The complement system in COVID-19

Open Access
Authors
  • E.H.T. Lim
Supervisors
Cosupervisors
  • M.C. Brouwer
  • S. de Bruin
Award date 31-05-2024
Number of pages 219
Organisations
  • Faculty of Medicine (AMC-UvA)
Abstract
In this thesis, complement activation in COVID-19 was described and the effect of targeting complement factor C5a with the monoclonal antibody vilobelimab in severely and critically ill COVID-19 patients. The aim was to determine the effect of vilobelimab on mortality and safety in critically ill COVID-19 patients, to assess its effects on biomarkers of inflammation and coagulation in severely and critically ill COVID-19 patients, and to analyse its pharmacokinetics. In this thesis, it was shown that vilobelimab improved survival in critically ill, mechanically ventilated COVID-19 patients. Vilobelimab was found to efficiently inhibit C5a in severely and critically ill COVID-19 patients, without evidence of immunogenicity in critically ill COVID-19 patients. Finally, vilobelimab was shown to decrease the inflammatory response by lowering concentrations of CXCL8 over time. Further research should investigate whether different subphenotypes in COVID-19 respond differently to vilobelimab treatment and focus on the role of C5a and C5a inhibition in other viral infections that lead to ARDS.
Document type PhD thesis
Language English
Downloads
Thesis (complete) (Embargo up to 2026-05-31)
Chapter 7: Regional comparison of efficacy and safety for vilobelimab in critically ill, invasively mechanically ventilated COVID-19 patients (Embargo up to 2026-05-31)
Chapter 8: Vilobelimab reduces CXCL8 in critically ill COVID-19 patients: A substudy of the phase 3 PANAMO trial (Embargo up to 2026-05-31)
Supplementary materials
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