Genetic liability to psoriasis predicts severe disease outcomes

  1. Jake R Saklatvala
  2. Samuel Lessard
  3. Maris Teder-Laving
  4. Laurent F Thomas
  5. Ravi Ramessur
  6. Bjørn Olav Åsvold
  7. Anne Barton
  8. David Baudry
  9. John Bowes
  10. Ben Brumpton
  11. Vinod Chandran
  12. Clément Chatelain
  13. Emanuele de Rinaldis
  14. James T Elder
  15. David Ellinghaus
  16. John Foerster
  17. Andre Franke
  18. Dafna D Gladman
  19. Wayne Gulliver
  20. Ulrike Hüffmeier
  21. Laura Huilaja
  22. Kristian Hveem
  23. Shameer Khader
  24. Külli Kingo
  25. Katherine Klinger
  26. Sulev Kõks
  27. Wilson Liao
  28. Rajan P Nair
  29. Joanne Nititham
  30. Proton Rahman
  31. André Reis
  32. Philip E Stuart
  33. Kaisa Tasanen
  34. Tanel Traks
  35. Lam C Tsoi
  36. Steffen Uebe
  37. Katie Watts
  38. BSTOP study group
  39. Jonathan N Barker
  40. Satveer K Mahil
  41. Sinéad M Langan
  42. FinnGen
  43. Estonian Biobank research team
  44. Sara J Brown
  45. Mari Løset
  46. Lavinia Paternoster
  47. Nick Dand
  48. Catherine H Smith
  49. Michael A Simpson
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Abstract

Background

Psoriasis is a common inflammatory skin disease with heterogeneous presentation. Up to 30% of individuals have severe disease with a greater surface area of skin involvement, co-morbidity burden and impact on quality of life. Prognostic biomarkers of psoriasis severity could improve allocation of clinical resources and enable earlier intervention to prevent disease progression, and a genetic biomarker would be cost-effective, stable over time, and unaffected by treatment or comorbidity.

Methods

Psoriasis severity was studied in four European population-based biobanks and classified based on level of clinical intervention received, with criteria for severe disease including hospitalisation due to psoriasis, use of systemic immunomodulating therapy or phototherapy. Common genetic variants, polygenic risk scores and traditional epidemiological risk factors were tested for association with severe psoriasis in each of the constituent biobanks and combined through meta-analysis. The distribution of psoriasis polygenic risk was also evaluated in a cohort of 4 151 participants in the UK-based severe psoriasis registry, BSTOP.

Results

In the population-based datasets, 9 738 of 44 904 individuals with psoriasis (21.7%) were classified as having severe disease. Genetic variants within the major histocompatibility complex (MHC) and the TNIP1 and IL12B psoriasis susceptibility loci were associated with severe disease at genome-wide significance (P<5.0×10 −8 ). Furthermore, a strong positive correlation was observed between psoriasis susceptibility and severity effect sizes across all psoriasis susceptibility loci. An individual’s genetic liability to psoriasis as measured with a polygenic risk score (PRS) strongly associated with disease severity, with a magnitude of effect comparable to established severity risk factors such as obesity and smoking. The top 5% of psoriasis cases by genetic liability to psoriasis were 1.23-to-2.00 times as likely than the average psoriasis case to have severe disease. Psoriasis cases in the BSTOP severe disease registry were 3.10-fold enriched for a PRS that exceeded the 95th percentile established among UK Biobank psoriasis cases.

Conclusions

The psoriasis susceptibility PRS demonstrates utility, and may be more effective than established epidemiological factors, as a stratification tool to identify those individuals that are at greatest risk of severe disease and may benefit most from early intervention.

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  1. Version published to 10.1101/2025.03.04.25323079v1 on medRxiv