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LL-37

Cathelicidin, hCAP-18, FALL-39, CAP-18

Quick Stats
Studies 2230
Trials 95
Score 1
2020 pubmed 56 citations

Current knowledge on autoantigens and autoantibodies in psoriasis.

Ten Bergen. Lisa Lynn LL; Petrovic. Aleksandra A; Aarebrot. Anders Krogh AK; Appel. Silke S

Key Findings

  • LL‑37 is identified as an autoantigen that can drive psoriasis lesions
  • Autoantibodies against LL‑37 are linked to psoriatic arthritis
  • The discovery of LL‑37 and other autoantigens opens the door for antigen‑targeted therapies

Practical Outcomes

  • For most health‑optimizers, this research doesn’t change daily practices. It suggests that measuring LL‑37 autoantibodies might help identify psoriasis or arthritis risk, but no specific supplement or dosage advice emerges from the study.

Summary

The paper explains that a protein called LL‑37 can trigger the immune system in people with psoriasis, leading to skin lesions and sometimes joint problems. Researchers have found that some patients develop antibodies against LL‑37, which may play a role in the disease and could become a target for future treatments.

Abstract

In the past decades, clinical and experimental evidence has demonstrated that psoriasis is an immune-mediated inflammatory disease of the skin that occurs in genetically susceptible individuals. Psoriasis also shows clear autoimmune pathomechanisms, but specific cellular targets for the onset and maintenance of psoriatic lesions were not established until 2014. Since then, four psoriasis autoantigens were discovered, namely cathelicidin LL-37, melanocytic ADAMTSL5, lipid antigen PLA2G4D and keratin 17. Autoreactive T cells against these autoantigens were found in a number of patients with moderate-to-severe plaque psoriasis. Moreover, the discovery of autoantibodies against LL-37 and ADAMTSL5 and their strong association with psoriatic arthritis (PsA) suggest a potential role of these autoantibodies in the pathogenesis of PsA. This review discusses the current studies on psoriatic autoantigens and the associated circulating autoantibodies and their mechanisms involved in the development and maintenance of psoriatic plaques. Recent autoimmune evidence fuelled the discussion on psoriasis as an autoimmune skin disorder and has the potential to develop new treatment strategies with protective and therapeutic antigen-targeted methods.

Study Information

Provider

pubmed

Year

2020

Date

2020-07-22T00:00:00.000Z

DOI

10.1111/sji.12945

Citations

56

References

54