Medicine

Psoriasis Drugs May Help Treat Metabolic Liver Disease in Patients

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This prospective study examined 35 adults with psoriatic disease and found that IL-17 inhibitor biologics, but not TNF inhibitors, were associated with improvements in liver fat content and disease activity markers over approximately 6 months. Using MRI imaging and immune cell profiling, researchers identified specific T-cell populations that were linked to baseline liver disease severity and treatment response. The findings suggest that certain biologic therapies for psoriatic disease may have differential effects on concurrent metabolic liver disease.


This research could inform treatment selection for patients with both psoriatic disease and fatty liver disease, a common comorbidity. The identification of immune signatures predicting liver response may eventually enable personalized medicine approaches, helping clinicians choose therapies that address both skin/joint and liver manifestations simultaneously.


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⚠️ Preprint – Noch nicht peer-reviewed

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Psoriatic disease (PsD) is associated with metabolic dysfunction-associated steatotic liver disease (MASLD), but the hepatic effects of biologic therapies are unclear. We evaluated paired liver MRI and multi-modal immunoprofiling in PsD patients initiating new systemic therapy. COLIPSO is a prospective cohort of adults with moderate-to-severe psoriasis or psoriatic arthritis (PsA) starting a new conventional synthetic or biologic disease-modifying antirheumatic drug (DMARD). Liver MRI was performed at baseline and ~6 months. A subset of participants with PsA underwent peripheral blood flow cytometry and single-cell RNA sequencing (scRNAseq). Primary outcomes were within-subject change in quantitative MRI measures of liver disease activity and fat content (iron-corrected T1 [cT1] and proton density fat fraction [PDFF]). Bayesian models were used. Thirty-five participants (mean age 50 +/- 13 years; 61% male) were followed for ~29 weeks. Baseline disease activity was moderate (mean DAPSA 29) and 40% had MASLD. IL 17 inhibitors (IL-17i) improved PDFF (-1.58 +/- 1.61%) and cT1(-43.6 +/- 52.7ms), whereas TNFi showed little change. Compared with csDMARD, IL 17i improved PDFF (probability of direction [pd] 89%) and cT1 (pd 93%), which was not seen with TNFi. Flow cytometry (n=17) linked baseline gamma delta T-cell and ThGM-CSF T-cell abundance with cT1 and PDFF. scRNAseq highlighted baseline transcriptomic signatures in MAIT cells associated with cT1 and PDFF. Naive T-cell RNA signatures at baseline were associated with MRI improvements. In PsD, only IL-17i were associated with improved liver disease in addition to improving clinical PsD outcomes. T-cell subtypes bridging innate and adaptive immunity were associated with liver disease features.

Source: Impact of disease-modifying therapies in adults with concomitant psoriatic and metabolic liver disease with integrated immunoprofiling