A blood atlas of COVID-19 defines hallmarks of disease severity and specificity

D J Ahern,Z Ai,Mark Ainsworth,Charlotte L. Allan,A Allcock,A Ansari,Carolina V. Arancibia-Cárcamo,Dominik Aschenbrenner,M Attar,J K Baillie,E. Barnes,R Bashford-Rogers,A Bashyal,S Beer,G. Berridge,A Beveridge,Sagida Bibi,Tihana Bicanic,L Blackwell,Paul Bowness,Andrew Brent,Anthony Brown,J Broxholme,David Buck,K L Burnham,Helen M. Byrne,S Camara,I Candido Ferreira,Philip D. Charles,W Chen,Chen Y-L.,A Y Chong,Elizabeth A. Clutterbuck,Mark Coles,Christopher P. Conlon,Richard J. Cornall,A P Cribbs,F Curion,E E Davenport,N Davidson,Simon J. Davis,C Dendrou,J. Dequaire,L Dib,J Docker,Christina Dold,T Dong,D Downes,A Drakesmith,Susanna Dunachie,D A Duncan,Chris Q. Eijsbouts,R Esnouf,A Espinosa,R Etherington,Benjamin P. Fairfax,R Fairhead,H Fang,S Fassih,S Felle,M Fernandez Mendoza,Ricardo C. Ferreira,Roman Fischer,T Foord,A Forrow,John Frater,A. Fries,V Gallardo Sanchez,L Garner,C Geeves,Dominique Georgiou,L Godfrey,Tanya Golubchik,M Gomez Vazquez,A Green,H Harper,H A Harrington,Raphael Heilig,Svenja Hester,J. Hill,Charles J. Hinds,C Hird,Ho L-P.,R Hoekzema,B Hollis,J. Hughes,P Hutton,M Jackson,A Jainarayanan,A. James-Bott,K Jansen,Katie Jeffery,E. Y. Jones,Luke Jostins,G Kerr,David Y. Kim,Paul Klenerman,Julian C. Knight,V Kumar,P Kumar Sharma,P Kurupati,A J Kwok,A Lee,A Linder,T Lockett,L. Lonie,M Lopopolo,M Lukoseviciute,J Luo,S Marinou,Brian D. Marsden,Jose Vicente Martinez,Paul M. Matthews,M Mazurczyk,S McGowan,Stuart McKechnie,A Mead,Alexander J. Mentzer,Y Mi,C Monaco,R Montadon,G Napolitani,Isar Nassiri,A Novak,D. OBrien,Daniel T. OConnor,D ODonnell,Graham S. Ogg,L Overend,I Park,Ian D. Pavord,Y Peng,F Penkava,M Pereira Pinho,E Perez,Andrew J. Pollard,F Powrie,B Psaila,T P Quan,E Repapi,S Revale,L Silva-Reyes,Richard J-B.,C Rich-Griffin,T G Ritter,C S Rollier,Matthew J. Rowland,F Ruehle,M Salio,S N Sansom,A Santos Delgado,T Sauka Spengler,R Schwessinger,G Scozzafava,Gavin R. Screaton,A Seigal,Malcolm G. Semple,M Sergeant,C Simoglou Karali,D Sims,Donal T Skelly,H Slawinski,A Sobrinodiaz,N Sousos,L Stafford,L Stockdale,M Strickland,O Sumray,B. Sun,C Taylor,S. Taylor,Andrew M. Taylor,S Thongjuea,H Thraves,John A. Todd,A Tomic,O Tong,A. Trebes,Dominik Trzupek,F A Tucci,Lance Turtle,Irina A. Udalova,Holm H. Uhlig,E van Grinsven,Iolanda Vendrell,M Verheul,A Voda,G Wang,L. Wang,D. Wang,Peter J. Watkinson,Robert A. Watson,M Weinberger,J Whalley,L Witty,K Wray,L Xue,H Y Yeung,Z. Yin,R K Young,Jonathan Youngs,P Zhang,Zurke Y-X.

A blood atlas of COVID-19 defines hallmarks of disease severity and specificity

2021

Treatment of severe COVID-19 is currently limited by clinical heterogeneity and incomplete understanding of potentially druggable immune mediators of disease. To advance this, we present a comprehensive multi-omic blood atlas in patients with varying COVID-19 severity and compare with influenza, sepsis and healthy volunteers. We identify immune signatures and correlates of host response. Hallmarks of disease severity revealed cells, their inflammatory mediators and networks as potential therapeutic targets, including progenitor cells and specific myeloid and lymphocyte subsets, features of the immune repertoire, acute phase response, metabolism and coagulation. Persisting immune activation involving AP-1/p38MAPK was a specific feature of COVID-19. The plasma proteome enabled sub-phenotyping into patient clusters, predictive of severity and outcome. Tensor and matrix decomposition of the overall dataset revealed feature groupings linked with disease severity and specificity. Our systems-based integrative approach and blood atlas will inform future drug development, clinical trial design and personalised medicine approaches for COVID-19.

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