Abstract
Psoriatic arthritis (PsA) is a chronic inflammatory arthritis associated with psoriasis. A third of psoriatic patients develop PsA via unknown mechanisms. No reliable diagnostic markers are available for PsA, or prognostic biomarkers for PsA development in psoriasis. We previously uncovered a pro-inflammatory role for cathelicidin LL37 in lesional psoriasis skin. LL37 binds nucleic acids and stimulates plasmacytoid/myeloid dendritic cells (pDC, mDCs) to secrete type I interferon (IFN-I) and pro-inflammatory factors. LL37 becomes an autoantigen for psoriatic Th1-Th17/CD8 T cells. Anti-LL37 antibodies were detected in systemic lupus erythematosus, an autoimmune disease characterized by neutrophil-extracellular-traps release (NETosis) in target organs. LL37 can be substrate of irreversible post-translational modifications, citrullination or carbamylation, linked to neutrophil activity. Here we analyzed inflammatory factors, included LL37, in PsA and psoriasis plasma and PsA synovial fluids (SF)/biopsies. We show that LL37 (as a product of infiltrating neutrophils) and autoantibodies to LL37 are elevated in PsA, but not OA SF. Anti-LL37 antibodies correlate with clinical inflammatory markers. Anti-carbamylated/citrullinated-LL37 antibodies are present in PsA SF/plasma and, at lower extent, in psoriasis plasma, but not in controls. Plasma anti-carbamylated-LL37 antibodies correlate with PsA (DAS44) but not psoriasis (PASI) disease activity. Ectopic lymphoid structures, and deposition of immunoglobulin-(Ig)G-complexes (IC) co-localizing with infiltrating neutrophils, are observed in PsA and not OA synovial tissues (ST). Activated complement (C5a, C9), GM-CSF and IFN-I are up-regulated in PsA and not OA synovia and in PsA and psoriasis plasma but not in HD. C9 and GM-CSF levels in PsA SF correlate with clinical inflammatory markers and DAS44 (C9) and with anti-carbamylated/citrullinated-LL37 antibodies (GM-CSF and IFN-I). Thus, we uncover a role for LL37 as a novel PsA autoantibody target and correlation studies suggest participation of anti-LL37 antibodies to PsA pathogenesis. Notably, plasma antibodies to carbamylated-LL37, which correlate with DAS44, suggest their use as new disease activity markers. GM-CSF and complement C5a and C9 elevation may be responsible for autoantigens release by neutrophils and their modification, fueling inflammation and autoreactivity establishment. Finally, targeting GM-CSF, C5a, C9 can be beneficial in PsA.
Highlights
Psoriasis is a systemic inflammatory and autoimmune skin disease of unclear etiology affecting 1–3% of individuals worldwide [1]
In order to investigate the putative role of LL37 in Psoriatic arthritis (PsA), we firstly analyzed whether LL37 was measurable in the synovial compartments
The antibody levels did not reach a statistical significance between PsA and OA synovial fluids (SF), p = 0.28, by setting a cut-off we found that autoantibodies to LL37 were present in 7 out of 19 PsA SF (37%) (Figure 2)
Summary
Psoriasis is a systemic inflammatory and autoimmune skin disease of unclear etiology affecting 1–3% of individuals worldwide [1]. Neutrophils can infiltrate psoriatic skin [17], and a study suggests that NETosis is possibly occurring in skin lesions [18], whether LL37 becomes the target of autoantibodies in psoriasis patients has not been investigated. Whether and how LL37 plays a role as autoantigen in PsA is still unknown In this picture, with the idea to: [1] identify the pathogenic players in PsA, [2] discriminate the immunological pathways that are in common or are distinct between psoriasis and PsA, and [3] identify new disease activity markers for PsA, we have investigated the presence of LL37 and related autoantibodies in PsA and psoriasis patients and analyzed their correlations with clinical parameters and inflammatory factors
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