Background: The CIAO trial recently demonstrated a probable clinical benefit of omalizumab in the treatment of severe COVID-19; however, the mechanism underlying this benefit remains unclear. Therefore, we sought to longitudinally assess the impact of omalizumab on serum cytokines in CIAO trial patients to determine its mechanism of action.
Methods: Blood samples were collected on days 0, 2, 7, and 14 from patients recruited into the CIAO trial and who consented to this substudy. Blood samples were tested by a panel of 25 inflammatory cytokines, as well as for markers of mast cell activation. Levels of inflammatory biomarkers were compared over time between omalizumab- and placebo-treated patients by generalized linear mixed-effects model. Associations between biomarkers and clinical outcomes were investigated by mixed-effects logistic regression.
Results: Nineteen patients were recruited into this substudy; 10 were assigned to placebo and 9 to omalizumab. Monokine induced by gamma interferon was significantly positively associated with severe COVID-19 (Odds Ratio [OR] = 1.06, 95%CI = 1.00-1.11, p = 0.043). Further, omalizumab significantly reduced interleukin-15 (Coefficient = -0.95, p = 0.048) and macrophage inflammatory protein-1 (Coefficient = -1.31, p = 0.010) levels. However, neither was significant in analyses adjusting for multiple hypothesis testing.
Conclusion: Although limited by a small sample size, these results suggest that omalizumab's potential benefit in COVID-19 may be mediated independently of modulation of the measured serum biomarkers. Further studies are needed to investigate omalizumab's mechanism of action in COVID-19.
Keywords: COVID-19; clinical trial; coronavirus; cytokine; omalizumab.
Copyright © 2024 Prosty, Le, Lu, Khoury, Cormier, Cheng, Fowler, Murthy, Tsang, Lejtenyi, Ben-Shoshan, Rahme, Golchi, Dendukuri, Lee and Netchiporouk.