Increased complement activation is a distinctive feature of severe SARS-CoV-2 infection

Lina Ma(Washington University in St. Louis), Sanjaya Kumar Sahu(Washington University in St. Louis), Marlene Cano(Washington University in St. Louis), Vasanthan Kuppuswamy(Washington University in St. Louis), Jamal Bajwa(Washington University in St. Louis), Ja’Nia McPhatter(University of Pittsburgh), Alexander B. Pine(Yale University), Matthew L. Meizlish(Yale University), George Goshua(Yale University), C‐Hong Chang(Yale University), Hanming Zhang(Yale University), Christina Price(Yale University), Parveen Bahel(Yale New Haven Health System), Henry M. Rinder(Yale New Haven Health System), Tingting Lei(Washington University in St. Louis), Aaron Day(Washington University in St. Louis), Daniel Reynolds(Washington University in St. Louis), Xiaobo Wu(Washington University in St. Louis), Rebecca E. Schriefer(Washington University in St. Louis), Adriana M. Rauseo(Washington University in St. Louis), Charles W. Goss(Washington University in St. Louis), Jane A. O’Halloran(Washington University in St. Louis), Rachel M. Presti(Washington University in St. Louis), Alfred H.J. Kim(Washington University in St. Louis), Andrew E. Gelman(Washington University in St. Louis), Charles S. Dela Cruz(Yale University), Alfred Ian Lee(Yale University), Phillip Mudd(Washington University in St. Louis), Hyung J. Chun(Yale University), John Atkinson(Washington University in St. Louis), Hrishikesh S. Kulkarni(Washington University in St. Louis)
bioRxiv (Cold Spring Harbor Laboratory)
February 23, 2021
10.1101/2021.02.22.432177
Cited by 60Open Access
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Abstract

ABSTRACT Complement activation has been implicated in the pathogenesis of severe SARS-CoV-2 infection. However, it remains to be determined whether increased complement activation is a broad indicator of critical illness (and thus, no different in COVID-19). It is also unclear which pathways are contributing to complement activation in COVID-19, and, if complement activation is associated with certain features of severe SARS-CoV-2 infection, such as endothelial injury and hypercoagulability. To address these questions, we investigated complement activation in the plasma from patients with COVID-19 prospectively enrolled at two tertiary care centers. We compared our patients to two non-COVID cohorts: (a) patients hospitalized with influenza, and (b) patients admitted to the intensive care unit (ICU) with acute respiratory failure requiring invasive mechanical ventilation (IMV). We demonstrate that circulating markers of complement activation (i.e., sC5b-9) are elevated in patients with COVID-19 compared to those with influenza and to patients with non-COVID-19 respiratory failure. Further, the results facilitate distinguishing those who are at higher risk of worse outcomes such as requiring ICU admission, or IMV. Moreover, the results indicate enhanced activation of the alternative complement pathway is most prevalent in patients with severe COVID-19 and is associated with markers of endothelial injury (i.e., Ang2) as well as hypercoagulability (i.e., thrombomodulin and von Willebrand factor). Our findings identify complement activation to be a distinctive feature of COVID-19, and provide specific targets that may be utilized for risk prognostication, drug discovery and personalized clinical trials. SUMMMARY Complement has been implicated in COVID-19. However, whether this is distinctive of COVID-19 remains unanswered. Ma et al report increased complement activation in COVID-19 compared to influenza and non-COVID respiratory failure, and demonstrate alternative pathway activation as a key marker of multiorgan failure and death.

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