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IL-21 shapes the B cell response in a context-dependent manner

Youngjun Kim, Francesca Manara, Simon Grassmann, Kalina T. Belcheva, Kanelly Reyes, Hyunu Kim, Stephanie Downs‐Canner, William T. Yewdell, Joseph C. Sun, Jayanta Chaudhuri

2025Cell Reports17 citationsDOIOpen Access PDF

Abstract

The T-cell-derived cytokine IL-21 is crucial for germinal center (GC) responses, but its precise role in B cell function has remained elusive. Using IL-21 receptor ( Il21r ) conditional knockout mice and ex vivo culture systems, we demonstrate that IL-21 has dual effects on B cells. While IL-21 induced apoptosis in a STAT3-dependent manner in naive B cells, it promoted the robust proliferation of pre-activated B cells, particularly IgG1 + B cells. In vivo , B-cell-specific Il21r deletion impaired IgG1 responses post-immunization and disrupted progression from pre-GC to GC states. Although Il21r deficiency did not affect the proportion of IgG1 + cells among GC B cells, it greatly diminished the proportion of IgG1 + cells among the plasmablast/plasma cell population. Collectively, our findings suggest that IL-21 serves as a critical regulator of B cell fates, influencing B cell apoptosis and proliferation in a context-dependent manner. • IL-21 induces apoptosis in naive B cells but promotes proliferation in activated B cells • IL-21 promotes preferential expansion of IgG1 + B cells through synergy with BCR signaling • Il21r deletion in B cells leads to quantitative and qualitative defects in GC responses Kim et al. observed that IL-21 regulates B cell fate in a context-dependent manner. IL-21 induces apoptosis in naive B cells but promotes proliferation of activated B cells, especially IgG1 + cells. B-cell-specific IL-21 receptor deficiency impairs GC formation and IgG1 antibody production.

Topics & Concepts

Context (archaeology)Cell biologyBiologyPaleontologyT-cell and B-cell ImmunologyImmune Cell Function and InteractionImmunotherapy and Immune Responses
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