Molecular Basis for Potent B Cell Responses to Antigen Displayed on Particles of Viral Size

Overview

Journal Nat Immunol

Date 2023 Aug 31

PMID 37653247

Authors

Jeremy F Brooks

Julianne Riggs

James L Mueller

Raisa Mathenge

Wei-Yun Wholey

Alexander R Meyer

Sekou-Tidiane Yoda

Vivasvan S Vykunta

Hailyn V Nielsen

Wei Cheng

Julie Zikherman

Affiliations

Soon will be listed here.

Abstract

Multivalent viral epitopes induce rapid, robust and T cell-independent humoral immune responses, but the biochemical basis for such potency remains incompletely understood. We take advantage of a set of liposomes of viral size engineered to display affinity mutants of the model antigen (Ag) hen egg lysozyme. Particulate Ag induces potent 'all-or-none' B cell responses that are density dependent but affinity independent. Unlike soluble Ag, particulate Ag induces signal amplification downstream of the B cell receptor by selectively evading LYN-dependent inhibitory pathways and maximally activates NF-κB in a manner that mimics T cell help. Such signaling induces MYC expression and enables even low doses of particulate Ag to trigger robust B cell proliferation in vivo in the absence of adjuvant. We uncover a molecular basis for highly sensitive B cell responses to viral Ag display that is independent of encapsulated nucleic acids and is not merely accounted for by avidity and B cell receptor cross-linking.

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