Dysregulated early transcriptional signatures linked to mast cell and interferon responses are implicated in COVID-19 severity

Rachel MacCann; Rachel MacCann; Rachel MacCann; Alejandro Abner Garcia Leon; Gabriel Gonzalez; Gabriel Gonzalez; Gabriel Gonzalez; Michael J. Carr; Michael J. Carr; Michael J. Carr; Eoin R. Feeney; Eoin R. Feeney; Obada Yousif; Aoife G. Cotter; Aoife G. Cotter; Eoghan de Barra; Eoghan de Barra; Corinna Sadlier; Peter Doran; Patrick W. Mallon; Patrick W. Mallon; Patrick W. Mallon

doi:10.3389/fimmu.2023.1166574

Frontiers in Immunology (May 2023)

Dysregulated early transcriptional signatures linked to mast cell and interferon responses are implicated in COVID-19 severity

Rachel MacCann,
Rachel MacCann,
Rachel MacCann,
Alejandro Abner Garcia Leon,
Gabriel Gonzalez,
Gabriel Gonzalez,
Gabriel Gonzalez,
Michael J. Carr,
Michael J. Carr,
Michael J. Carr,
Eoin R. Feeney,
Eoin R. Feeney,
Obada Yousif,
Aoife G. Cotter,
Aoife G. Cotter,
Eoghan de Barra,
Eoghan de Barra,
Corinna Sadlier,
Peter Doran,
Patrick W. Mallon,
Patrick W. Mallon,
Patrick W. Mallon

Affiliations

Rachel MacCann: School of Medicine, University College Dublin, Dublin, Ireland
Rachel MacCann: Department of Infectious Diseases, St. Vincent’s University Hospital, Dublin, Ireland
Rachel MacCann: Centre for Experimental Pathogen Host Research (CEPHR), University College Dublin, Dublin, Ireland
Alejandro Abner Garcia Leon: Centre for Experimental Pathogen Host Research (CEPHR), University College Dublin, Dublin, Ireland
Gabriel Gonzalez: Centre for Experimental Pathogen Host Research (CEPHR), University College Dublin, Dublin, Ireland
Gabriel Gonzalez: National Virus Reference Laboratory, University College Dublin, Dublin, Ireland
Gabriel Gonzalez: Japan Initiative for World-leading Vaccine Research and Development Centers, Hokkaido University, Institute for Vaccine Research and Development, Hokkaido, Japan
Michael J. Carr: School of Medicine, University College Dublin, Dublin, Ireland
Michael J. Carr: National Virus Reference Laboratory, University College Dublin, Dublin, Ireland
Michael J. Carr: International Collaboration Unit, International Institute for Zoonosis Control, Hokkaido University, Sapporo, Hokkaido, Japan
Eoin R. Feeney: School of Medicine, University College Dublin, Dublin, Ireland
Eoin R. Feeney: Department of Infectious Diseases, St. Vincent’s University Hospital, Dublin, Ireland
Obada Yousif: Endocrinology Department, Wexford General Hospital, Wexford, Ireland
Aoife G. Cotter: Centre for Experimental Pathogen Host Research (CEPHR), University College Dublin, Dublin, Ireland
Aoife G. Cotter: Department of Infectious Diseases, Mater Misericordiae University Hospital, Dublin, Ireland
Eoghan de Barra: Department of Infectious Diseases, Beaumont Hospital, Beaumont, Dublin, Ireland
Eoghan de Barra: 0Department of International Health and Tropical Medicine, Royal College of Surgeons in Ireland, Dublin, Ireland
Corinna Sadlier: 1Department of Infectious Diseases, Cork University Hospital, Cork, Ireland
Peter Doran: School of Medicine, University College Dublin, Dublin, Ireland
Patrick W. Mallon: School of Medicine, University College Dublin, Dublin, Ireland
Patrick W. Mallon: Department of Infectious Diseases, St. Vincent’s University Hospital, Dublin, Ireland
Patrick W. Mallon: Centre for Experimental Pathogen Host Research (CEPHR), University College Dublin, Dublin, Ireland

DOI: https://doi.org/10.3389/fimmu.2023.1166574
Journal volume & issue: Vol. 14

Abstract

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BackgroundDysregulated immune responses to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection are thought to underlie the progression of coronavirus disease 2019 (COVID-19) to severe disease. We sought to determine whether early host immune-related gene expression could predict clinical progression to severe disease.MethodsWe analysed the expression of 579 immunological genes in peripheral blood mononuclear cells taken early after symptom onset using the NanoString nCounter and compared SARS-CoV-2 negative controls with SARS-CoV-2 positive subjects with mild (SARS+ Mild) and Moderate/Severe disease to evaluate disease outcomes. Biobanked plasma samples were also assessed for type I (IFN-α2a and IFN-β), type II (IFN-γ) and type III (IFN-λ1) interferons (IFNs) as well as 10 additional cytokines using multiplex immunoassays.ResultsWe identified 19 significantly deregulated genes in 62 SARS-CoV-2 positive subject samples within 5 days of symptom onset and 58 SARS-CoV-2 negative controls and found that type I interferon (IFN) signalling (MX1, IRF7, IFITM1, IFI35, STAT2, IRF4, PML, BST2, STAT1) and genes encoding proinflammatory cytokines (TNF, TNFSF4, PTGS2 and IL1B) were upregulated in both SARS+ groups. Moreover, we found that FCER1, involved in mast cell activation, was upregulated in the SARS+ Mild group but significantly downregulated in the SARS+ Moderate/Severe group. In both SARS+ groups we discovered elevated interferon type I IFN-α2a, type II IFN and type III IFN λ1 plasma levels together with higher IL-10 and IL-6. These results indicate that those with moderate or severe disease are characterised by deficiencies in a mast cell response together with IFN hyper-responsiveness, suggesting that early host antiviral immune responses could be a cause and not a consequence of severe COVID-19.ConclusionsThis study suggests that early host immune responses linking defects in mast cell activation with host interferon responses correlates with more severe outcomes in COVID-19. Further characterisation of this pathway could help inform better treatment for vulnerable individuals.

Published in Frontiers in Immunology

ISSN: 1664-3224 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: http://journal.frontiersin.org/journal/immunology

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