Sustained IFN signaling is associated with delayed development of 
SARS-CoV-2-specific immunity

Brunet-Ratnasingham, Elsa; Morin, Sacha; Randolph, Haley E.; Labrecque, Marjorie; Bélair, Justin; Lima-Barbosa, Raphaël; Pagliuzza, Amélie; Marchitto, Lorie; Hultström, Michael; Niessl, Julia; Cloutier, Rose; Sreng Flores, Alina M.; Brassard, Nathalie; Benlarbi, Mehdi; Prévost, Jérémie; Ding, Shilei; Anand, Sai Priya; Sannier, Gérémy; Marks, Amanda; Wågsäter, Dick; Bareke, Eric; Zeberg, Hugo; Lipcsey, Miklos; Frithiof, Robert; Larsson, Anders; Zhou, Sirui; Nakanishi, Tomoko; Morrison, David; Vezina, Dani; Bourassa, Catherine; Gendron-Lepage, Gabrielle; Medjahed, Halima; Point, Floriane; Richard, Jonathan; Larochelle, Catherine; Prat, Alexandre; Cunningham, Janet L.; Arbour, Nathalie; Durand, Madeleine; Richards, J. Brent; Moon, Kevin; Chomont, Nicolas; Finzi, Andrés; Tétreault, Martine; Barreiro, Luis; Wolf, Guy; Kaufmann, Daniel E.

doi:10.1038/s41467-024-48556-y

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Sustained IFN signaling is associated with delayed development of SARS-CoV-2-specific immunity

Brunet-Ratnasingham, E., Morin, S., Randolph, H. E., Labrecque, M., Bélair, J., Lima-Barbosa, R., et al. (2024). Sustained IFN signaling is associated with delayed development of SARS-CoV-2-specific immunity. Nature Communications, 15: 4177. doi:10.1038/s41467-024-48556-y.

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Item Permalink: https://hdl.handle.net/21.11116/0000-000F-58BB-C Version Permalink: https://hdl.handle.net/21.11116/0000-000F-58BE-9

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Creators:
Brunet-Ratnasingham, Elsa, Author
Morin, Sacha, Author
Randolph, Haley E., Author
Labrecque, Marjorie, Author
Bélair, Justin, Author
Lima-Barbosa, Raphaël, Author
Pagliuzza, Amélie, Author
Marchitto, Lorie, Author
Hultström, Michael, Author
Niessl, Julia, Author
Cloutier, Rose, Author
Sreng Flores, Alina M., Author
Brassard, Nathalie, Author
Benlarbi, Mehdi, Author
Prévost, Jérémie, Author
Ding, Shilei, Author
Anand, Sai Priya, Author
Sannier, Gérémy, Author
Marks, Amanda, Author
Wågsäter, Dick, Author
Bareke, Eric, AuthorZeberg, Hugo¹, Author Lipcsey, Miklos, AuthorFrithiof, Robert, AuthorLarsson, Anders, AuthorZhou, Sirui, AuthorNakanishi, Tomoko, AuthorMorrison, David, AuthorVezina, Dani, AuthorBourassa, Catherine, AuthorGendron-Lepage, Gabrielle, AuthorMedjahed, Halima, AuthorPoint, Floriane, AuthorRichard, Jonathan, AuthorLarochelle, Catherine, AuthorPrat, Alexandre, AuthorCunningham, Janet L., AuthorArbour, Nathalie, AuthorDurand, Madeleine, AuthorRichards, J. Brent, AuthorMoon, Kevin, AuthorChomont, Nicolas, AuthorFinzi, Andrés, AuthorTétreault, Martine, AuthorBarreiro, Luis, AuthorWolf, Guy, AuthorKaufmann, Daniel E., Author more..

Affiliations:
1Department of Evolutionary Genetics, Max Planck Institute for Evolutionary Anthropology, Max Planck Society, ou_1497672

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Free keywords: Adult; Aged; Antibodies, Viral; CD4-Positive T-Lymphocytes; COVID-19; Female; Humans; Immunoglobulin G; Interferons; Male; Middle Aged; SARS-CoV-2; Signal Transduction; Spike Glycoprotein, Coronavirus

Abstract: Plasma RNAemia, delayed antibody responses and inflammation predict COVID-19 outcomes, but the mechanisms underlying these immunovirological patterns are poorly understood. We profile 782 longitudinal plasma samples from 318 hospitalized patients with COVID-19. Integrated analysis using k-means reveals four patient clusters in a discovery cohort: mechanically ventilated critically-ill cases are subdivided into good prognosis and high-fatality clusters (reproduced in a validation cohort), while non-critical survivors segregate into high and low early antibody responders. Only the high-fatality cluster is enriched for transcriptomic signatures associated with COVID-19 severity, and each cluster has distinct RBD-specific antibody elicitation kinetics. Both critical and non-critical clusters with delayed antibody responses exhibit sustained IFN signatures, which negatively correlate with contemporaneous RBD-specific IgG levels and absolute SARS-CoV-2-specific B and CD4+ T cell frequencies. These data suggest that the “Interferon paradox” previously described in murine LCMV models is operative in COVID-19, with excessive IFN signaling delaying development of adaptive virus-specific immunity. © The Author(s) 2024.

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Language(s): eng - English

Dates: Published Online: 2024-05-16

Publication Status: Published online

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Rev. Type: Peer

Identifiers: DOI: 10.1038/s41467-024-48556-y

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Title: Nature Communications

Source Genre: Journal

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Pages: - Volume / Issue: 15 Sequence Number: 4177 Start / End Page: - Identifier: ISSN: 2041-1723