Advanced Science (Nov 2024)

Specific Requirement of the p84/p110γ Complex of PI3Kγ for Antibody‐Activated, Inducible Cross‐Presentation in Murine Type 2 DCs

  • Despoina Koumantou,
  • Aimé Cézaire Adiko,
  • Pierre Bourdely,
  • Mathilde Nugue,
  • Erwan Boedec,
  • Jamel El‐Benna,
  • Renato Monteiro,
  • Cosmin Saveanu,
  • Muriel Laffargue,
  • Matthias P. Wymann,
  • Marc Dalod,
  • Pierre Guermonprez,
  • Loredana Saveanu

DOI
https://doi.org/10.1002/advs.202401179
Journal volume & issue
Vol. 11, no. 44
pp. n/a – n/a

Abstract

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Abstract Cross‐presentation by MHCI is optimally efficient in type 1 dendritic cells (DC) due to their high capacity for antigen processing. However, through specific pathways, other DCs, such as type 2 DCs and inflammatory DCs (iDCs) can also cross‐present antigens. FcγR‐mediated uptake by type 2 DC and iDC subsets mediates antibody‐dependent cross‐presentation and activation of CD8+ T cell responses. Here, an important role for the p84 regulatory subunit of PI3Kγ in mediating efficient cross‐presentation of exogenous antigens in otherwise inefficient cross‐presenting cells, such as type 2 DCs and GM‐CSF‐derived iDCs is identified. FcγR‐mediated cross‐presentation is shown in type 2 and iDCs depend on the enzymatic activity of the p84/p110γ complex of PI3Kγ, which controls the activity of the NADPH oxidase NOX2 and ROS production in murine spleen type 2 DCs and GM‐CSF‐derived iDCs. In contrast, p84/p110γ is largely dispensable for cross‐presentation by type 1 DCs. These findings suggest that PI3Kγ‐targeted therapies, currently considered for oncological practice, may interfere with the ability of type 2 DCs and iDCs to cross‐present antigens contained in immune complexes.

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