Consequences of cathepsin C inactivation for membrane exposure of proteinase 3, the target antigen in autoimmune vasculitis

Seda Seren; Maha Rashed Abouzaid; Claudia Eulenberg-Gustavus; Josefine Hirschfeld; Hala Nasr Soliman; Uwe Jerke; Koffi N'Guessan; Sandrine Dallet-Choisy; Adam Lesner; Conni Lauritzen; Beate Schacher; Peter Eickholz; Nikoletta Nagy; Marta Szell; Cécile Croix; Marie-Claude Viaud-Massuard; Abdullah Al Farraj Aldosari; Shivanna Ragunatha; Mostafa Ibrahim Mostafa; Francesca Giampieri; Maurizio Battino; Hélène Cornillier; Gérard Lorette; Jean-Louis Stephan; Cyril Goizet; John Pedersen; Francis Gauthier; Dieter E Jenne; Sylvain Marchand-Adam; Iain L Chapple; Ralph Kettritz; Brice Korkmaz

doi:10.1074/jbc.RA118.001922

Consequences of cathepsin C inactivation for membrane exposure of proteinase 3, the target antigen in autoimmune vasculitis

J Biol Chem. 2018 Aug 10;293(32):12415-12428. doi: 10.1074/jbc.RA118.001922. Epub 2018 Jun 20.

Authors

Seda Seren¹, Maha Rashed Abouzaid², Claudia Eulenberg-Gustavus³, Josefine Hirschfeld⁴, Hala Nasr Soliman⁵, Uwe Jerke³, Koffi N'Guessan¹, Sandrine Dallet-Choisy¹, Adam Lesner⁶, Conni Lauritzen⁷, Beate Schacher⁸, Peter Eickholz⁸, Nikoletta Nagy⁹, Marta Szell⁹, Cécile Croix¹⁰, Marie-Claude Viaud-Massuard¹⁰, Abdullah Al Farraj Aldosari¹¹, Shivanna Ragunatha¹², Mostafa Ibrahim Mostafa², Francesca Giampieri¹³, Maurizio Battino¹³, Hélène Cornillier¹⁴, Gérard Lorette¹⁵, Jean-Louis Stephan¹⁶, Cyril Goizet¹⁷, John Pedersen⁷, Francis Gauthier¹, Dieter E Jenne^{18

19}, Sylvain Marchand-Adam¹, Iain L Chapple⁴, Ralph Kettritz^{3

20}, Brice Korkmaz²¹

Affiliations

¹ From the INSERM U-1100, "Centre d'Etude des Pathologies Respiratoires" and Université de Tours, 37000 Tours, France.
² the Departments of Oro-Dental Genetics and.
³ the Experimental and Clinical Research Center, Charité und Max-Delbrück-Centrum für Molekulare Medizin in der Helmholtz-Gemeinschaft (MDC), 13125 Berlin, Germany.
⁴ the Institute of Clinical Sciences, College of Medical and Dental Sciences, Periodontal Research Group, University of Birmingham and Birmingham Community Health Trust, Edgbaston, Birmingham B5 7EG, United Kingdom.
⁵ Medical Molecular Genetics, National Research Centre, Cairo 12622, Egypt.
⁶ the Faculty of Chemistry, University of Gdansk, 80-309 Gdansk, Poland.
⁷ Unizyme Laboratories A/S, 2970 Hørsholm, Denmark.
⁸ the Department of Periodontology, Johann Wolfgang Goethe-University Frankfurt, 60323 Frankfurt, Germany.
⁹ the Department of Medical Genetics, University of Szeged, Szeged 6720, Hungary.
¹⁰ UMR-CNRS 7292 "Génétique, Immunothérapie, Chimie et Cancer" and Université François Rabelais, 37000 Tours, France.
¹¹ the Department of Prosthetic Dental Science, College of Dentistry, King Saud University, Riyadh 12372, Kingdom of Saudi Arabia.
¹² the Department of Dermatology, Venereology, and Leprosy, ESIC Medical College and PGIMSR Rajajinagar, Bengaluru, Karnataka 560010, India.
¹³ the Department of Clinical Sciences, Università Politecnica delle Marche, 60121 Ancona, Italy.
¹⁴ Service de Dermatologie, Centre Hospitalier Universitaire de Tours, Université de Tours, 37000 Tours, France.
¹⁵ UMR-INRA1282 "Laboratoire de Virologie et Immunologie Moléculaires," Université de Tours, 37000 Tours, France.
¹⁶ the Service d'Hématologie Immunologie et Rhumatologie Pédiatrique, Centre Hospitalier Universitaire de Saint-Etienne, 42270 Saint-Priest-en-Jarez, France.
¹⁷ INSERM U-1211, Rare Diseases, Genetic and Metabolism, MRGM Laboratory, Pellegrin Hospital and University, 33000 Bordeaux, France.
¹⁸ the Comprehensive Pneumology Center, Institute of Lung Biology and Disease, German Center for Lung Research (DZL), 81377 Munich, Germany.
¹⁹ the Max Planck Institute of Neurobiology, 82152 Planegg-Martinsried, Germany, and.
²⁰ the Division of Nephrology and Intensive Care Medicine, Medical Department, Charité-Universitätsmedizin, 10117 Berlin, Germany.
²¹ From the INSERM U-1100, "Centre d'Etude des Pathologies Respiratoires" and Université de Tours, 37000 Tours, France, brice.korkmaz@inserm.fr.

Abstract

Membrane-bound proteinase 3 (PR3^m) is the main target antigen of anti-neutrophil cytoplasmic autoantibodies (ANCA) in granulomatosis with polyangiitis, a systemic small-vessel vasculitis. Binding of ANCA to PR3^m triggers neutrophil activation with the secretion of enzymatically active PR3 and related neutrophil serine proteases, thereby contributing to vascular damage. PR3 and related proteases are activated from pro-forms by the lysosomal cysteine protease cathepsin C (CatC) during neutrophil maturation. We hypothesized that pharmacological inhibition of CatC provides an effective measure to reduce PR3^m and therefore has implications as a novel therapeutic approach in granulomatosis with polyangiitis. We first studied neutrophilic PR3 from 24 patients with Papillon-Lefèvre syndrome (PLS), a genetic form of CatC deficiency. PLS neutrophil lysates showed a largely reduced but still detectable (0.5-4%) PR3 activity when compared with healthy control cells. Despite extremely low levels of cellular PR3, the amount of constitutive PR3^m expressed on the surface of quiescent neutrophils and the typical bimodal membrane distribution pattern were similar to what was observed in healthy neutrophils. However, following cell activation, there was no significant increase in the total amount of PR3^m on PLS neutrophils, whereas the total amount of PR3^m on healthy neutrophils was significantly increased. We then explored the effect of pharmacological CatC inhibition on PR3 stability in normal neutrophils using a potent cell-permeable CatC inhibitor and a CD34⁺ hematopoietic stem cell model. Human CD34⁺ hematopoietic stem cells were treated with the inhibitor during neutrophil differentiation over 10 days. We observed strong reductions in PR3^m, cellular PR3 protein, and proteolytic PR3 activity, whereas neutrophil differentiation was not compromised.

Keywords: Papillon-Lefèvre syndrome; aminopeptidase; antigen; autoimmune disease; cathepsin C; genetic disease; granulomatosis with polyangiitis; neutrophil; protease; protease inhibitor; proteinase 3.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Adult
Case-Control Studies
Cathepsin C / antagonists & inhibitors*
Cell Membrane / metabolism*
Child
Child, Preschool
Cysteine Proteinase Inhibitors / pharmacology*
Female
Granulomatosis with Polyangiitis / drug therapy
Granulomatosis with Polyangiitis / genetics
Granulomatosis with Polyangiitis / metabolism
Granulomatosis with Polyangiitis / pathology*
Humans
Male
Myeloblastin / genetics
Myeloblastin / metabolism*
Neutrophils / enzymology
Proteolysis
Young Adult

Substances

Cysteine Proteinase Inhibitors
CTSC protein, human
Cathepsin C
Myeloblastin