Limited role for ASC and NLRP3 during in vivo Salmonella Typhimurium infection.

[typhoid]

The inflammasome is an intracellular protein complex triggered by exposure to intracellular pathogens , its components or other endogenous proteins . It leads to the activation of and subsequent release of proinflammatory cytokines such as IL -1 β and IL -18 . S . Typhimurium is a Gram -negative intracellular bacterium , which is known to trigger inflammasome assembly via recognition by the cytosolic receptors , NLRP 3 and NLRC 4 (which act via the adaptor protein , ASC ) to induce cell death and cytokine release . We sought to characterize the role of ASC and NLRP 3 in two different murine models (typhoid and colitis ) of systemic Salmonella infection .Release of the inflammasome cytokine IL -18 was hampered in Asc-/- but not Nlrp 3 -/- mice (background C 5 7 BL /6 ) during S . Typhimurium infection . Unexpectedly , neither ASC nor NLRP 3 played a significant role in host defense against S . Typhimurium infection , as reflected by equal bacterial counts in WT , Asc-/- and Nlrp 3 -/- mice at all time points , in both the typhoid and colitis models . Proinflammatory cytokine levels (TNF -α , IL -6 ) and the extent of hepatic and splenic pathology did not differ between groups in the typhoid model . In the colitis model small differences were seen with regard to splenic and hepatic inflammation , although this was IL -18 independent .IL -18 release was reduced in Asc-/- but not Nlrp 3 -/- mice during S . Typhimurium infection . Despite this reduction , bacterial counts , cytokine levels and histological inflammation did not differ between wild-type and knockout mice in either model . Our results reveal a limited role for ASC and NLRP 3 during in vivo S . Typhimurium infection despite its role in cytokine maturation .