Transcriptome signatures preceding the induction of anti-stalk antibodies elicited after universal influenza vaccination.
Teresa A Aydillo GomezAna Silvia Gonzalez-ReicheDaniel StadlbauerMary Anne AmperVenugopalan D NairChiara MariottiniStuart C SealfonHarm van BakelPeter PaleseFlorian KrammerAdolfo García-SastrePublished in: NPJ vaccines (2022)
A phase 1 clinical trial to test the immunogenicity of a chimeric group 1 HA (cHA) universal influenza virus vaccine targeting the conserved stalk domain of the hemagglutinin of influenza viruses was carried out. Vaccination with adjuvanted-inactivated vaccines induced high anti-stalk antibody titers. We sought to identify gene expression signatures that correlate with such induction. Messenger-RNA sequencing in whole blood was performed on the peripheral blood of 53 vaccinees. We generated longitudinal data on the peripheral blood of 53 volunteers, at early (days 3 and 7) and late (28 days) time points after priming and boosting with cHAs. Differentially expressed gene analysis showed no differences between placebo and live-attenuated vaccine groups. However, an upregulation of genes involved in innate immune responses and type I interferon signaling was found at day 3 after vaccination with inactivated adjuvanted formulations. Cell type deconvolution analysis revealed a significant enrichment for monocyte markers and different subsets of dendritic cells as mediators for optimal B cell responses and significant increase of anti-stalk antibodies in sera. A significant upregulation of immunoglobulin-related genes was only observed after administration of adjuvanted vaccines (either as primer or booster) with specific induction of anti-stalk IGVH1-69. This approach informed of specific immune signatures that correlate with robust anti-stalk antibody responses, while also helping to understand the regulation of gene expression induced by cHA proteins under different vaccine regimens.
Keyphrases
- peripheral blood
- gene expression
- dendritic cells
- immune response
- genome wide
- clinical trial
- single cell
- dna methylation
- signaling pathway
- endothelial cells
- stem cells
- study protocol
- cross sectional
- randomized controlled trial
- open label
- cancer therapy
- mesenchymal stem cells
- double blind
- oxidative stress
- high glucose
- drug induced
- diabetic rats
- phase iii