Longitudinal multi-omics analysis identifies responses of megakaryocytes, erythroid cells and plasmablasts as hallmarks of severe COVID-19 trajectories

Joana P. Bernardes(Christian-Albrechts-Universität zu Kiel), Neha Mishra(Christian-Albrechts-Universität zu Kiel), Florian Tran(Christian-Albrechts-Universität zu Kiel), Thomas Bahmer, Lena Best, Johanna I. Blase(Christian-Albrechts-Universität zu Kiel), Dora Bordoni(Christian-Albrechts-Universität zu Kiel), Jeanette Franzenburg(Christian-Albrechts-Universität zu Kiel), Ulf Geisen(University Hospital Schleswig-Holstein), Jonathan Josephs‐Spaulding, Philipp Köhler(University of Cologne), Axel Künstner(University of Lübeck), Elisa Rosati(Christian-Albrechts-Universität zu Kiel), Anna C. Aschenbrenner(University of Bonn), Petra Bächer(Christian-Albrechts-Universität zu Kiel), Nathan Baran(Christian-Albrechts-Universität zu Kiel), Teide Jens Boysen(Christian-Albrechts-Universität zu Kiel), Burkhard Brandt, Niklas Bruse(Radboud University Nijmegen), Jonathan Dörr(University Hospital Schleswig-Holstein), Andreas Dräger(German Center for Infection Research), Gunnar Elke(University Hospital Schleswig-Holstein), David Ellinghaus(Christian-Albrechts-Universität zu Kiel), Julia Fischer(University of Cologne), Michael Förster(Christian-Albrechts-Universität zu Kiel), André Franke(Christian-Albrechts-Universität zu Kiel), Sören Franzenburg(Christian-Albrechts-Universität zu Kiel), Norbert Frey, Anette Friedrichs, Janina Fuß(Christian-Albrechts-Universität zu Kiel), Andreas Glück, Jacob Hamm(Christian-Albrechts-Universität zu Kiel), Finn Hinrichsen(Christian-Albrechts-Universität zu Kiel), Marc P. Hoeppner(Christian-Albrechts-Universität zu Kiel), Simon Imm(Christian-Albrechts-Universität zu Kiel), Ralf Junker, Sina Kaiser(University Hospital Schleswig-Holstein), Ying H. Kan(Christian-Albrechts-Universität zu Kiel), Rainer Knoll(University of Bonn), Christoph Lange(German Center for Infection Research), Georg Laue(Christian-Albrechts-Universität zu Kiel), Clemens Lier, Matthias Lindner(Radboud University Nijmegen), Γεώργιος Μαρίνος, Robert Markewitz, Jacob Nattermann(University of Bonn), Rainer Noth, Peter Pickkers(Radboud University Nijmegen), Klaus F. Rabe(Christian-Albrechts-Universität zu Kiel), Alina Renz(German Center for Infection Research), Christoph Röcken(University Hospital Schleswig-Holstein), Jan Rupp(University of Lübeck), Annika Schaffarzyk(University Hospital Schleswig-Holstein), Alexander Scheffold, Jonas Schulte-Schrepping(University of Bonn), Domagoj Schunck(University Hospital Schleswig-Holstein), Dirk Skowasch(University Hospital Bonn), Thomas Ulas(University of Bonn), Klaus‐Peter Wandinger, Michael Wittig(Christian-Albrechts-Universität zu Kiel), Johannes Zimmermann, Hauke Busch(University of Lübeck), Bimba F. Hoyer(University Hospital Schleswig-Holstein), Christoph Kaleta, Jan Heyckendorf(German Center for Infection Research), Matthijs Kox(Radboud University Nijmegen), Jan Rybniker(University of Cologne), Stefan Schreiber(Christian-Albrechts-Universität zu Kiel), Joachim L. Schultze(University of Bonn), Philip Rosenstiel(Christian-Albrechts-Universität zu Kiel), HCA Lung Biological Network and the Deutsche COVID-19 Omics Initiative (DeCOI)
medRxiv
September 18, 2020
10.1101/2020.09.11.20187369
Cited by 5Open Access
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Abstract

Abstract The pandemic spread of the potentially life-threatening disease COVID-19 requires a thorough understanding of the longitudinal dynamics of host responses. Temporal resolution of cellular features associated with a severe disease trajectory will be a pre-requisite for finding disease outcome predictors. Here, we performed a longitudinal multi-omics study using a two-centre German cohort of 13 patients (from Cologne and Kiel, cohort 1). We analysed the bulk transcriptome, bulk DNA methylome, and single-cell transcriptome (>358,000 cells, including BCR profiles) of peripheral blood samples harvested from up to 5 time points. The results from single-cell and bulk transcriptome analyses were validated in two independent cohorts of COVID-19 patients from Bonn (18 patients, cohort 2) and Nijmegen (40 patients, cohort 3), respectively. We observed an increase of proliferating, activated plasmablasts in severe COVID-19, and show a distinct expression pattern related to a hyperactive cellular metabolism of these cells. We further identified a notable expansion of type I IFN-activated circulating megakaryocytes and their progenitors, indicative of emergency megakaryopoiesis, which was confirmed in cohort 2. These changes were accompanied by increased erythropoiesis in the critical phase of the disease with features of hypoxic signalling. Finally, projecting megakaryocyte- and erythroid cell-derived co-expression modules to longitudinal blood transcriptome samples from cohort 3 confirmed an association of early temporal changes of these features with fatal COVID-19 disease outcome. In sum, our longitudinal multi-omics study demonstrates distinct cellular and gene expression dynamics upon SARS-CoV-2 infection, which point to metabolic shifts of circulating immune cells, and reveals changes in megakaryocytes and increased erythropoiesis as important outcome indicators in severe COVID-19 patients.

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