Altered fibrin clot structure contributes to thrombosis risk in severe COVID-19

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Wygrecka, Malgorzata | Birnhuber, Anna | Seeliger, Benjamin | Michalick, Laura | Pak, Oleg | Schultz, Astrid-Solveig | Schramm, Fabian | Zacharias, Martin | Gorkiewicz, Gregor | David, Sascha | Welte, Tobias | Schmidt, Julius | Weissmann, Norbert | Schermuly, Ralph | Barreto, Guillermo | Schaefer, Liliana | Markart, Philipp | Brack, Markus | Hippenstiel, Stefan | Kurth, Florian | Sander, Leif | Witzenrath, Martin | Kuebler, Wolfgang | Kwapiszewska, Grazyna | Preissner, Klaus

Edité par CCSD -

Abstract The high incidence of thrombotic events suggests a possible role of the contact system pathway in COVID-19 pathology. Here, we demonstrate altered levels of factor XII (FXII) and its activation products in two independent cohorts of critically ill COVID-19 patients in comparison to patients suffering from severe acute respiratory distress syndrome due to influenza virus (ARDS-influenza). Compatible with this data, we report rapid consumption of FXII in COVID-19, but not in ARDS-influenza, plasma. Interestingly, the kaolin clotting time was not prolonged in COVID-19 as compared to ARDS-influenza. Using confocal and electron microscopy, we show that increased FXII activation rate, in conjunction with elevated fibrinogen levels, triggers formation of fibrinolysis-resistant, compact clots with thin fibers and small pores in COVID-19. Accordingly, we observed clot lysis in 30% of COVID-19 patients and 84% of ARDS-influenza subjects. Analysis of lung tissue sections revealed wide-spread extra- and intra-vascular compact fibrin deposits in COVID-19. Together, our results indicate that elevated fibrinogen levels and increased FXII activation rate promote thrombosis and thrombolysis resistance via enhanced thrombus formation and stability in COVID-19.

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