Pharmacological inhibition of cathepsin S and of NSPs-AAP-1 (a novel, alternative protease driving the activation of neutrophil serine proteases)

Roxane Domain; Seda Seren; Uwe Jerke; Manousos Makridakis; Kuan-Ju Chen; Jérôme Zoidakis; Moez Rhimi; Xian Zhang; Tillia Bonvent; Cécile Croix; Loïc Gonzalez; Dedong Li; Jessica Basso; Christophe Paget; Marie-Claude Viaud-Massuard; Gilles Lalmanach; Guo-Ping Shi; Ali Aghdassi; Antonia Vlahou; Patrick P McDonald; Isabelle Couillin; Rich Williams; Ralph Kettritz; Brice Korkmaz

doi:10.1016/j.bcp.2024.116114

Pharmacological inhibition of cathepsin S and of NSPs-AAP-1 (a novel, alternative protease driving the activation of neutrophil serine proteases)

Biochem Pharmacol. 2024 Nov:229:116114. doi: 10.1016/j.bcp.2024.116114. Epub 2024 Sep 16.

Authors

Roxane Domain¹, Seda Seren¹, Uwe Jerke², Manousos Makridakis³, Kuan-Ju Chen⁴, Jérôme Zoidakis³, Moez Rhimi⁵, Xian Zhang⁶, Tillia Bonvent¹, Cécile Croix¹, Loïc Gonzalez¹, Dedong Li⁴, Jessica Basso⁴, Christophe Paget¹, Marie-Claude Viaud-Massuard¹, Gilles Lalmanach¹, Guo-Ping Shi⁷, Ali Aghdassi⁸, Antonia Vlahou³, Patrick P McDonald⁴, Isabelle Couillin⁹, Rich Williams¹⁰, Ralph Kettritz¹¹, Brice Korkmaz¹²

Affiliations

¹ INSERM UMR-1100, Research Center for Respiratory Diseases, Tours, France; Université de Tours, Tours, France.
² Experimental and Clinical Research Center, Charité und Max-Delbrück-Centrum für Molekulare Medizin in der Helmholtz-Gemeinschaft (MDC), Berlin, Germany.
³ Biotechnology Division, Biomedical Research Foundation, Academy of Athens, Athens, Greece.
⁴ Research Department, Insmed Incorporated, Bridgewater, NJ, USA.
⁵ INRAE UMR-1319, Microbiota Interaction with Human and Animal Team (MIHA), Micalis Institute, AgroParisTech, Université Paris-Saclay, Jouy-en-Josas, France.
⁶ School of Food and Biological Engineering, Hefei University of Technology, Hefei, Anhui, China.
⁷ Department of Medicine, Cardiovascular Medicine, Brigham and Women's Hospital and Harvard Medical School, Boston, MA, USA.
⁸ Department of Medicine A - Gastroenterology, Nephrology, Endocrinology and Rheumatology, University Medicine Greifswald, Greifswald, Germany.
⁹ CNRS UMR-7355, Experimental and Molecular Immunology and Neurogenetics, Université d'Orléans, Orleans, France.
¹⁰ The Patrick G Johnston Center for Cancer Research, Queen's University, Belfast, UK.
¹¹ Experimental and Clinical Research Center, Charité und Max-Delbrück-Centrum für Molekulare Medizin in der Helmholtz-Gemeinschaft (MDC), Berlin, Germany; Nephrology and Intensive Care Medicine, Charité-Universitätsmedizin, Berlin, Germany.
¹² INSERM UMR-1100, Research Center for Respiratory Diseases, Tours, France; Université de Tours, Tours, France. Electronic address: [email protected].

PMID: 39455238
DOI: 10.1016/j.bcp.2024.116114

Abstract

An uncontrolled activity of neutrophil serine proteases (NSPs) contributes to inflammatory diseases. Cathepsin C (CatC) is known to activate NSPs during neutrophilic differentiation and represents a promising pharmacological target in NSP-mediated diseases. In humans, Papillon-Lefèvre syndrome (PLS) patients have mutations in theirCTSC gene, resulting in the complete absence of CatC activity. Despite this, low residual NSP activities are detected in PLS neutrophils (<10% vs healthy individuals), suggesting the involvement of CatC-independent proteolytic pathway(s) in the activation of proNSPs. This prompted us to characterize CatC-independent NSP activation pathways by blocking proCatC maturation. In this study, we show that inhibition of intracellular CatS almost completely blocked CatC maturation in human promyeloid HL-60 cells. Despite this, NSP activation was not significantly reduced, confirming the presence of a CatC-independent activation pathway involving a CatC-like protease that we termed NSPs-AAP-1. Similarly, when human CD34⁺ progenitor cells were treated with CatS inhibitors during neutrophilic differentiation in vitro, CatC activity was nearly abrogated but ∼30% NSP activities remained, further supporting the existence of NSPs-AAP-1. Our data indicate that NSPs-AAP-1 is a cysteine protease that is inhibited by reversible nitrile compounds designed for CatC inhibition. We further established a proof of concept for the indirect, although incomplete, inhibition of NSPs by pharmacological targeting of CatC maturation using CatS inhibitors. This emphasizes the potential of CatS as a therapeutic target for inflammatory diseases. Thus, preventing proNSP maturation using a CatS inhibitor, alone or in combination with a CatC/NSPs-AAP-1 inhibitor, represents a promising approach to efficiently control the extent of tissue injury in neutrophil-mediated inflammatory diseases.

Keywords: Cathepsin C; Cysteine cathepsin; Neutrophil serine protease; Synthetic inhibitor; Therapeutic approach; Zymogen.

Publication types

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

MeSH terms

Cathepsin C / antagonists & inhibitors
Cathepsin C / metabolism
Cathepsins* / antagonists & inhibitors
Cathepsins* / metabolism
Enzyme Activation / drug effects
Enzyme Activation / physiology
HL-60 Cells
Humans
Neutrophils* / drug effects
Neutrophils* / enzymology
Neutrophils* / metabolism
Papillon-Lefevre Disease / drug therapy
Papillon-Lefevre Disease / metabolism
Serine Proteases / metabolism
Serine Proteinase Inhibitors / pharmacology

Substances

Cathepsins
cathepsin S
Cathepsin C
Serine Proteases
Serine Proteinase Inhibitors