Coagulation factor V is a T-cell inhibitor expressed by leukocytes in COVID-19

Wang, Jun; Kotagiri, Prasanti; Lyons, Paul A; Al-Lamki, Rafia S; Mescia, Federica; Bergamaschi, Laura; Turner, Lorinda; Morgan, Michael D; Calero-Nieto, Fernando J; Bach, Karsten; Mende, Nicole; Wilson, Nicola K; Watts, Emily R; Maxwell, Patrick H; Chinnery, Patrick F; Kingston, Nathalie; Papadia, Sofia; Stirrups, Kathleen E; Walker, Neil; Gupta, Ravindra K; Menon, David K; Allinson, Kieren; Aitken, Sarah J; Toshner, Mark; Weekes, Michael P; Nathan, James A; Walmsley, Sarah R; Ouwehand, Willem H; Kasanicki, Mary; Göttgens, Berthold; Marioni, John C; Smith, Kenneth G C; Pober, Jordan S; Bradley, John R

doi:10.1016/j.isci.2022.103971

Clotting Factor V (FV) is primarily synthesized in the liver and when cleaved by thrombin forms pro-coagulant Factor Va (FVa). Using whole blood RNAseq and scRNAseq of peripheral blood mononuclear cells, we find that FV mRNA is expressed in leukocytes, and identify neutrophils, monocytes, and T regulatory cells as sources of increased FV in hospitalized patients with COVID-19. Proteomic analysis confirms increased FV in circulating neutrophils in severe COVID-19, and immunofluorescence microscopy identifies FV in lung-infiltrating leukocytes in COVID-19 lung disease. Increased leukocyte FV expression in severe disease correlates with T-cell lymphopenia. Both plasma-derived and a cleavage resistant recombinant FV, but not thrombin cleaved FVa, suppress T-cell proliferation in vitro. Anticoagulants that reduce FV conversion to FVa, including heparin, may have the unintended consequence of suppressing the adaptive immune system.