Deciphering the state of immune silence in fatal COVID-19 patients

Author:

Bost Pierre,De Sanctis Francesco,Canè Stefania,Ugel StefanoORCID,Donadello Katia,Castellucci Monica,Eyal David,Fiore Alessandra,Anselmi Cristina,Barouni Roza Maria,Trovato Rosalinda,Caligola SimoneORCID,Lamolinara AlessiaORCID,Iezzi ManuelaORCID,Facciotti FedericaORCID,Mazzariol Annarita,Gibellini Davide,De Nardo Pasquale,Tacconelli Evelina,Gottin Leonardo,Polati Enrico,Schwikowski BennoORCID,Amit IdoORCID,Bronte VincenzoORCID

Abstract

AbstractSince the beginning of the SARS-CoV-2 pandemic, COVID-19 appeared as a unique disease with unconventional tissue and systemic immune features. Here we show a COVID-19 immune signature associated with severity by integrating single-cell RNA-seq analysis from blood samples and broncho-alveolar lavage fluids with clinical, immunological and functional ex vivo data. This signature is characterized by lung accumulation of naïve lymphoid cells associated with a systemic expansion and activation of myeloid cells. Myeloid-driven immune suppression is a hallmark of COVID-19 evolution, highlighting arginase-1 expression with immune regulatory features of monocytes. Monocyte-dependent and neutrophil-dependent immune suppression loss is associated with fatal clinical outcome in severe patients. Additionally, our analysis shows a lung CXCR6+ effector memory T cell subset is associated with better prognosis in patients with severe COVID-19. In summary, COVID-19-induced myeloid dysregulation and lymphoid impairment establish a condition of ‘immune silence’ in patients with critical COVID-19.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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