Papillon-Lefèvre syndrome patient reveals species-dependent requirements for neutrophil defenses
Ole E. Sørensen, … , Finn Cilius Nielsen, Niels Borregaard
Ole E. Sørensen, … , Finn Cilius Nielsen, Niels Borregaard
Published September 17, 2014
Citation Information: J Clin Invest. 2014;124(10):4539-4548. https://doi.org/10.1172/JCI76009.
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Research Article

Papillon-Lefèvre syndrome patient reveals species-dependent requirements for neutrophil defenses

Abstract

Papillon-Lefèvre syndrome (PLS) results from mutations that inactivate cysteine protease cathepsin C (CTSC), which processes a variety of serine proteases considered essential for antimicrobial defense. Despite serine protease–deficient immune cell populations, PLS patients do not exhibit marked immunodeficiency. Here, we characterized a 24-year-old woman who had suffered from severe juvenile periodontal disease, but was otherwise healthy, and identified a homozygous missense mutation in CTSC indicative of PLS. Proteome analysis of patient neutrophil granules revealed that several proteins that normally localize to azurophil granules, including the major serine proteases, elastase, cathepsin G, and proteinase 3, were absent. Accordingly, neutrophils from this patient were incapable of producing neutrophil extracellular traps (NETs) in response to ROS and were unable to process endogenous cathelicidin hCAP-18 into the antibacterial peptide LL-37 in response to ionomycin. In immature myeloid cells from patient bone marrow, biosynthesis of CTSC and neutrophil serine proteases appeared normal along with initial processing and sorting to cellular storage. In contrast, these proteins were completely absent in mature neutrophils, indicating that CTSC mutation promotes protease degradation in more mature hematopoietic subsets, but does not affect protease production in progenitor cells. Together, these data indicate CTSC protects serine proteases from degradation in mature immune cells and suggest that neutrophil serine proteases are dispensable for human immunoprotection.

Authors

Ole E. Sørensen, Stine N. Clemmensen, Sara L. Dahl, Ole Østergaard, Niels H. Heegaard, Andreas Glenthøj, Finn Cilius Nielsen, Niels Borregaard

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Figure 1

Deficiency of cathepsin C and serine proteases in PLS neutrophils.

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Deficiency of cathepsin C and serine proteases in PLS neutrophils. (A) C...
(A) Coommassie-stained 4%–12% SDS-PAGE–separated proteins from isolated azurophil granules (α), specific granules (β1), gelatinase granules (β2), and light membranes (γ) from PLS neutrophils and neutrophils from a normal control. Molecular weight (MW) standards are indicated with black arrows: from top, 225; 102; 76; 52; 38; 31; 24; 17; 12 kDa. Selected proteins are indicated by white arrows. SP, serine proteases; Lys, lysozyme; Def, defensins; LF, lactoferrin; Gela, gelatinase. (BF) Western blotting for proteases of the isolated fractions α, β1, β2, and γ and of the postnuclear supernatant (S1), which is the material loaded onto the density gradient. (B) CTSC and lysozyme (Lyso); (C) NE and lysozyme; (D) defensin (control and patient samples were run on 2 separate gels that had a slightly curved run); (E) CTSG and lysozyme; (F) PR3 and lysozyme. Blotting was done first for serine proteases. The blots were then stripped and reprobed with antibody against lysozyme as a loading control.