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Maturation signatures of conventional dendritic cell subtypes in COVID‐19 suggest direct viral sensing

Authors :
Valeria Bevilacqua
Fabio A. Facchini
Roberto Spreafico
Nicasio Mancini
Luca Nespoli
Giulia Protti
Maria Lucia Sarnicola
Valeria Ranzani
Francesca Mingozzi
Andrea Biondi
Serena Curti
Laura Marongiu
Mariella D'Angiò
Mariacristina Crosti
Sergio Abrignani
Francesca Granucci
Laura Rachele Bettini
Anna Rita Putignano
Nicolò Tamini
Lorenzo Salviati
Nicola Clementi
Mihai Valache
Marongiu, Laura
Protti, Giulia
Facchini, Fabio A.
Valache, Mihai
Mingozzi, Francesca
Ranzani, Valeria
Putignano, Anna Rita
Salviati, Lorenzo
Bevilacqua, Valeria
Curti, Serena
Crosti, Mariacristina
Sarnicola, Maria Lucia
D'Angiò, Mariella
Bettini, Laura Rachele
Biondi, Andrea
Nespoli, Luca
Tamini, Nicolò
Clementi, Nicola
Mancini, Nicasio
Abrignani, Sergio
Spreafico, Roberto
Granucci, Francesca
Marongiu, L
Protti, G
Facchini, F
Valache, M
Mingozzi, F
Ranzani, V
Putignano, A
Salviati, L
Bevilacqua, V
Curti, S
Crosti, M
Sarnicola, M
D'Angio, M
Bettini, L
Biondi, A
Nespoli, L
Tamini, N
Clementi, N
Mancini, N
Abrignani, S
Spreafico, R
Granucci, F
Source :
European Journal of Immunology
Publication Year :
2021

Abstract

Growing evidence suggests that conventional dendritic cells (cDCs) undergo aberrant maturation in COVID‐19, which negatively affects T‐cell activation. The presence of effector T cells in patients with mild disease and dysfunctional T cells in severely ill patients suggests that adequate T‐cell responses limit disease severity. Understanding how cDCs cope with SARS‐CoV‐2 can help elucidate how protective immune responses are generated. Here, we report that cDC2 subtypes exhibit similar infection‐induced gene signatures, with the upregulation of interferon‐stimulated genes and interleukin (IL)‐6 signaling pathways. Furthermore, comparison of cDCs between patients with severe and mild disease showed severely ill patients to exhibit profound downregulation of genes encoding molecules involved in antigen presentation, such as MHCII, TAP, and costimulatory proteins, whereas we observed the opposite for proinflammatory molecules, such as complement and coagulation factors. Thus, as disease severity increases, cDC2s exhibit enhanced inflammatory properties and lose antigen presentation capacity. Moreover, DC3s showed upregulation of anti‐apoptotic genes and accumulated during infection. Direct exposure of cDC2s to the virus in vitro recapitulated the activation profile observed in vivo. Our findings suggest that SARS‐CoV‐2 interacts directly with cDC2s and implements an efficient immune escape mechanism that correlates with disease severity by downregulating crucial molecules required for T‐cell activation. This article is protected by copyright. All rights reserved

Subjects

Subjects :
SARS-CoV-2
dendritic cell
Effector
T-Lymphocytes
Immunology
Antigen presentation
Immunity to infection
COVID-19
Interleukin
Dendritic Cells
Biology
Lymphocyte Activation
single cell transcriptomics
Proinflammatory cytokine
Immune system
Downregulation and upregulation
Humans
Immunology and Allergy
Research Article|Basic
Basic
Signal transduction
Conventional Dendritic Cell
Signal Transduction
Research Article

Details

Database :
OpenAIRE
Journal :
European Journal of Immunology
Accession number :
edsair.doi.dedup.....4817681591ffa5c564024fb1196c0ed8

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