Cell Reports (Nov 2021)

Essential role of TOSO/FAIM3 in intestinal IgM reverse transcytosis

  • Nicolas Rochereau,
  • Eva Michaud,
  • Louis Waeckel,
  • Martin Killian,
  • Rémi Gayet,
  • Roman Goguyer-Deschaumes,
  • Xavier Roblin,
  • Gilles Biolley,
  • Blaise Corthésy,
  • Stéphane Paul

Journal volume & issue
Vol. 37, no. 7
p. 110006

Abstract

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Summary: Secretory immunoglobulin A (SIgA) can travel to and from the lumen and transport antigen to subepithelial cells. However, IgM can also multimerize into functional secretory component-bound immunoglobulin. While it is already known that both SIgA and SIgM undergo transcytosis to be secreted at the mucosal surface, only SIgA has been shown to perform retrotranscytosis through microfold cells (M cells) of the Peyer’s patch. Here, we investigate whether SIgM could also be taken up by M cells via retrotranscytosis. This transport involves FcμR binding at the apical membrane of M cells. We then demonstrate that SIgM can be exploited by SIgM-p24 (HIV-capsid protein) complexes during immunization in the nasal- or gut-associated lymphoid tissue (NALT or GALT), conferring efficient immune responses against p24. Our data demonstrate a mucosal function of SIgM, which could play a role in the regulation of mucosal immunity.

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