Litcius/Paper detail

Critical roles of chronic BCR signaling in the differentiation of anergic B cells into age-associated B cells in aging and autoimmunity

Keisuke Imabayashi, Yutaro Yada, Kazuhiko Kawata, Motoki Yoshimura, Takeshi Iwasaki, Akemi Baba, Akihito Harada, Koichi Akashi, Hiroaki Niiro, Yoshihiro Baba

2025Science Advances13 citationsDOIOpen Access PDF

Abstract

Age-associated B cells (ABCs) with autoreactive properties accumulate with age and expand prematurely in autoimmune diseases. However, the mechanisms behind ABC generation and maintenance remain poorly understood. We show that continuous B cell receptor (BCR) signaling is essential for ABC development from anergic B cells in aged and autoimmune mice. ABCs exhibit constitutive BCR activation, with surface BCRs being internalized. Notably, anergic B cells, but not nonautoreactive B cells, contributed to ABC formation in these models. Anergic B cells also showed a greater propensity for in vitro differentiation into ABCs, which was inhibited by the expression of the transcription factor Nr4a1. Bruton's tyrosine kinase (Btk), a key BCR signaling component, was constitutively activated in ABCs from aged and autoimmune mice as well as patients with lupus. Inhibiting Btk reduced ABC numbers and ameliorated the pathogenicity of lupus mice. Our findings reveal critical mechanisms underlying ABC development and offer previously unrecognized therapeutic insights for autoimmune diseases.

Topics & Concepts

Bruton's tyrosine kinaseAutoimmunitybreakpoint cluster regionImmunologyB-cell receptorBiologyB cellSignal transductionCell biologyTyrosine kinaseCancer researchReceptorImmune systemGeneticsAntibodyT-cell and B-cell ImmunologyImmune Cell Function and InteractionImmunotherapy and Immune Responses