Frontiers in Immunology (May 2024)

IgG sialylation occurs in B cells pre antibody secretion

  • Anja Werner,
  • Maja Hanić,
  • Olga O. Zaitseva,
  • Gordan Lauc,
  • Anja Lux,
  • Anja Lux,
  • Lars Nitschke,
  • Lars Nitschke,
  • Falk Nimmerjahn,
  • Falk Nimmerjahn

DOI
https://doi.org/10.3389/fimmu.2024.1402000
Journal volume & issue
Vol. 15

Abstract

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Sialic acids as terminal sugar residues on cell surface or secreted proteins have many functional roles. In particular, the presence or absence of α2,6-linked sialic acid residues at the immunoglobulin G (IgG) Fc fragment can switch IgG effector functions from pro- to anti-inflammatory activity. IgG glycosylation is considered to take place inside the plasma blast/plasma cell while the molecule travels through the endoplasmic reticulum and Golgi apparatus before being secreted. However, more recent studies have suggested that IgG sialylation may occur predominantly post-antibody secretion. To what extent this extracellular IgG sialylation process contributes to overall IgG sialylation remains unclear, however. By generating bone marrow chimeric mice with a B cell-specific deletion of ST6Gal1, the key enzyme required for IgG sialylation, we now show that sialylation of the IgG Fc fragment exclusively occurs within B cells pre-IgG secretion. We further demonstrate that B cells expressing ST6Gal1 have a developmental advantage over B cells lacking ST6Gal1 expression and thus dominate the plasma cell pool and the resulting serum IgG population in mouse models in which both ST6Gal1-sufficient and -deficient B cells are present.

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