Prior Vaccination Exceeds Prior Infection in Eliciting Innate and Humoral Immune Responses in Omicron Infected Outpatients

Prior Vaccination Exceeds Prior Infection in Eliciting Innate and Humoral Immune Responses in Omicron Infected Outpatients

Antibody response following Omicron infection is reported to be less robust than that to other variants. Here we investigated how prior vaccination and/or prior infection modulates that response. Disease severity, antibody responses and immune transcriptomes were characterized in four groups of Omic...

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Published in:Frontiers in immunology Vol. 13; p. 916686
Main Authors: Lee, Hye Kyung, Knabl, Ludwig, Walter, Mary, Dai, Yuhai, Füßl, Magdalena, Caf, Yasemin, Jeller, Claudia, Knabl, Philipp, Obermoser, Martina, Baurecht, Christof, Kaiser, Norbert, Zabernigg, August, Wurdinger, Gernot M., Furth, Priscilla A., Hennighausen, Lothar
Format: Journal Article
Language:English
Published: Frontiers Media S.A 15-06-2022
Subjects:
antibody responses
COVID-19 alpha infection
immune transcriptome
Immunology
interferon response
prior COVID-19 infection
SARS-CoV-2 omicron infection
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Summary:Antibody response following Omicron infection is reported to be less robust than that to other variants. Here we investigated how prior vaccination and/or prior infection modulates that response. Disease severity, antibody responses and immune transcriptomes were characterized in four groups of Omicron-infected outpatients (n=83): unvaccinated/no prior infection, vaccinated/no prior infection, unvaccinated/prior infection and vaccinated/prior infection. The percentage of patients with asymptomatic or mild disease was highest in the vaccinated/no prior infection group (87%) and lowest in the unvaccinated/no prior infection group (47%). Significant anti-Omicron spike antibody levels and neutralizing activity were detected in the vaccinated group immediately after infection but were not present in the unvaccinated/no prior infection group. Within two weeks, antibody levels against Omicron, increased. Omicron neutralizing activity in the vaccinated group exceeded that of the prior infection group. No increase in neutralizing activity in the unvaccinated/no prior infection group was seen. The unvaccinated/prior infection group showed an intermediate response. We then investigated the early transcriptomic response following Omicron infection in these outpatient populations and compared it to that found in unvaccinated hospitalized patients with Alpha infection. Omicron infected patients showed a gradient of transcriptional response dependent upon whether or not they were previously vaccinated or infected. Vaccinated patients showed a significantly blunted interferon response as compared to both unvaccinated Omicron infected outpatients and unvaccinated Alpha infected hospitalized patients typified by the response of specific gene classes such as OAS and IFIT that control anti-viral responses and IFI27, a predictor of disease outcome.
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These authors have contributed equally to this work
Edited by: Yongjun Sui, National Cancer Institute (NIH), United States
This article was submitted to Vaccines and Molecular Therapeutics, a section of the journal Frontiers in Immunology
Reviewed by: Marion Russier, Max Planck Institute of Biochemistry, Germany; Eva Gizella Rakasz, University of Wisconsin-Madison, United States
This author has senior authorship
ISSN:1664-3224
1664-3224
DOI:10.3389/fimmu.2022.916686