Risk of Paradoxical Eczema in Patients Receiving Biologics for Psoriasis

JAMA Dermatology
Open Access

Clinical Summary

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What was studied

A prospective cohort from the UK/Ireland BADBIR registry evaluated adults with plaque psoriasis treated with biologics (TNF, IL-17, IL‑12/23, IL‑23) between 2007 and 2022 to compare paradoxical eczema risk. The analysis included 24,997 drug exposures from 13,699 participants over 81,441 patient-years using propensity score–weighted Cox models.

Key findings

Paradoxical eczema occurred in 273 exposures (1%). Adjusted incidence rates were 1.22, 0.94, 0.80, and 0.56 per 100,000 person-years for IL‑17, TNF, IL‑12/23, and IL‑23 inhibitors, respectively; versus TNF, IL‑23 inhibitors had lower risk (HR 0.39; 95% CI 0.19‑0.81), while IL‑17 (HR 1.03; 0.74‑1.42) and IL‑12/23 (HR 0.87; 0.66‑1.16) showed no difference. Higher risk was associated with increasing age (HR 1.02 per year; 1.01‑1.03), prior atopic dermatitis (HR 12.40; 6.97‑22.06) or hay fever (HR 3.78; 1.49‑9.53); males had lower risk (HR 0.60; 0.45‑0.78).

Clinical implications

Paradoxical eczema was rare in biologic-treated psoriasis, with the lowest observed risk on IL‑23 inhibitors. Screen for personal history of atopic dermatitis or hay fever and consider age and sex when counseling about this risk.