Specific targeting of IL-1β activity to CD8+ T cells allows for safe use as a vaccine adjuvant

Author:

Van Den Eeckhout BramORCID,Van Hoecke LienORCID,Burg Elianne,Van Lint SandraORCID,Peelman Frank,Kley Niko,Uzé Gilles,Saelens XavierORCID,Tavernier JanORCID,Gerlo SarahORCID

Abstract

AbstractAnnual administration and reformulation of influenza vaccines is required for protection against seasonal infections. However, the induction of strong and long-lasting T cells is critical to reach broad and potentially lifelong antiviral immunity. The NLRP3 inflammasome and its product interleukin-1β (IL-1β) are pivotal mediators of cellular immune responses to influenza, yet, overactivation of these systems leads to side effects, which hamper clinical applications. Here, we present a bypass around these toxicities by targeting the activity of IL-1β to CD8+ T cells. Using this approach, we demonstrate safe inclusion of IL-1β as an adjuvant in vaccination strategies, leading to full protection of mice against a high influenza virus challenge dose by raising potent T cell responses. In conclusion, this paper proposes a class of IL-1β-based vaccine adjuvants and also provides further insight in the mechanics of cellular immune responses driven by IL-1β.

Funder

Fonds Wetenschappelijk Onderzoek

Universiteit Gent

European Research Council Orionis Biosciences Inc.

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Infectious Diseases,Pharmacology,Immunology

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