Complex Subsets but Redundant Clonality After B Cells Egress from Spontaneous Germinal Centers

Overview

Journal Elife

Specialty Biology

Date 2023 Jun 21

PMID 37341394

Authors

Carlos Castrillon

Lea Simoni

Theo van den Broek

Cees van der Poel

Elliot H Akama-Garren

Minghe Ma

Michael C Carroll

Affiliations

Soon will be listed here.

Abstract

Affinity matured self-reactive antibodies are found in autoimmune diseases like systemic lupus erythematous. Here, we used fate-mapping reporter mice and single-cell transcriptomics coupled to antibody repertoire analysis to characterize the post-germinal center (GC) B cell compartment in a new mouse model of autoimmunity. Antibody-secreting cells (ASCs) and memory B cells (MemBs) from spontaneous GCs grouped into multiple subclusters. ASCs matured into two terminal clusters, with distinct secretion, antibody repertoire and metabolic profiles. MemBs contained FCRL5+ and CD23+ subsets, with different in vivo localization in the spleen. GC-derived FCRL5+ MemBs share transcriptomic and repertoire properties with atypical B cells found in aging and infection and localize to the marginal zone, suggesting a similar contribution to recall responses. While transcriptomically diverse, ASC and MemB subsets maintained an underlying clonal redundancy. Therefore, self-reactive clones could escape subset-targeting therapy by perpetuation of self-reactivity in distinct subsets.

Citing Articles

Germinal center versus extrafollicular responses in systemic autoimmunity: Who turns the blade on self?.

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