Borek et al. Rare Dis Orphan Drugs J 2023;2:5  https://dx.doi.org/10.20517/rdodj.2022.20  Page 9 of 14

               central regulators of many biological processes that are necessary for tissue homeostasis. This complexity
               requires a delicate balance between targeting serine proteases to achieve therapeutic benefits while avoiding
               disruption to normal tissue function. It is important to note that broad-spectrum inhibition of serine
               proteases can be detrimental, as demonstrated by Aprotinin, the administration of which significantly
               increases the risk of end-organ damage and death . For safety reasons, a more refined, targeted approach
                                                         [120]
               needs to be favored. Elafin (NE and PR3 inhibitor) is currently being investigated in a phase 1 clinical trial
               for the treatment of PAH (ClinicalTrials.gov Identifier: NCT03522935). Cathepsin C (CtsC) makes another
               interesting target for modulating serine-proteases-mediated tissue damage and inflammation, as it is an
               upstream activator of NSPs, tryptase, chymase, and granzymes. Brensocatib, a CtsC inhibitor, has recently
                                                                                              [121]
               been confirmed as safe and effective in phase 2 clinical trials involving bronchiectasis patients . Given the
               strong implication of neutrophil and MC serine proteases in the development of PAH, targeting CtsC to
               reduce proteolytic activity in the tissue - by preventing the conversion of zymogens to active enzymes  -
                                                                                                       [45]
               emerges as a potential therapy to treat PAH. Genetic inactivation of CtsC in humans leads to Papillon-Lefè
               vre syndrome (PLS, OMIM: 245000), an autosomal recessive disorder in which NSP activity is minimal or
                     [122]
               absent . Because the clinical consequences of this disorder are mild, small molecule inhibitors targeting
               CtsC activity are considered safe and represent an attractive therapeutic strategy to modulate NSP-mediated
               tissue damage and inflammation. However, given that neutrophil NSPs and MC serine proteases have a
               broad range of targets and affect various aspects of inflammation and tissue damage, inhibiting their activity
               could have immunomodulatory and anti-remodeling effects not only in PAH but also in many other
               diseases.


               DECLARATIONS
               Authors’ contributions
               Wrote and edited the manuscript: Borek I
               Provided a critical review of the manuscript: Kwapiszewska G

               Availability of data and materials
               Not applicable.


               Financial support and sponsorship
               None.


               Conflicts of interest
               Both authors declared that there are no conflicts of interest.


               Ethical approval and consent to participate
               Not applicable.


               Consent for publication
               Not applicable.


               Copyright
               © The Authors 2023.

               REFERENCES
               1.       Simonneau G, Montani D, Celermajer DS, et al. Haemodynamic definitions and updated clinical classification of pulmonary
                    hypertension. Eur Respir J 2019;53:1801913.  DOI  PubMed  PMC
               2.       Chang KY, Duval S, Badesch DB, et al; PHAR Investigators*. Mortality in pulmonary arterial hypertension in the modern era: early
                    insights from the Pulmonary Hypertension Association Registry. J Am Heart Assoc 2022;11:e024969.  DOI  PubMed  PMC