Time-resolved Systems Immunology Reveals a Late Juncture Linked to Fatal COVID-19

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2021 Mar 13

PMID 33713619

Citations 128

Authors

Can Liu

Andrew J Martins

William W Lau

Nicholas Rachmaninoff

Jinguo Chen

Luisa Imberti

Darius Mostaghimi

Danielle L Fink

Peter D Burbelo

Kerry Dobbs

Ottavia M Delmonte

Neha Bansal

Laura Failla

Alessandra Sottini

Eugenia Quiros-Roldan

Kyu Lee Han

Brian A Sellers

Foo Cheung

Rachel Sparks

Tae-Wook Chun

Susan Moir

Michail S Lionakis

Camillo Rossi

Helen C Su

Douglas B Kuhns

Jeffrey I Cohen

Luigi D Notarangelo

John S Tsang

Affiliations

Soon will be listed here.

Abstract

COVID-19 exhibits extensive patient-to-patient heterogeneity. To link immune response variation to disease severity and outcome over time, we longitudinally assessed circulating proteins as well as 188 surface protein markers, transcriptome, and T cell receptor sequence simultaneously in single peripheral immune cells from COVID-19 patients. Conditional-independence network analysis revealed primary correlates of disease severity, including gene expression signatures of apoptosis in plasmacytoid dendritic cells and attenuated inflammation but increased fatty acid metabolism in CD56CD16 NK cells linked positively to circulating interleukin (IL)-15. CD8 T cell activation was apparent without signs of exhaustion. Although cellular inflammation was depressed in severe patients early after hospitalization, it became elevated by days 17-23 post symptom onset, suggestive of a late wave of inflammatory responses. Furthermore, circulating protein trajectories at this time were divergent between and predictive of recovery versus fatal outcomes. Our findings stress the importance of timing in the analysis, clinical monitoring, and therapeutic intervention of COVID-19.

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