A Systemic Immune-State Axis Distinguishes Psoriatic Arthritis from Psoriasis
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Abstract
Psoriasis and psoriatic arthritis (PsA) are systemic immune-mediated diseases, but the features that distinguish cutaneous-dominant psoriasis from musculoskeletal involvement remain unclear. We analyzed four core public cross-sectional datasets spanning whole-blood methylation, PBMC single-cell RNA sequencing summarized at the subject level, skin RNA sequencing, and purified CD4+ T-cell methylation, and used two additional public skin cohorts for external contextual checks to define an inflammatory disease axis (DIR) and a contrast-resolved systemic-state coordinate (CRS) representing additional systemic immune-state variation associated with PsA. In whole-blood methylation, DIR primarily separated healthy controls from psoriasis, whereas CRS separated psoriasis from PsA with minimal correlation to DIR. In PBMC single-cell data, CRS was higher in PsA and in the source-defined PSX subgroup (joint pain without CASPAR-classified PsA) than in PsO. Cell-type-resolved analyses localized CRS-related shifts to CD8 naive T cells, NK cells, CD14 monocytes, and regulatory T cells and identified multicompartment pathway-state remodeling along the CRS continuum. In contrast, skin RNA sequencing mainly captured lesional inflammatory burden and showed only limited additional PsA-related separation within the same tissue state. These findings support a model in which PsA is distinguished from psoriasis by an additional systemic immune-state axis rather than by skin inflammatory burden alone.
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- europepmc
- last seen: 2026-05-20T01:45:00.602351+00:00