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Sphingosine-1-Phosphate Receptor Type 4 (S1P4) Is Differentially Regulated in Peritoneal B1 B Cells upon TLR4 Stimulation and Facilitates the Egress of Peritoneal B1a B Cells and Subsequent Accumulation of Splenic IRA B Cells under Inflammatory Conditions.

Janik RieseAlina GromannFelix LührsAnnabel KleinwortTobias Schulze
Published in: International journal of molecular sciences (2021)
The S1P-S1PR system is implicated in the trafficking of LPS-activated peritoneal B cells. Given the protective role of peritoneal B1a B cells in peritoneal sepsis, further experiments to investigate the impact of S1P4-mediated signaling on the severity and mortality of peritoneal sepsis are warranted.
Keyphrases
  • intensive care unit
  • inflammatory response
  • immune response
  • oxidative stress
  • type diabetes
  • toll like receptor
  • septic shock
  • nuclear factor