Anti-SARS-CoV-2 IgG from severely ill COVID-19 patients promotes macrophage hyper-inflammatory responses

  1. Willianne Hoepel
  2. Hung-Jen Chen
  3. Sona Allahverdiyeva
  4. Xue Manz
  5. Jurjan Aman
  6. Amsterdam UMC COVID-19 Biobank
  7. Peter Bonta
  8. Philip Brouwer
  9. Steven de Taeye
  10. Tom Caniels
  11. Karlijn van der Straten
  12. Korneliusz Golebski
  13. Guillermo Griffith
  14. René Jonkers
  15. Mads Larsen
  16. Federica Linty
  17. Annette Neele
  18. Jan Nouta
  19. Frank van Baarle
  20. Cornelis van Drunen
  21. Alexander Vlaar
  22. Godelieve de Bree
  23. Rogier Sanders
  24. Lisa Willemsen
  25. Manfred Wuhrer
  26. Harm Jan Bogaard
  27. Marit van Gils
  28. Gestur Vidarsson
  29. Menno de Winther
  30. Jeroen den Dunnen
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Abstract

For yet unknown reasons, severely ill COVID-19 patients often become critically ill around the time of activation of adaptive immunity. Here, we show that anti-Spike IgG from serum of severely ill COVID-19 patients induces a hyper-inflammatory response by human macrophages, which subsequently breaks pulmonary endothelial barrier integrity and induces microvascular thrombosis. The excessive inflammatory capacity of this anti-Spike IgG is related to glycosylation changes in the IgG Fc tail. Moreover, the hyper-inflammatory response induced by anti-Spike IgG can be specifically counteracted in vitro by use of the active component of fostamatinib, an FDA- and EMA-approved therapeutic small molecule inhibitor of Syk.

One sentence summary

Anti-Spike IgG promotes hyper-inflammation.

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