Author: Henry, Brandon Michael; Szergyuk, Ivan; de Oliveira, Maria Helena Santos; Lippi, Giuseppe; Benoit, Justin L.; Vikse, Jens; Benoit, Stefanie W.
Title: Complement levels at admission as a reflection of coronavirus disease 2019 (COVIDâ€19) severity state Cord-id: qrcz7yzq Document date: 2021_5_19
ID: qrcz7yzq
Snippet: Complement system hyperactivation has been proposed as a potential driver of adverse outcomes in severe acute respiratory syndrome coronavirus 2 infected patients, given prior research of complement deposits found in tissue and blood samples, as well as evidence of clinical improvement with anticomplement therapy. Its role in augmenting thrombotic microangiopathy mediated organ damage has also been implicated in coronavirus disease 2019 (COVIDâ€19). This study aimed to examine associations betw
Document: Complement system hyperactivation has been proposed as a potential driver of adverse outcomes in severe acute respiratory syndrome coronavirus 2 infected patients, given prior research of complement deposits found in tissue and blood samples, as well as evidence of clinical improvement with anticomplement therapy. Its role in augmenting thrombotic microangiopathy mediated organ damage has also been implicated in coronavirus disease 2019 (COVIDâ€19). This study aimed to examine associations between complement parameters and progression to severe COVIDâ€19 illness, as well as correlations with other systems. Blood samples of COVIDâ€19 patients presenting to the emergency department (ED) were analyzed for a wide panel of complement and inflammatory biomarkers. The primary outcome was COVIDâ€19 severity at index ED visit, while the secondary outcome was peak disease severity over the course of illness. Fiftyâ€two COVIDâ€19 patients were enrolled. C3a (p = 0.018), C3a/C3 ratio (p = 0.002), and sC5bâ€9/C3 ratio (p = 0.021) were significantly elevated in with severe disease at ED presentation. Over the course of illness, C3a (p = 0.028) and C3a/C3 ratio (p = 0.003) were highest in the moderate severity group. In multivariate regression controlled for confounders, complement hyperactivation failed to predict progression to severe disease. C3a, C3a/C3 ratio, and sC5bâ€9/C3 ratio were correlated positively with numerous inflammatory biomarkers, fibrinogen, and VWF:Ag, and negatively with plasminogen and ADAMTS13 activity. We found evidence of complement hyperactivation in COVIDâ€19, associated with hyperinflammation and thrombotic microangiopathy. Complement inhibition should be further investigated for potential benefit in patients displaying a hyperinflammatory and microangiopathic phenotype.
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