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TLR7 Signaling Shapes and Maintains Antibody Diversity Upon Virus-Like Particle Immunization

Xinyue Chang, Pascal S. Krenger, Caroline C. Krueger, Lisha Zha, Jiami Han, Alexander Yermanos, Salony Roongta, Mona O. Mohsen, Annette Oxenius, Monique Vogel, Martin F. Bachmann

2022Frontiers in Immunology44 citationsDOIOpen Access PDF

Abstract

Virus-like particles (VLPs) are used in different marketed vaccines and are able to induce potent antibody responses. The innate pattern recognition receptors TLR7/8 recognize single stranded (ss) RNA naturally packaged into some VLPs and have been shown to enhance the production of IgG antibodies upon immunization. Here we demonstrate that, upon immunization with RNA-loaded bacteriophage-derived VLP Qβ, TLR7 signaling accelerates germinal center formation, promotes affinity/avidity maturation of VLP-specific IgG and isotype switching to IgG2b/2c. These findings extrapolated to antigens displayed on Qβ; as Fel d 1, the major cat allergen, chemically attached to Qβ also induced higher affinity/avidity IgG2b/2c antibodies in a TLR7-dependent fashion. Chimeric mice lacking TLR7-expression exclusively in B cells demonstrated that the enhanced IgG responses were driven by a B cell intrinsic mechanism. Importantly, deep sequencing of the BCR repertoire of antigen-specific B cells demonstrated higher diversity in mice with TLR7 signaling in B cells, suggesting that TLR7-signaling drives BCR repertoire development and diversity. Furthermore, the current data demonstrate that high levels of clonal diversity are reached early in the response and maintained by TLR7 signaling. In conclusion, TLR7 signaling enhances levels and quality of IgG antibodies, and this finding has major implications for vaccine design.

Topics & Concepts

TLR7BiologyImmunoglobulin class switchingAntibodyAvidityGerminal centerB-cell receptorCell biologyRNAAntigenVirologyMolecular biologyB cellImmune systemImmunologyToll-like receptorInnate immune systemGeneGeneticsImmunotherapy and Immune ResponsesT-cell and B-cell ImmunologyImmune Cell Function and Interaction