Author
Listed:
- Morgane Gossez
(Lyon-Sud & Edouard Herriot University Hospitals
ENS de Lyon)
- Clara Vigneron
(ENS de Lyon)
- Alexandra Vandermoeten
(Structure Fédérative de Recherche (SFR) Santé Lyon Est)
- Margot Lepage
(Lyon-Sud & Edouard Herriot University Hospitals
ENS de Lyon)
- Louise Courcol
(ENS de Lyon)
- Remy Coudereau
(Lyon-Sud & Edouard Herriot University Hospitals
bioMérieux))
- Helena Paidassai
(ENS de Lyon)
- Laurent Jallades
(ENS de Lyon
Hematology Laboratory)
- Jonathan Lopez
(Lyon Sud University Hospital)
- Khalil Kandara
(Lyon-Sud & Edouard Herriot University Hospitals)
- Marine Ortillon
(Lyon-Sud & Edouard Herriot University Hospitals)
- Marine Mommert
(bioMérieux))
- Astrid Fabri
(Lyon-Sud & Edouard Herriot University Hospitals)
- Estelle Peronnet
(bioMérieux))
- Clémence Grosjean
(bioMérieux))
- Marielle Buisson
(Hospices Civils de Lyon)
- Anne-Claire Lukaszewicz
(bioMérieux)
Edouard Herriot Hospital)
- Thomas Rimmelé
(bioMérieux)
Edouard Herriot Hospital)
- Laurent Argaud
(Edouard Herriot Hospital)
- Martin Cour
(Edouard Herriot Hospital)
- Bénédicte F. Py
(ENS de Lyon)
- Olivier Thaunat
(ENS de Lyon)
- Thierry Defrance
(ENS de Lyon)
- Guillaume Monneret
(Lyon-Sud & Edouard Herriot University Hospitals
bioMérieux))
- Fabienne Venet
(Lyon-Sud & Edouard Herriot University Hospitals
ENS de Lyon)
Abstract
Sepsis, a leading cause of death in intensive care units, is associated with immune alterations that increase the patients’ risk of secondary infections and mortality, so better understandings of the pathophysiology of sepsis-induced immunosuppression is essential for the development of therapeutic strategies. In a murine model of sepsis that recapitulates immune alterations observed in patients, here we demonstrate that PD-L1+CD44+B220LowCD138+IgM+ regulatory plasma cells are induced in spleen and regulate ex vivo proliferation and IFNɣ secretion induced by stimulation of T splenocytes. This effect is mediated both by cell-cell contact through increased PD-L1 expression on plasma cells and by production of a soluble factor. These observations are recapitulated in three cohorts of critically ill patients with bacterial and viral sepsis in association with increased mortality. Our findings thus reveal the function of regulatory plasma cells in the pathophysiology of sepsis-induced immune alterations, and present a potential therapeutic target for improving immune cell function impaired by sepsis.
Suggested Citation
Morgane Gossez & Clara Vigneron & Alexandra Vandermoeten & Margot Lepage & Louise Courcol & Remy Coudereau & Helena Paidassai & Laurent Jallades & Jonathan Lopez & Khalil Kandara & Marine Ortillon & M, 2025.
"PD-L1+ plasma cells suppress T lymphocyte responses in patients with sepsis and mouse sepsis models,"
Nature Communications, Nature, vol. 16(1), pages 1-17, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-57706-9
DOI: 10.1038/s41467-025-57706-9
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