Author: Conway, Edward M.; Pryzdial, Edward L.G.
Title: Is the COVIDâ€19 thrombotic catastrophe complementâ€connected? Cord-id: wq7c4jsw Document date: 2020_8_6
ID: wq7c4jsw
Snippet: In December 2019, the world was introduced to a new betacoronavirus, referred to as severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) for its propensity to cause rapidly progressive lung damage, resulting in high death rates. As fast as the virus spread, it became evident that COVIDâ€19 is a multiâ€system disease, that may involve multiple organs, and has a high risk of thrombosis, associated with striking elevations in proâ€inflammatory cytokines, Dâ€dimer and fibrinogen, but
Document: In December 2019, the world was introduced to a new betacoronavirus, referred to as severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) for its propensity to cause rapidly progressive lung damage, resulting in high death rates. As fast as the virus spread, it became evident that COVIDâ€19 is a multiâ€system disease, that may involve multiple organs, and has a high risk of thrombosis, associated with striking elevations in proâ€inflammatory cytokines, Dâ€dimer and fibrinogen, but without disseminated intravascular coagulation. Postmortem studies have confirmed the high incidence of venous thromboembolism (VTE), but also notably revealed diffuse microvascular thrombi with endothelial swelling, consistent with a thrombotic microangiopathy (TMA), and interâ€alveolar endothelial deposits of complement activation fragments. The clinicopathologic presentation of COVIDâ€19 thus parallels that of other thrombotic diseases, such as atypical hemolytic uremic syndrome (aHUS), that are caused by dysregulation of the complement system. This raises the specter that many of the thrombotic complications arising from SARSâ€CoVâ€2 infections may be triggered and/or exacerbated by excess complement activation. This is of major potential clinical relevance, as currently available antiâ€complement therapies that are highly effective in protecting against thrombosis in aHUS, could be efficacious in COVIDâ€19. In this review, we provide mounting evidence for complement participating in the pathophysiology underlying the thrombotic diathesis associated with pathogenic coronaviruses, including SARSâ€CoVâ€2. Based on current knowledge of complement, coagulation and the virus, we suggest lines of study to identify novel therapeutic targets and the rationale for clinical trials with currently available antiâ€complement agents for COVIDâ€19.
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