Hyperinflammatory environment drives dysfunctional myeloid cell effector response to bacterial challenge in COVID-19

Srikanth Mairpady Shambat; Alejandro Gómez-Mejia; Tiziano A Schweizer; Markus Huemer; Chun-Chi Chang; Claudio Acevedo; Judith Bergada-Pijuan; Clément Vulin; Daniel A Hofmaenner; Thomas C Scheier; Sanne Hertegonne; Elena Parietti; Nataliya Miroshnikova; Pedro D Wendel Garcia; Matthias P Hilty; Philipp Karl Buehler; Reto A Schuepbach; Silvio D Brugger; Annelies S Zinkernagel

doi:10.1371/journal.ppat.1010176

Hyperinflammatory environment drives dysfunctional myeloid cell effector response to bacterial challenge in COVID-19

PLoS Pathog. 2022 Jan 10;18(1):e1010176. doi: 10.1371/journal.ppat.1010176. eCollection 2022 Jan.

Authors

Srikanth Mairpady Shambat¹, Alejandro Gómez-Mejia¹, Tiziano A Schweizer¹, Markus Huemer¹, Chun-Chi Chang¹, Claudio Acevedo¹, Judith Bergada-Pijuan¹, Clément Vulin¹, Daniel A Hofmaenner², Thomas C Scheier¹, Sanne Hertegonne¹, Elena Parietti¹, Nataliya Miroshnikova¹, Pedro D Wendel Garcia², Matthias P Hilty², Philipp Karl Buehler², Reto A Schuepbach², Silvio D Brugger¹, Annelies S Zinkernagel¹

Affiliations

¹ Department of Infectious Diseases and Hospital Epidemiology, University Hospital of Zurich, University of Zurich, Zurich, Switzerland.
² Institute of Intensive Care, University Hospital of Zurich, University of Zurich, Zurich, Switzerland.

Abstract

COVID-19 displays diverse disease severities and symptoms including acute systemic inflammation and hypercytokinemia, with subsequent dysregulation of immune cells. Bacterial superinfections in COVID-19 can further complicate the disease course and are associated with increased mortality. However, there is limited understanding of how SARS-CoV-2 pathogenesis and hypercytokinemia impede the innate immune function against bacterial superinfections. We assessed the influence of COVID-19 plasma hypercytokinemia on the functional responses of myeloid immune cells upon bacterial challenges from acute-phase COVID-19 patients and their corresponding recovery-phase. We show that a severe hypercytokinemia status in COVID-19 patients correlates with the development of bacterial superinfections. Neutrophils and monocytes derived from COVID-19 patients in their acute-phase showed an impaired intracellular microbicidal capacity upon bacterial challenges. The impaired microbicidal capacity was reflected by abrogated MPO and reduced NETs production in neutrophils along with reduced ROS production in both neutrophils and monocytes. Moreover, we observed a distinct pattern of cell surface receptor expression on both neutrophils and monocytes, in line with suppressed autocrine and paracrine cytokine signaling. This phenotype was characterized by a high expression of CD66b, CXCR4 and low expression of CXCR1, CXCR2 and CD15 in neutrophils and low expression of HLA-DR, CD86 and high expression of CD163 and CD11b in monocytes. Furthermore, the impaired antibacterial effector function was mediated by synergistic effect of the cytokines TNF-α, IFN-γ and IL-4. COVID-19 patients receiving dexamethasone showed a significant reduction of overall inflammatory markers in the plasma as well as exhibited an enhanced immune response towards bacterial challenge ex vivo. Finally, broad anti-inflammatory treatment was associated with a reduction in CRP, IL-6 levels as well as length of ICU stay and ventilation-days in critically ill COVID-19 patients. Our data provides insights into the transient functional dysregulation of myeloid immune cells against subsequent bacterial infections in COVID-19 patients and describe a beneficial role for the use of dexamethasone in these patients.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

COVID-19 / microbiology*
COVID-19 / virology
Cytokine Release Syndrome / complications*
Cytokine Release Syndrome / microbiology
Cytokine Release Syndrome / virology
Cytokines / metabolism*
Humans
Lymphocytes / immunology
Lymphocytes / microbiology
Lymphocytes / virology
Monocytes / immunology
Monocytes / microbiology
Monocytes / virology*
Neutrophils / immunology
Neutrophils / microbiology
Neutrophils / virology*
SARS-CoV-2 / pathogenicity

Substances

Cytokines

Grants and funding

This work was funded by the Swiss National Science Foundation project grant 31003A_176252 (to A.S.Z), http://www.snf.ch/en/Pages/default.aspx the Swiss National Science Foundation Biobanking grant 31BK30_185401 (to A.S.Z), http://www.snf.ch/en/Pages/default.aspx the Uniscientia Foundation Grant (to A.S.Z, S.M.S), https://www.uzhfoundation.ch/en/ by the Swedish Society for Medical Research (SSMF) foundation grant P17-0179 (to S.M.S), https://www.ssmf.se/about-ssmf-in-english/ the Promedica Foundation 1449/M (to S.D.B) https://stiftungen.stiftungschweiz.ch/organizations/promedica-stiftung The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.