Thromboxane receptor activation in dendritic cells mitigates sepsis by suppressing S100a8/a9-mediated neutrophil recruitment
Summary
Dendritic cells (DCs) regulate both innate and adaptive immunity during sepsis. Prostaglandins (PGs), small lipid molecules derived from arachidonic acid via COX enzymes, are crucial regulators of immune homeostasis and inflammation. However, their role in sepsis pathogenesis remains poorly defined. In this study, we identified a significant negative correlation between DC depletion and disease severity in patients with sepsis. Thromboxane (TX) A2 receptor (TP) expression was markedly redu
Content
# Thromboxane receptor activation in dendritic cells mitigates sepsis by suppressing S100a8/a9-mediated neutrophil recruitment
*Published: 2026 Mar 3*
Dendritic cells (DCs) regulate both innate and adaptive immunity during sepsis.
Prostaglandins (PGs), small lipid molecules derived from arachidonic acid via
COX enzymes, are crucial regulators of immune homeostasis and inflammation.
However, their role in sepsis pathogenesis remains poorly defined. In this
study, we identified a significant negative correlation between DC depletion and
disease severity in patients with sepsis. Thromboxane (TX) A2 receptor (TP)
expression was markedly reduced in the blood DCs of patients with sepsis.
Patients with low DC-TP expression presented increased blood neutrophil counts
and worsened disease severity. In murine models of sepsis induced by cecal
ligation and puncture and lipopolysaccharide challenge, DC-specific TP
deficiency exacerbated sepsis by promoting S100a8/a9-mediated neutrophil
recruitment and, subsequently, neutrophil extracellular trap (NET) formation and
lung injury. Genetic and pharmacological inhibition of the S100a8/a9-TLR4 axis
protected TP-deficient mice from fatal sepsis. Mechanistically, TP signaling
suppressed S100a8/a9 expression in DCs via PKCĪ“-Stat1 signaling, thereby
restricting neutrophil infiltration and NET formation. Finally, the targeted
activation of TP in DCs via the nanodrug DCpep-U-46619 effectively alleviated
sepsis-induced lung injury in mice. These findings establish TP as a critical
immunoregulatory receptor in DCs, highlighting its potential as a therapeutic
target for sepsis.
DOI: 10.1038/s41392-026-02592-w