C1 esterase inhibitor-mediated immunosuppression in COVID-19: Friend or foe?

Melissa A. Hausburg; Jason S. Williams; Kaysie L. Banton; Charles W. Mains; Michael Roshon; David Bar-Or

Clinical Immunology Communications (Dec 2022)

C1 esterase inhibitor-mediated immunosuppression in COVID-19: Friend or foe?

Melissa A. Hausburg,
Jason S. Williams,
Kaysie L. Banton,
Charles W. Mains,
Michael Roshon,
David Bar-Or

Affiliations

Melissa A. Hausburg: Department of Trauma Research, Swedish Medical Center, 501 E. Hampden, Englewood, CO 80113, USA; Department of Trauma Research, St. Anthony Hospital, 11600 W 2nd Pl, Lakewood, CO 80228, USA; Department of Trauma Research, Penrose Hospital, 2222 N Nevada Ave, Colorado Springs, CO 80907, USA
Jason S. Williams: Department of Trauma Research, Swedish Medical Center, 501 E. Hampden, Englewood, CO 80113, USA; Department of Trauma Research, St. Anthony Hospital, 11600 W 2nd Pl, Lakewood, CO 80228, USA; Department of Trauma Research, Penrose Hospital, 2222 N Nevada Ave, Colorado Springs, CO 80907, USA
Kaysie L. Banton: Department of Trauma Research, Swedish Medical Center, 501 E. Hampden, Englewood, CO 80113, USA
Charles W. Mains: Centura Health Trauma Systems, Centura Health, 9100 E Mineral Circle, Centennial, CO 80112, USA
Michael Roshon: Centura Health Trauma Systems, Centura Health, 9100 E Mineral Circle, Centennial, CO 80112, USA; Department of Emergency Services, Penrose Hospital, 2222 N Nevada Ave, Colorado Springs, CO 80907, USA
David Bar-Or: Department of Trauma Research, Swedish Medical Center, 501 E. Hampden, Englewood, CO 80113, USA; Department of Trauma Research, St. Anthony Hospital, 11600 W 2nd Pl, Lakewood, CO 80228, USA; Department of Trauma Research, Penrose Hospital, 2222 N Nevada Ave, Colorado Springs, CO 80907, USA; Department of Molecular Biology, Rocky Vista University, 8401 S Chambers Rd, Parker, CO 80134, USA; Corresponding author at: 501 E. Hampden Ave, Rm 4-454, Englewood, CO 80113, USA.

Journal volume & issue: Vol. 2
pp. 83 – 90

Abstract

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From asymptomatic to severe, SARS-CoV-2, causative agent of COVID-19, elicits varying disease severities. Moreover, understanding innate and adaptive immune responses to SARS-CoV-2 is imperative since variants such as Omicron negatively impact adaptive antibody neutralization. Severe COVID-19 is, in part, associated with aberrant activation of complement and Factor XII (FXIIa), initiator of contact system activation. Paradoxically, a protein that inhibits the three known pathways of complement activation and FXIIa, C1 esterase inhibitor (C1-INH), is increased in COVID-19 patient plasma and is associated with disease severity. Here we review the role of C1-INH in the regulation of innate and adaptive immune responses. Additionally, we contextualize regulation of C1-INH and SERPING1, the gene encoding C1-INH, by other pathogens and SARS viruses and propose that viral proteins bind to C1-INH to inhibit its function in severe COVID-19. Finally, we review the current clinical trials and published results of exogenous C1-INH treatment in COVID-19 patients.

Published in Clinical Immunology Communications

ISSN: 2772-6134 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://www.journals.elsevier.com/clinical-immunology-communications

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