alexandre Karras

Xavier Puechal

Loic Guillevin

Benjamin Terrier

Philippe Frachet

Mauro Perretti

Luc Mouthon

Veronique Witko-Sarsat

Affiliations

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Abstract

Granulomatosis with polyangiitis (GPA) is an autoimmune vasculitis associated with anti-neutrophil-cytoplasmic antibodies (ANCA) against proteinase 3 leading to kidney damage. Neutrophils from those patients have increased expression of membrane proteinase 3 during apoptosis. Here we examined whether neutrophils from patients with GPA have dysregulated protein expressions associated with apoptosis. A global proteomic analysis was performed comparing neutrophils from patients with GPA, with healthy individuals under basal conditions and during apoptosis. At disease onset, the cytosolic proteome of neutrophils of patients with GPA before treatment was significantly different from healthy controls, and this dysregulation was more pronounced following ex vivo apoptosis. Proteins involved in cell death/survival were altered in neutrophils of patients with GPA. Several proteins identified were PR3-binding partners involved in the clearance of apoptotic cells, namely calreticulin, annexin-A1 and phospholipid scramblase 1. These proteins form a platform at the membrane of apoptotic neutrophils in patients with GPA but not healthy individuals and this was associated with the clinical presentation of GPA. Thus, our study shows that neutrophils from patients with GPA have an intrinsic dysregulation in proteins involved in apoptotic cell clearance, which could contribute to the unabated inflammation and autoimmunity in GPA. Hence, harnessing these dysregulated pathways could lead to novel biomarkers and targeted therapeutic opportunities to treat kidney disease.

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