Increased inducible apoptosis in CD4+T lymphocytes during polymicrobial sepsis is mediated by Fas ligand and not endotoxin

Abstract

Recent studies suggest that increased lymphocyte apoptosis (A_o) detected in peripheral blood T cells from burn patients appears to contribute to decreased lymphocyte immunoresponsiveness. However, while it is known that sepsis induces a marked depression in the splenocyte immune response (i.e. decreased interleukin-2, interferon-γ production and proliferation) in response to the T-cell mitogen concanavalin A (Con A), it is unknown whether this depression is associated with an increase in inducible A_o and if so, which mediators control this process. To assess this, splenocytes were harvested from mice at 24 hr (a period associated with decreased Con A response) after the onset of polymicrobial sepsis [caecal ligation and puncture (CLP)] or sham-CLP (Sham) and then stimulated with 2·5 μg Con A/ml (24 hr). Septic mouse splenocytes stimulated with Con A, while not showing a change in their phenotypic make-up, did exhibit a marked increase in the percentage of splenocyte that were A_o⁺ which was associated with altered cytokine release. This appears to be due to an increase in the percentage of A_o⁺ cells in the CD4⁺ CD8⁻ population and was associated with enhanced Fas antigen expression as well as an increase in mRNA for the Fas–FasL gene family. To determine if the changes in A_o are due to either endotoxin (a product of Gram-negative bacteria seen in CLP mice) or the expression of Fas ligand (FasL; a mediator of activation-induced lymphocyte A_o), a second set of studies examining Con A-inducible A_o was performed with splenocytes harvested from septic endotoxin-tolerant C3H/HeJ and the FasL-deficient C3H/HeJ-Fasl ^gld mice. The results show that increased splenocyte A_o detected following CLP is due to a FasL-mediated process and not to endotoxin. Thus the inadvertent up-regulation of FasL-mediated splenocyte A_o may contribute to the depression of splenocyte immune responses seen during polymicrobial sepsis.