Yu Adachi scite author profile

Despite the importance of memory B cells in protection from reinfection, how such memory cells are selected and generated during germinal-center (GC) reactions remains unclear. We found here that light-zone (LZ) GC B cells with B cell antigen receptors (BCRs) of lower affinity were prone to enter the memory B cell pool. Mechanistically, cells in this memory-prone fraction had higher expression of the transcriptional repressor Bach2 than that of their counterparts with BCRs of higher affinity. Haploinsufficiency of Bach2 resulted in reduced generation of memory B cells, independently of suppression of the gene encoding the transcription factor Blimp-1. Bach2 expression in GC cells was inversely correlated with the strength of help provided by T cells. Thus, we propose an instructive model in which weak help from T cells maintains relatively high expression of Bach2, which predisposes GC cells to enter the memory pool.

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Antibodies to a Conserved Influenza Head Interface Epitope Protect by an IgG Subtype-Dependent Mechanism

Watanabe

McCarthy

Kuraoka

et al. 2019

Cell

164

219

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Distinct germinal center selection at local sites shapes memory B cell response to viral escape

et al. 2015

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Temporal maturation of neutralizing antibodies in COVID-19 convalescent individuals improves potency and breadth to circulating SARS-CoV-2 variants

et al. 2021

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Protective neutralizing influenza antibody response in the absence of T follicular helper cells

et al. 2016

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Virus infection induces the development of T follicular helper (T) and T helper 1 (T1) cells. Although T cells are important in anti-viral humoral immunity, the contribution of T1 cells to a protective antibody response remains unknown. We found that IgG2 antibodies predominated in the response to vaccination with inactivated influenza A virus (IAV) and were responsible for protective immunity to lethal challenge with pathogenic H5N1 and pandemic H1N1 IAV strains, even in mice that lacked T cells and germinal centers. The cytokines interleukin-21 and interferon-γ, which are secreted from T1 cells, were essential for the observed greater persistence and higher titers of IgG2 protective antibodies. Our results suggest that T1 induction could be a promising strategy for producing effective neutralizing antibodies against emerging influenza viruses.

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Yu Adachi

Regulated selection of germinal-center cells into the memory B cell compartment

Antibodies to a Conserved Influenza Head Interface Epitope Protect by an IgG Subtype-Dependent Mechanism

Distinct germinal center selection at local sites shapes memory B cell response to viral escape

Temporal maturation of neutralizing antibodies in COVID-19 convalescent individuals improves potency and breadth to circulating SARS-CoV-2 variants

Protective neutralizing influenza antibody response in the absence of T follicular helper cells

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