Author: Hollerbach, Anne; Müllerâ€Calleja, Nadine; Pedrosa, Denise; Canisius, Antje; Sprinzl, Martin F.; Falter, Tanja; Rossmann, Heidi; Bodenstein, Marc; Werner, Christian; Sagoschen, Ingo; Münzel, Thomas; Schreiner, Oliver; Sivanathan, Visvakanth; Reuter, Michael; Niermann, Johannes; Galle, Peter R.; Teyton, Luc; Ruf, Wolfram; Lackner, Karl J.
Title: Pathogenic lipidâ€binding antiphospholipid antibodies are associated with severity of COVIDâ€19 Cord-id: y9b0o98h Document date: 2021_7_22
ID: y9b0o98h
Snippet: BACKGROUND: Coronavirus disease 19 (COVIDâ€19)–associated coagulopathy is a hallmark of disease severity and poor prognosis. The key manifestations of this prothrombotic syndrome—microvascular thrombosis, stroke, and venous and pulmonary clots—are also observed in severe and catastrophic antiphospholipid syndrome. Antiphospholipid antibodies (aPL) are detectable in COVIDâ€19 patients, but their association with the clinical course of COVIDâ€19 remains unproven. OBJECTIVES: To analyze th
Document: BACKGROUND: Coronavirus disease 19 (COVIDâ€19)–associated coagulopathy is a hallmark of disease severity and poor prognosis. The key manifestations of this prothrombotic syndrome—microvascular thrombosis, stroke, and venous and pulmonary clots—are also observed in severe and catastrophic antiphospholipid syndrome. Antiphospholipid antibodies (aPL) are detectable in COVIDâ€19 patients, but their association with the clinical course of COVIDâ€19 remains unproven. OBJECTIVES: To analyze the presence and relevance of lipidâ€binding aPL in hospitalized COVIDâ€19 patients. METHODS: Two cohorts of 53 and 121 patients from a single center hospitalized for PCRâ€proven severe acute respiratory syndrome–coronavirus 2 infection were analyzed for the presence of aPL and clinical severity of COVIDâ€19. RESULTS: We here demonstrate that lipidâ€binding aPL are common in COVIDâ€19. COVIDâ€19 patients with lipidâ€binding aPL have higher median concentrations of Câ€reactive protein and Dâ€dimer, and are more likely to have a critical clinical course and fatal outcome. Lipidâ€binding aPL isolated from COVIDâ€19 patients target the recently described cell surface complex of lysobisphosphatidic acid (LBPA) with the protein C receptor (EPCR) to induce prothrombotic and inflammatory responses in monocytes and endothelial cells. We show that B1a cells producing lipidâ€reactive aPL of the IgG isotype circulate in the blood of COVIDâ€19 patients. In vivo, COVIDâ€19 aPL accelerate thrombus formation in an experimental mouse model dependent on the recently delineated signaling pathway involving EPCRâ€LBPA. CONCLUSIONS: COVIDâ€19 patients rapidly expand B1a cells secreting pathogenic lipidâ€binding aPL with broad thrombotic and inflammatory effects. The association with markers of inflammation and coagulation, clinical severity, and mortality suggests a causal role of aPL in COVIDâ€19–associated coagulopathy.
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