Literature DB >> 29842917

Therapeutic targeting of cathepsin C: from pathophysiology to treatment.

Brice Korkmaz1, George H Caughey2, Iain Chapple3, Francis Gauthier4, Josefine Hirschfeld3, Dieter E Jenne5, Ralph Kettritz6, Gilles Lalmanach4, Anne-Sophie Lamort5, Conni Lauritzen7, Monika Łȩgowska8, Adam Lesner8, Sylvain Marchand-Adam4, Sarah J McKaig9, Celia Moss10, John Pedersen7, Helen Roberts3, Adrian Schreiber6, Seda Seren4, Nalin S Thakker11.   

Abstract

Cathepsin C (CatC) is a highly conserved tetrameric lysosomal cysteine dipeptidyl aminopeptidase. The best characterized physiological function of CatC is the activation of pro-inflammatory granule-associated serine proteases. These proteases are synthesized as inactive zymogens containing an N-terminal pro-dipeptide, which maintains the zymogen in its inactive conformation and prevents premature activation, which is potentially toxic to the cell. The activation of serine protease zymogens occurs through cleavage of the N-terminal dipeptide by CatC during cell maturation in the bone marrow. In vivo data suggest that pharmacological inhibition of pro-inflammatory serine proteases would suppress or attenuate deleterious effects mediated by these proteases in inflammatory/auto-immune disorders. The pathological deficiency in CatC is associated with Papillon-Lefèvre syndrome (PLS). The patients however do not present marked immunodeficiency despite the absence of active serine proteases in immune defense cells. Hence, the transitory pharmacological blockade of CatC activity in the precursor cells of the bone marrow may represent an attractive therapeutic strategy to regulate activity of serine proteases in inflammatory and immunologic conditions. A variety of CatC inhibitors have been developed both by pharmaceutical companies and academic investigators, some of which are currently being employed and evaluated in preclinical/clinical trials.
Copyright © 2018 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Cathepsin C; Elastase; Inflammatory/autoimmune diseases; Papillon-Lefèvre syndrome; Pharmacological targeting; Proteinase 3; Serine proteases; Therapeutic inhibitors

Mesh:

Substances:

Year:  2018        PMID: 29842917     DOI: 10.1016/j.pharmthera.2018.05.011

Source DB:  PubMed          Journal:  Pharmacol Ther        ISSN: 0163-7258            Impact factor:   12.310


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