Cathepsin S: therapeutic, diagnostic, and prognostic potential

Wilkinson, Richard D.; Williams, Richard V.; Scott, Christopher J.; Burden, Roberta E.

doi:10.1515/hsz-2015-0114

Cited by 160 publications

(136 citation statements)

References 124 publications

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“…Hence active NSPs together with CatC can be secreted to fulfill additional extracellular functions in peripheral tissues. Our view is consistent with previous observations on neutrophils (20,39) and monoblastic U937 cells (1) and with ongoing clinical trials that evaluate the potential of CatS inhibitors in patients with psoriasis or rheumatoid arthritis (40).…”

Section: Discussionsupporting

confidence: 93%

Neutrophilic Cathepsin C Is Maturated by a Multistep Proteolytic Process and Secreted by Activated Cells during Inflammatory Lung Diseases

Hamon

Łęgowska

Hervé

et al. 2016

Journal of Biological Chemistry

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The cysteine protease cathepsin C (CatC) activates granuleassociated proinflammatory serine proteases in hematopoietic precursor cells. Its early inhibition in the bone marrow is regarded as a new therapeutic strategy for treating proteolysisdriven chronic inflammatory diseases, but its complete inhibition is elusive in vivo. Controlling the activity of CatC may be achieved by directly inhibiting its activity with a specific inhibitor or/and by preventing its maturation. We have investigated immunochemically and kinetically the occurrence of CatC and its proform in human hematopoietic precursor cells and in differentiated mature immune cells in lung secretions. The maturation of proCatC obeys a multistep mechanism that can be entirely managed by CatS in neutrophilic precursor cells. CatS inhibition by a cell-permeable inhibitor abrogated the release of the heavy and light chains from proCatC and blocked ϳ80% of CatC activity. Under these conditions the activity of neutrophil serine proteases, however, was not abolished in precursor cell cultures. In patients with neutrophilic lung inflammation, mature CatC is found in large amounts in sputa. It is secreted by activated neutrophils as confirmed through lipopolysaccharide administration in a nonhuman primate model. CatS inhibitors currently in clinical trials are expected to decrease the activity of neutrophilic CatC without affecting those of elastase-like serine proteases.

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Section: Discussionsupporting

confidence: 93%

Neutrophilic Cathepsin C Is Maturated by a Multistep Proteolytic Process and Secreted by Activated Cells during Inflammatory Lung Diseases

Hamon

Łęgowska

Hervé

et al. 2016

Journal of Biological Chemistry

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“…Pro-CatC maturation is mainly controlled by cysteine proteases, with cathepsin S (CatS) being a major actor in human neutrophil precursors cells (Hamon et al, 2016). Several CatS inhibitors were recently developed and are currently in clinical trials (Wilkinson et al, 2015). The combination of CatS and CatC inhibitors should not only reduce the NSP burden within neutrophils, but it should also impair cell recruitment at inflammatory sites.…”

Section: Indirect Targeting Of Proteinase 3 In Diseasesmentioning

confidence: 99%

Inhibitors and Antibody Fragments as Potential Anti-Inflammatory Therapeutics Targeting Neutrophil Proteinase 3 in Human Disease

Korkmaz¹,

Lesner²,

Guarino³

et al. 2016

Pharmacol Rev

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Proteinase 3 (PR3) has received great scientific attention after its identification as the essential antigenic target of antineutrophil cytoplasm antibodies in Wegener's granulomatosis (now called granulomatosis with polyangiitis). Despite many structural and functional similarities between neutrophil elastase (NE) and PR3 during biosynthesis, storage, and extracellular release, unique properties and pathobiological functions have emerged from detailed studies in recent years. The development of highly sensitive substrates and inhibitors of human PR3 and the creation of PR3-selective single knockout mice led to the identification of nonredundant roles of PR3 in cell death induction via procaspase-3 activation in cell cultures and in mouse models. According to a study in knockout mice, PR3 shortens the lifespan of infiltrating neutrophils in tissues and accelerates the clearance of aged neutrophils in mice. Membrane exposure of active human PR3 on apoptotic neutrophils reprograms the response of macrophages to phagocytosed neutrophils, triggers secretion of proinflammatory cytokines, and undermines immune silencing and tissue regeneration. PR3-induced disruption of the anti-inflammatory effect of efferocytosis may be relevant for not only granulomatosis with polyangiitis but also for other autoimmune diseases with high neutrophil turnover. Inhibition of membrane-bound PR3 by endogenous inhibitors such as the alpha-1-protease inhibitor is comparatively weaker than that of NE, suggesting that the adverse effects of unopposed PR3 activity resurface earlier than those of NE in individuals with alpha-1-protease inhibitor deficiency. Effective coverage of PR3 by anti-inflammatory tools and simultaneous inhibition of both PR3 and NE should be most promising in the future

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“…One member of this family, cathepsin S, has been implicated in the pathogenesis of a range of disease states. 6 Cathepsin S contributes to protein degradation in the endosomal/lysosomal pathway, including proteolytic degradation of the li chaperone protein, which allows peptide antigens to bind to MHC class 2 molecules and be presented to T lymphocytes. In addition to its well defined role in the adaptive immune response, cathepsin S can also be secreted.…”

mentioning

confidence: 99%

“…Cathepsin S enzymatic activity operates across a relatively wide range of pH values, which enables activity in acidic endosomes as well as the more neutral conditions of the extracellular space, in which it can cleave substrates, such as elastin, E-cadherin, secretory leukoprotease inhibitor, junctional adhesion molecule-B, and PAR-2. 6 One distinct feature of cathepsin S is that its expression is largely restricted to leukocyte subsets, particularly macrophages, although cathepsin S expression can be induced in a variety of nonleukocyte cell types. Experimental studies using cathepsin S gene-deficient mice or cathepsin S inhibitors have defined a role for this enzyme in autoimmune diseases, atherosclerosis, airway hyper-responsiveness, cancer metastasis, neovascularization, and neuropathic pain.…”

mentioning

confidence: 99%

“…Experimental studies using cathepsin S gene-deficient mice or cathepsin S inhibitors have defined a role for this enzyme in autoimmune diseases, atherosclerosis, airway hyper-responsiveness, cancer metastasis, neovascularization, and neuropathic pain. 6 In addition, elevated serum levels of cathepsin S have been described in a number of diseases and correlate with insulin resistance, diabetes, atherosclerosis, and heart disease. 7,8 The study by Kumar et al 5 proposes that macrophagederived cathepsin S induces endothelial cell damage by activation of PAR-2 on the endothelial cell surface.…”

mentioning

confidence: 99%

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Cathepsin S–Dependent Protease–Activated Receptor-2 Activation: A New Mechanism of Endothelial Dysfunction

Nikolic-Paterson

2015

JASN

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Cathepsin S: therapeutic, diagnostic, and prognostic potential

Cited by 160 publications

References 124 publications

Neutrophilic Cathepsin C Is Maturated by a Multistep Proteolytic Process and Secreted by Activated Cells during Inflammatory Lung Diseases

Neutrophilic Cathepsin C Is Maturated by a Multistep Proteolytic Process and Secreted by Activated Cells during Inflammatory Lung Diseases

Inhibitors and Antibody Fragments as Potential Anti-Inflammatory Therapeutics Targeting Neutrophil Proteinase 3 in Human Disease

Cathepsin S–Dependent Protease–Activated Receptor-2 Activation: A New Mechanism of Endothelial Dysfunction

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