Major alterations in the mononuclear phagocyte landscape associated with COVID-19 severity

Egle Kvedaraite(Karolinska University Hospital), Laura Hertwig(Karolinska University Hospital), Indranil Sinha(Karolinska Institutet), Andrea Ponzetta(Karolinska University Hospital), Ida Hed Myrberg(Karolinska Institutet), Magda Lourda(Karolinska University Hospital), Majda Dzidic(Karolinska University Hospital), Mira Akber(Karolinska University Hospital), Jonas Klingström(Karolinska University Hospital), Elin Folkesson(Karolinska University Hospital), Jagadeeswara Rao Muvva(Karolinska University Hospital), Puran Chen(Karolinska University Hospital), Sara Gredmark‐Russ(Karolinska University Hospital), Susanna Brighenti(Karolinska University Hospital), Anna Norrby‐Teglund(Karolinska University Hospital), Lars I. Eriksson(Karolinska University Hospital), Olav Rooyackers(Karolinska University Hospital), Soo Aleman(Karolinska University Hospital), Kristoffer Strålin(Karolinska University Hospital), Hans‐Gustaf Ljunggren(Karolinska University Hospital), Florent Ginhoux(Agency for Science, Technology and Research), Niklas K. Björkström(Karolinska University Hospital), Jan‐Inge Henter(Karolinska University Hospital), Mattias Svensson(Karolinska University Hospital), Karolinska KI/K COVID-19 Study Group, John Tyler Sandberg, Helena Bergsten(Karolinska University Hospital), Niklas K. Björkström(Karolinska University Hospital), Susanna Brighenti(Karolinska University Hospital), Marcus Buggert, Marta Butrym, Benedict J. Chambers(Karolinska University Hospital), Puran Chen(Karolinska University Hospital), Martin Cornillet, Angélica Cuapio, Isabel Diaz Lozano(Karolinska University Hospital), Majda Dzidic(Karolinska University Hospital), Johanna Emgård, Malin Flodström‐Tullberg, Jean‐Baptiste Gorin(Karolinska University Hospital), Sara Gredmark‐Russ(Karolinska University Hospital), Alvaro Haroun-Izquierdo(Karolinska University Hospital), Laura Hertwig(Karolinska University Hospital), Sadaf Kalsum(Karolinska University Hospital), Jonas Klingström(Karolinska University Hospital), Efthymia Kokkinou(Karolinska University Hospital), Egle Kvedaraite(Karolinska University Hospital), Hans‐Gustaf Ljunggren(Karolinska University Hospital), Nicole Marquardt(Karolinska University Hospital), Magda Lourda(Karolinska University Hospital), Kimia T. Maleki, Karl‐Johan Malmberg, Jakob Michaëlsson, Jenny Mjösberg, Kirsten Moll(Karolinska University Hospital), Jagadeeswara Rao Muvva(Karolinska University Hospital), Anna Norrby‐Teglund(Karolinska University Hospital), Laura M. Palma Medina, Tiphaine Parrot, Lena Radler, Emma Ringqvist, Johan K. Sandberg, Takuya Sekine, Tea Soini(Karolinska University Hospital), Mattias Svensson(Karolinska University Hospital), Janne Tynell, Andreas von Kries, David Wullimann(Karolinska University Hospital), André Perez‐Potti, Olga Rivera‐Ballesteros, Christopher Maucourant, Renata Varnaitė(Karolinska University Hospital), Mira Akber(Karolinska University Hospital), Lena Berglin, Demi Brownlie, Marco Giulio Loreti, Ebba Sohlberg, Tobias Kammann, Elisabet Welin Henriksson(Karolinska University Hospital), Kristoffer Strålin(Karolinska University Hospital), Soo Aleman(Karolinska University Hospital), Anders Sönnerborg, Lena Dillner(Karolinska University Hospital), Anna Färnert, Hedvig Glans, Pontus Nauclér(Karolinska University Hospital), Olav Rooyackers(Karolinska University Hospital), Johan Mårtensson(Karolinska University Hospital), Lars I. Eriksson(Karolinska University Hospital), Björn P. Persson, Jonathan Grip, Christian Unge
Proceedings of the National Academy of Sciences
January 21, 2021
10.1073/pnas.2018587118
Cited by 136Open Access
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Abstract

Dendritic cells (DCs) and monocytes are crucial mediators of innate and adaptive immune responses during viral infection, but misdirected responses by these cells may contribute to immunopathology. Here, we performed high-dimensional flow cytometry-analysis focusing on mononuclear phagocyte (MNP) lineages in SARS-CoV-2-infected patients with moderate and severe COVID-19. We provide a deep and comprehensive map of the MNP landscape in COVID-19. A redistribution of monocyte subsets toward intermediate monocytes and a general decrease in circulating DCs was observed in response to infection. Severe disease coincided with the appearance of monocytic myeloid-derived suppressor cell-like cells and a higher frequency of pre-DC2. Furthermore, phenotypic alterations in MNPs, and their late precursors, were cell-lineage-specific and associated either with the general response against SARS-CoV-2 or COVID-19 severity. This included an interferon-imprint in DC1s observed in all patients and a decreased expression of the coinhibitory molecule CD200R in pre-DCs, DC2s, and DC3 subsets of severely sick patients. Finally, unsupervised analysis revealed that the MNP profile, alone, pointed to a cluster of COVID-19 nonsurvivors. This study provides a reference for the MNP response to SARS-CoV-2 infection and unravels mononuclear phagocyte dysregulations associated with severe COVID-19.

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