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Herring roe oil reduces inflammatory biomarkers in mild-to-moderate psoriasis

Herring roe oil reduces inflammatory biomarkers in mild-to-moderate psoriasis
Photo by Natallia Photo / Unsplash
Key Takeaway
Consider baseline SII for stratification; HRO-associated biomarker changes are exploratory and not causal.

This post hoc analysis of a randomized controlled trial evaluated oral herring roe oil (HRO) supplementation versus placebo over 26 weeks in 64 patients with mild-to-moderate psoriasis; biomarker analyses included 60 participants. The study did not report a primary outcome or whether randomization and blinding procedures were used.

At week 26, HRO was associated with significant mean reductions compared with placebo in the systemic immune-inflammation index (SII), the systemic inflammation response index (SIRI), and the platelet-to-lymphocyte ratio (PLR). PASI50 response rates at week 26 were statistically significant in the HRO arm among patients with lower baseline SII. No absolute numbers, effect sizes, p-values, or confidence intervals were reported.

Safety and tolerability were not reported; there were no data on adverse events, serious adverse events, or study discontinuations.

Key limitations include the exploratory post hoc design, exclusion of patients missing baseline complete blood counts, lack of a prespecified primary outcome, and uncertainty about randomization and blinding. Causality is not established. In practice, baseline SII may help predict treatment response and could be useful for stratification in future trials in mild-to-moderate psoriasis.

Study Details

Study typeRct
Sample sizen = 64
EvidenceLevel 2
PublishedApr 2026
View Original Abstract ↓
Background: Psoriasis is a chronic immune-mediated inflammatory disease (IMID) with systemic involvement. In mild-to-moderate disease, circulating cytokines may inadequately capture systemic inflammatory burden. Composite haematological indices derived from complete blood counts, such as the systemic immune-inflammation index (SII) and systemic inflammation response index (SIRI), have emerged as sensitive prognostic markers of systemic inflammation, including in psoriasis. This exploratory post hoc analysis investigated the effects of orally administered herring roe oil (HRO), a phospholipid-rich marine oil, on systemic inflammation in patients with mild-to-moderate psoriasis utilizing these biomarkers. Methods: Data were analysed from a randomized, double-blind, placebo-controlled 26-week clinical study which investigated HRO supplementation in patients (N = 64) with mild-to-moderate psoriasis (NCT03359577). SII, SIRI, neutrophil-to-lymphocyte ratio (NLR), platelet-to-lymphocyte ratio (PLR), and monocyte-to-lymphocyte ratio (MLR) were calculated at baseline, week 12, and week 26 for patients where baseline complete blood counts (CBCs) were available (n = 60). Patients missing baseline CBCs were excluded from the analysis. Continuous changes were assessed using ANCOVA with baseline adjustment. Categorical responder analyses were performed with 25% and 30% reduction thresholds and stratification by baseline biomarker medians were performed to evaluate treatment responses and impact of baseline inflammation. Results: Compared with placebo, HRO treatment resulted in significant mean reductions in SII, SIRI, and PLR at week 26, with supportive trends and responder effects observed as early as week 12 compared to placebo. Patients with elevated baseline inflammatory indices showed the greatest reductions in systemic inflammation. Stratification by baseline SII further revealed enhanced clinical benefit, with statistically significant PASI50 response rates in the HRO arm at week 26 among patients with lower baseline SII. Conclusion: HRO supplementation was associated with a time-dependent reduction in systemic inflammatory biomarkers in mild-to-moderate psoriasis patients. These findings support the utility of composite inflammatory indices for monitoring systemic inflammation and suggest that baseline SII may have utility in predicting treatment response and may be a useful tool for stratification in clinical trials in mild to moderate psoriasis patients. These results could also suggest platform-potential of HRO for resolution-oriented interventions across several inflammatory conditions.
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