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YTHDF2 suppresses the plasmablast genetic program and promotes germinal center formation

Amalie Grenov, Hadas Hezroni, Lior Lasman, Jacob H. Hanna, Ziv Shulman

2022Cell Reports45 citationsDOIOpen Access PDF

Abstract

Antibody-mediated immunity is initiated by B cell differentiation into multiple cell subsets, including plasmablast, memory, and germinal center (GC) cells. B cell differentiation trajectories are determined by transcription factors, yet very few mechanisms that specifically determine early B cell fates have been described. Here, we report a post-transcriptional mechanism that suppresses the plasmablast genetic program and promotes GC B cell fate commitment. Single-cell RNA-sequencing analysis reveals that antigen-specific B cell precursors at the pre-GC stage upregulate YTHDF2, which enhances the decay of methylated transcripts. Ythdf2-deficient B cells exhibit intact proliferation and activation, whereas differentiation into GC B cells is blocked. Mechanistically, B cells require YTHDF2 to attenuate the plasmablast genetic program during GC seeding, and transcripts of key plasmablast-regulating genes are methylated and bound by YTHDF2. Collectively, this study reveals how post-transcriptional suppression of gene expression directs appropriate B cell fate commitment during initiation of the adaptive immune response.

Topics & Concepts

Germinal centerBiologyB cellCell biologyCellular differentiationTranscription factorDownregulation and upregulationCellMemory B cellGeneGeneticsAntibodyImmune Cell Function and InteractionT-cell and B-cell ImmunologyRNA modifications and cancer
YTHDF2 suppresses the plasmablast genetic program and promotes germinal center formation | Litcius