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Type I interferon restricts mRNA vaccine efficacy through suppression of antigen uptake in cDCs

Tyson Lobb, Alexandria Dickson, Wenzheng Guo, Samashritha Beeram, Javier A. Carrero, Yago R. Dalben, Richard J. DiPaolo, Elise Alspach, Longping V. Tse, Stephen T. Ferris

2026npj Vaccines6 citationsDOIOpen Access PDF

Abstract

Type I interferons (IFN) are key mediators of innate immune activation, promoting upregulation of costimulatory molecules and Major Histocompatibility Complex (MHC) I/II on antigen-presenting cells (APCs). However, IFN also suppress endogenous translation to restrict viral replication. Critically, IFN-stimulated APCs lose the capacity to acquire new antigens, making the timing of IFN signaling a crucial determinant of vaccine efficacy. Here, we show that both DC-specific loss of IFNα/β receptor (IFNαR) and transient blockade of IFNαR before vaccination enhances vaccine uptake and expression within DCs, improves CD8⁺ T cell priming, and leads to superior tumor control. We also demonstrate that IFN signaling before vaccination, triggered by prior infection or administration of a different vaccine, impairs dendritic cell uptake of mRNA-LNP vaccines and reduces the magnitude of vaccine-specific CD8⁺ T cell responses. These findings highlight the dual-edged nature of IFN signaling and offer a potential strategy for enhancing vaccine-induced immunity.

Topics & Concepts

InterferonImmune systemDownregulation and upregulationInnate immune systemImmunologyInterferon type IVaccinationBiologyT cellCell biologySignal transductionBlockadeMajor histocompatibility complexAntigenAcquired immune systemDendritic cellImmunotherapyReceptorVaccine efficacyEndogenyCellAlpha interferonImmunityAntigen-presenting cellVirologyTranslation (biology)Cell signalingMessenger RNAT-cell receptorAntigen presentationCell typeViral infectionInterferon gammaCytokineImmunotherapy and Immune ResponsesCancer Immunotherapy and Biomarkersinterferon and immune responses
Type I interferon restricts mRNA vaccine efficacy through suppression of antigen uptake in cDCs | Litcius